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TW201111364A - Renin inhibitors - Google Patents

Renin inhibitors Download PDF

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Publication number
TW201111364A
TW201111364A TW98132739A TW98132739A TW201111364A TW 201111364 A TW201111364 A TW 201111364A TW 98132739 A TW98132739 A TW 98132739A TW 98132739 A TW98132739 A TW 98132739A TW 201111364 A TW201111364 A TW 201111364A
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Taiwan
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alkyl
halogens
compound
etoac
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TW98132739A
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Chinese (zh)
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TWI472524B (en
Inventor
Austin Chih-Yu Chen
Daniel Dube
Pierre-Andre Fournier
Erich L Grimm
Patrick Lacombe
Sebastien Laliberte
Dwight Macdonald
D Bruce Mackay
Daniel James Mckay
Tom Yao-Hsiang Wu
Louis-Charles Campeau
Jeremy Peter Scott
Nadine Bremeyer
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Merck Frosst Canada Ltd
Merck Sharp & Dohme
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Priority to TW98132739A priority Critical patent/TWI472524B/en
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Abstract

The present invention relates to pyridine-bearing amino amide-based renin inhibitor compounds, and their use in treating cardiovascular events and renal insufficiency.

Description

201111364 六、發明說明: 【發明所屬之技術領域】 本發明係關於新穎通式(I)腎素抑制劑。本發明亦關於一 些相關方面,包括製備該化合物之方法’含有一或多種式 (I)化合物之醫藥組合物,及尤其是其在心血管事件與腎機 能不全中作為腎素抑制劑之用途。 本申請案係主張個別於2008年8月7日與2008年5月5日提 出申請之美國臨時申請案號61Λ88,303與61/126,529之權益。 • 【先前技術】 在腎素-血管收縮素系統(RAS)中,生物活性企管收縮素π (Ang II)係藉由兩步驟機制產生。高度專一酵素腎素會使血 管收縮素原分裂成血管收縮素I (Ang I),其係接著藉由較不 專一之血管收縮素轉化酶(ACE),進一步被處理成Ang II。 已知Ang II會在至少兩種稱為AT!與AT2之受體亞型上發生 作用。雖然八丁丨似乎會傳輸Ang II之大部份已知功能,但aT2 之角色仍然為未知。 ® RAS之調制係代表心血管疾病治療上之一項主要進展。 ACE抑制劑與AT!阻斷劑已被接受,以治療高血壓(Waeber B. 專人,"腎素-血官收縮素系統:於實驗與人類高血壓上之角 色 '在 Birkenhager W. H” Reid J. L.(編著):Hyperiewsion,Amsterdam, Elsevier 科學出版公司,1986, 489-519; Weber M. A.,Am. J. Z/yperie/w., 1992, 5, 247S中)。此外,ACE抑制劑係用於腎保護(Rosenberg M. E.等人,沿办Jniemaiiona/,1994, 45, 403 ; Breyer J. Α·等人,沿也❹ ㈣2/,1994, 45, S156),以預防鬱血性心衰竭(Vaughan D. Ε· 143482-1 201111364 等人,Qzrd/oviwc. /?α·,1994,2S,159 ; Fouad-Tarazi F.等人,Am. 乂 Med.,1988,私(# 龙 3A),83)與心肌梗塞(Pfeffer M. A.等人,Μ J. Mei/.,1992, 327, 669)。 發展腎素抑制劑之理論基礎是腎素之專一性(1^&1111· D.,Cari/wwwc. Dmgj·,1995,9, 645)。關於腎素所已知之唯一受 質係為血管收縮素原,其僅能夠被腎素處理(在生理學條件 下)。對照上而言,ACE除了 Ang I之外,亦可使血管舒緩激 肽分裂,且可被糜蛋白酶旁通,該蛋白酶為一種絲胺酸蛋 白酶(Husain A·, J. //沙州泛肌,1993, 7i, 1155)。於病患中,ACE之 抑制因此會導致血管舒緩激肽蓄積,造成咳嗷(5-20%),及 潛在地威脅生命之血管神經性水腫(0.1-0.2%) (Israili Z. H.等 人,冷存卒鑑,1992, W7, 234)。糜蛋白酶不會被ACE抑制劑抑 制。因此,Ang II之形成,在以ACE抑制劑治療之病患中仍 然可能。於另一方面,AT\受體之阻抑(例如藉由若沙坦 (losartan)),會使其他AT-受體亞型(例如AT2)過度曝露至Ang II,其濃度係因AT!受體之阻抑而顯著地增加。概略言之, 預期腎素抑制劑,關於在阻斷RAS之功效及在安全性方面 上,係展現與ACE抑制劑及AT!阻斷劑不同之醫藥作用形 態。 本發明係關於具有非肽性質與低分子量之腎素抑制劑之 確認。明確言之,口服活性腎素抑制劑係經描述,其具有 長作用期,且在除了血壓調節以外之適應徵上具有活性, 其中組織腎素-糜蛋白酶系統可被活化,導致以病理生理學 方式改變之局部功能,譬如腎、心臟及血管改造,動脈粥 143482-1 201111364 瘤硬化,及可能為再狹窄。 於本發明中所述之化合物係表示 種類。 【發明内容】 w之新穎結構 本發明係針對某些化合物,及其在腎素酵素 途,包括治療已知與腎素系統有關聯之症狀。' 本發明係特別針對式I化合物: 抑制上 之用201111364 VI. Description of the Invention: TECHNICAL FIELD OF THE INVENTION The present invention relates to novel renin inhibitors of the general formula (I). The invention also relates to some related aspects, including a method of preparing the compound, a pharmaceutical composition comprising one or more compounds of formula (I), and especially its use as a renin inhibitor in cardiovascular events and renal insufficiency. This application claims the benefit of U.S. Provisional Application Nos. 61, 88, 303 and 61/126, 529, filed on August 7, 2008, and on May 5, 2008. • [Prior Art] In the renin-angiotensin system (RAS), the bioactive vasoconstrictor π (Ang II) is produced by a two-step mechanism. The highly specific enzyme renin cleaves vasopressin into angiotensin I (Ang I), which is then further processed into Ang II by a less specific angiotensin converting enzyme (ACE). Ang II is known to act on at least two receptor subtypes called AT! and AT2. Although Octopus seems to transmit most of the known functions of Ang II, the role of aT2 is still unknown. ® RAS modulation represents a major advance in the treatment of cardiovascular disease. ACE inhibitors and AT! blockers have been accepted to treat hypertension (Waeber B. Dedicated, "Renin-Cytokinin system: role in experiments and human hypertension' at Birkenhager W. H" Reid JL (eds.): Hyperiewsion, Amsterdam, Elsevier Science Publishing Company, 1986, 489-519; Weber MA, Am. J. Z/yperie/w., 1992, 5, 247S). In addition, ACE inhibitors are used. Kidney protection (Rosenberg ME et al., Junimaiiona/, 1994, 45, 403; Breyer J. Α· et al., Yan Ye (4) 2/, 1994, 45, S156) to prevent septic heart failure (Vaughan D Ε· 143482-1 201111364 et al., Qzrd/oviwc. /?α·, 1994, 2S, 159; Fouad-Tarazi F. et al., Am. 乂Med., 1988, private (#龙3A), 83) And myocardial infarction (Pfeffer MA et al, Μ J. Mei/., 1992, 327, 669). The theoretical basis for the development of renin inhibitors is the specificity of renin (1^&1111·D., Cari/wwwc Dmgj·, 1995, 9, 645). The only substrate known to renin is angiotensinogen, which can only be treated with renin (under physiological conditions). In addition to Ang I, ACE can also cause vasopressin cleavage and can be bypassed by chymotrypsin, which is a serine protease (Husain A·, J. //Shazhou Pan Muscle, 1993, 7i , 1155). In patients, inhibition of ACE results in accumulation of vasopressin, coughing (5-20%), and potentially life-threatening vascular edema (0.1-0.2%) (Israili ZH Et al., Chilling, 1992, W7, 234). Chymotrypsin is not inhibited by ACE inhibitors. Therefore, the formation of Ang II is still possible in patients treated with ACE inhibitors. Repression of AT\receptors (eg, by losartan) overexpresses other AT-receptor subtypes (eg, AT2) to Ang II at concentrations that are inhibited by AT! receptors Significantly increased. In summary, renin inhibitors are expected to exhibit different pharmacological modalities from ACE inhibitors and AT! blockers in terms of their efficacy in blocking RAS and in terms of safety. Confirmation of a renin inhibitor with non-peptide properties and low molecular weight. Specifically, oral active renin inhibitors are described as having a long duration of action and are active in indications other than blood pressure regulation, wherein the tissue renin-chymotrypsin system can be activated, resulting in pathophysiology Local changes in the way, such as kidney, heart and blood vessel transformation, atherosclerosis 143482-1 201111364 tumor hardening, and possibly restenosis. The compounds described in the present invention represent the species. SUMMARY OF THE INVENTION The novel structure of w is directed to certain compounds, and their effects on the renin enzyme, including the treatment of symptoms known to be associated with the renin system. ' The invention is specifically directed to compounds of formula I: for inhibition

R2 R3R2 R3

(Ζ)η1Υ(Ζ)η1Υ

及其光學上純對掌異構物’對掌異構物之混合物,…卜 消旋物,非對映異構物,非對映異構物之混合物,::映 異構外消旋物,非對映異構外消旋物之混合物内消旋开; 式,鹽,溶劑合物及形態學形式,其中組份成員係提= 本文中。 ' 揭示内容之詳細說明 本發明係提供具有式I之化合物: 143482-1And optically pure mixture of palmo-isomers, palmo isomers, ... racemates, diastereomers, mixtures of diastereomers, :: imager racemates a mixture of diastereomeric racemates in the form of a racemic formula; a salt, a solvate, and a morphological form, wherein the members of the component are referred to herein. DETAILED DESCRIPTION OF THE DISCLOSURE The present invention provides a compound having Formula I: 143482-1

I I201111364I I201111364

或其藥學上可接受之鹽,其中: R1係選自下列組成之組群:Ci_C6_院基、環烧基、 CVC6烯基、CVC:6環烯基及仏必炔基,其中各前述係視情況 被1-3個鹵素及/或Cl _C5烷氧基取代; R2與R3係獨立選自下列組成之組群:氫、•素、c]_c5 烧基、c3-c8環烧基' c2_c5稀基、C3_Cyf稀基、炔基、 氛基、Cl-C:5烷氧基、芳基及雜芳基, 其中該雜芳基含有1至3個雜原子,獨立選自下列 組成之組群:N、Ο及S,其中各⑽視情況呈氧化物之形 式’且各S係視情況呈氧化物之形式,選自下列組成之組 群:S(=〇)與 s(=〇)2, 其中該芳基與雜芳基係視情況被M個鹵素取代, 其中該烷基、環烷基、烯基、環烯基、炔基及烷 氧基係視情況被丨_3個取代基取代,其每一個係獨立選自下 列組成之組群:_素、c丨-C5烷基、c2_C5烯基、氰基及Ci_c5 烷氧基,其中各前述烷基、烯基及烷氧基取代基係視情況 被1-3個鹵素取代; 你為環丙基,未經取代或被氟單-、二-、三-、四-或 143482-1 2011Π364 五取代; X係選自下列組成之組群:OR4、R4、-(C丨-〇5伸炫基)-(〇)〇-1 -芳基及-(Ci 伸烧基)_(〇)〇-1 -雜芳基’ 其中R4係選自下列組成之組群:氫、C〗-C5烷基、 C3_C8環烧基、C2-C5稀基、C3-C8環稀基、C2-C5炔基、C1-C5-氰基、-(C, -C5 伸烷基)-〇-R5、-(q -c5 伸烷基)-N(-R5 )-0(=0)-((^ -C5 烷基)、-(C! -C5 伸烷基)-C(=〇)-N(-R5 HQ -C5 烷基)、-(C! -C5 伸烷 基)-N(-R5 )-(:(=0)-0-((:】-C5 烷基)、-(C, -C5 伸烷基)-0-C(=0)-N(-R5 )-(C! -C5 烧基);-(Ci -C5 伸院基)-N(-R5)-% -C5 炫基)、-(Ci -C5 伸烧 基)-S-A -C5 烷基)、-(C! -C5 伸烷基)-5(=0)-((^ -C5 烷基)及-(C! -C5 伸烷基)4(=0)2-((^-(:5 烷基), 其中R4 ’除了氫以外’係視情況被i_3個取代基取 代,取代基獨立選自下列組成之組群:鹵素、C(=〇)〇H、q -C5 烧基、CyC:5烯基及C〖-C:5烷氧基,其中各烷基、烯基及烷氧 基取代基係視情況被1-3個鹵素取代, 其中-(C! -C:5伸烷基)-(0)〇_ t -雜芳基之雜芳基含有1-3 個雜原子’獨立選自下列組成之組群:N、〇及s ,其中各 N係視情況呈氧化物之形式,且各3係視情況呈氧化物之形 式,選自下列組成之組群:s(=0)與s(=〇)2, 其中-(c! -cs伸烷基)-(〇)〇_】_芳基與_(Ci _C5伸烷基)_ (〇)〇M雜芳基之芳基與雜芳基係個別視情況被1-4個鹵素取 代,且 其中R5係選自下列組成之組群:氫、Ci_C6烷基、 C3 C6%烷基' C2-C6烯基、C3_C6環烯基及C2-C6炔基,其中 143482-1 201111364 各前述烧基、環隸、絲、㈣基及絲取代基係視情 況被1-3個鹵素取代; 乙為(:1-〇2伸烷基,視情況被μ2個取代基取代,取代基 獨立選自下列組成之組群:盘素、Ci々烷基及。環烷基: 其中前述院基與環烧基取代基係視情況被U㈣素取代; nl為0或1 ; 二⑴五-或六-員飽和或不飽和雜環族或碳環族 狀環單環狀環,V或⑻五·或六項飽和或不飽和雜環族或 =環族環,其係、經桐合至五.或六.員飽和或不飽和雜環族 或碳環族環(,,稠合環"), 其中⑴或⑻之雜環含有丨_3個獨立選自N、〇及3之 其中各N係視情況呈氧化物之形式,且各s係視情 氧化:之形式,選自下列組成之組群:s(=〇)與s(=〇)2 ’ _ _ “中⑴或⑻之雜環族或碳環族環係視情況經單_、 ;列二:、四-、五-或六取代,其中各取代基係獨立選自 夕』組成之組群: ⑴ii素, (2) -OH, ⑶-NH(R6), (4) 酮基, (5) -C(=〇).r6 , (6) -0-C(=〇).r6 , ()c〗-C5烷基,視情況被13個鹵素取代, ⑻Q-C8環炫基’視情況被Μ個鹵素取代, 143482-] 201111364 (9) C2 -C5烯基’視情況被ι_3個鹵素取代, (10) C3 -C8環烯基’視情況被1_3個鹵素取代, (11) C2-C5炔基,視情況被1_3個鹵素取代, (12) C】-C5烧氧基,視情況被1-3個鹵素取代, (13) 氰基, (14) 氰基’視情況被1-3個鹵素取代, (15) -OCF3, (16) -C(R7)3, (17) -(C〗 -CI5伸烧基)-OR8,視情況被ι_3個鹵素取代, (18) -NCR6)-% -Q伸烧基)-〇R8,視情況被1_3個鹵素 取代, (19) -0-(C丨-C5伸烧基)-OR8,視情況被1-3個鹵素取代, (20) -S-(C! -C5伸烧基)-OR8 ’視情況被1-3個_素取代, (21) -S(=0)-(C] -C5伸烧基)-OR8,視情況被1-3個鹵素取 代, (22) -S(=0)2-(C丨-C5伸院基)-OR8 ’視情況被1-3個鹵素 取代, (23) -(C〗-C5 伸烷基)-N(R6)-C(=0)-(Cl _c5 伸烷基)_R8,視 情況被1-3個鹵素取代, (24) -(C】伸烷基)-N(R0)-C(=〇)-〇R8,視情況被 1-3 個 鹵素取代, (25) -(C! -C:5伸烷基)-N(R6 )(R8) ’視情況被!_3個齒素取 代, (26) -CKC〗-C5 伸烷基)-C(R6)2-C(=〇)〇r8,視情況被 13 143482-1 201111364 個鹵素取代, (27) -(C] -C5 伸烷基)-C(R6)2-C(=0)-0R8,視情況被 1-3 個鹵素取代, (28) -0-((:! -C5伸烷基)-嗎福啉,視情況被1-3個鹵素 取代, (29) -0C(=0)-嗎福啉, (30) -SR8, (31) -S(=0)-R8, (32) -S(=0)2-R8 (33) -N(R6)(R8), (34) -(C] -C5伸烷基)-C(R6)2-(R8),視情況被1-3個鹵素 取代, (35) -(R9)〇-iR10 5 (36) C2-C5烯基-OR8 ’視情況被1-3個鹵素取代, (37) C2-C5炔基-OR8,視情況被1-3個鹵素取代, (38) -(C! -C5 伸烷基-C5 伸烷基)-R8,視情況 被1-3個鹵素取代’ (39) -(C! -Q 伸烷基)-〇-C(=0)-(C丨-C5 伸烷基)-R8,視情 況被1-3個鹵素取代’ (40) _(CrC5伸烷基)-C(=0)-N(R6)(R8),視情況被 1-3 個 鹵素取代, (41) -(q -C5 伸烷基)-0-C(=0)-N(R6)(R8),視情況被 1-3 個鹵素取代, (42MQ _C5伸烷基)-张8 ’視情況被1-3個i素取代’ 143482-1 •10- 201111364 (43) -(q -C:5伸烧基)-S(=〇)-R8 ’視情況被1-3個鹵素取 代,及 (44) -(q -C5伸烷基)-S(=〇)2 -R8,視情況被μ3個鹵素取 代, 其中R6係選自下列組成之組群:氫、Cl _c6烷基、 Q-c:8環烷基、q-c:6烯基、Q-C8環烯基及匸2_匚6炔基,其中 各前述烷基、環烷基、烯基、環烯基及炔基取代基係視情 況被1-3個鹵素取代,Or a pharmaceutically acceptable salt thereof, wherein: R1 is selected from the group consisting of Ci_C6_homoyl, cycloalkyl, CVC6 alkenyl, CVC: 6 cycloalkenyl and azetidinyl, wherein each of the foregoing Depending on the case, it is substituted by 1-3 halogens and/or Cl _C5 alkoxy groups; R 2 and R 3 are independently selected from the group consisting of hydrogen, ketone, c] _c5 alkyl, c3-c8 cycloalkyl 'c2_c5 a dilute group, a C3_Cyf dilute group, an alkynyl group, an aryl group, a Cl-C: 5 alkoxy group, an aryl group and a heteroaryl group, wherein the heteroaryl group has 1 to 3 hetero atoms, and is independently selected from the group consisting of the following groups : N, Ο and S, wherein each (10) is in the form of an oxide as appropriate and each S is in the form of an oxide, selected from the group consisting of: S (= 〇) and s (= 〇) 2 Wherein the aryl group and the heteroaryl group are optionally substituted by M halogens, wherein the alkyl group, the cycloalkyl group, the alkenyl group, the cycloalkenyl group, the alkynyl group and the alkoxy group are optionally referred to as _3 substituents. Substituting each of them independently selected from the group consisting of _, c丨-C5 alkyl, c2_C5 alkenyl, cyano and Ci_c5 alkoxy, wherein each of the aforementioned alkyl, alkenyl and alkoxy groups is substituted Base system as appropriate Substituted by 1-3 halogens; you are cyclopropyl, unsubstituted or substituted by fluorine mono-, di-, tri-, tetra- or 143482-1 2011Π364 five; X is selected from the group consisting of: OR4 , R4, -(C丨-〇5), -(〇)〇-1 -aryl and -(Ci extended alkyl)_(〇)〇-1 -heteroaryl' wherein R4 is selected from the following Group consisting of: hydrogen, C--C5 alkyl, C3_C8 cycloalkyl, C2-C5 dilute, C3-C8 cycloaliphatic, C2-C5 alkynyl, C1-C5-cyano, -(C, - C5 alkyl)-〇-R5, -(q-c5 alkyl)-N(-R5)-0(=0)-((^-C5 alkyl), -(C!-C5 alkyl) )-C(=〇)-N(-R5 HQ -C5 alkyl), -(C! -C5 alkylene)-N(-R5)-(:(=0)-0-((:]- C5 alkyl), -(C, -C5 alkyl)-0-C(=0)-N(-R5)-(C!-C5 alkyl);-(Ci-C5 extension)-N (-R5)-%-C5 炫基), -(Ci-C5 alkyl)-SA-C5 alkyl), -(C!-C5 alkyl)-5(=0)-((^ C5 alkyl) and -(C! -C5 alkyl) 4(=0)2-((^-(:5 alkyl), wherein R4 'except hydrogen is replaced by i_3 substituents as appropriate, The substituents are independently selected from the group consisting of halogen, C(=〇)〇H, q-C5 alkyl, CyC: 5 alkenyl and C 〖-C: 5 alkoxy, wherein each alkyl, alkenyl and alkoxy substituent is optionally substituted with 1-3 halogens, wherein -(C! -C:5 The alkyl)-(0)〇_t-heteroaryl heteroaryl group contains 1-3 heteroatoms' independently selected from the group consisting of N, hydrazine and s, wherein each N is optionally an oxide In the form of an oxide, each of which is optionally in the form of an oxide selected from the group consisting of s(=0) and s(=〇)2, wherein -(c!-csalkyl)-(〇 〇 _ _ _ aryl and _ (Ci _C5 alkyl) 〇 (〇) 〇 M heteroaryl aryl and heteroaryl are individually substituted by 1-4 halogens, and wherein R 5 is selected from a group consisting of hydrogen, Ci_C6 alkyl, C3 C6% alkyl 'C2-C6 alkenyl, C3_C6 cycloalkenyl and C2-C6 alkynyl, wherein 143482-1 201111364 each of the aforementioned alkyl, ring, silk, (d) The base and silk substituents are optionally substituted by 1-3 halogens; B is (: 1-〇2 alkylene, optionally substituted by μ2 substituents, the substituents are independently selected from the group consisting of: , Ci, alkyl and. Cycloalkyl: wherein the aforementioned substituent and cycloalkyl substituent are optionally substituted by U(tetra); nl is 0 or 1; di(1)5- or 6-membered saturated or unsaturated heterocyclic or carbocyclic ring Cyclic ring, V or (8) penta- or six-membered saturated or unsaturated heterocyclic or = cyclocyclic ring, which is a sulphonic or unsaturated heterocyclic or carbocyclic ring. (,, fused ring "), wherein the hetero ring of (1) or (8) contains 丨_3 independently selected from N, 〇 and 3, each of which is in the form of an oxide, and each s is oxidized as it is. : a form selected from the group consisting of: s(=〇) and s(=〇)2 ' _ _ "the heterocyclic or carbocyclic ring of (1) or (8) is optionally treated as a single _; Two: four-, five- or six-substituted, wherein each substituent is independently selected from the group consisting of: (1) ii, (2) -OH, (3)-NH(R6), (4) keto, ( 5) -C(=〇).r6 , (6) -0-C(=〇).r6 , ()c〗-C5 alkyl, optionally substituted by 13 halogens, (8) Q-C8 cyclodextrin The situation is replaced by a halogen, 143482-] 201111364 (9) C2 -C5 alkenyl' is replaced by ι_3 halogens, (10) C3 -C8 cycloalkenyl 'Substituted by 1_3 halogens, (11) C2-C5 alkynyl, optionally substituted by 1_3 halogens, (12) C]-C5 alkoxy, optionally substituted by 1-3 halogens, (13) Cyano, (14) Cyano' is optionally substituted by 1-3 halogens, (15) -OCF3, (16) -C(R7)3, (17) -(C) -CI5 extended alkyl)-OR8 , as the case may be replaced by ι_3 halogens, (18) -NCR6)-% -Q extended alkyl)-〇R8, optionally substituted by 1_3 halogens, (19) -0-(C丨-C5 stretching base) -OR8, substituted by 1-3 halogens as appropriate, (20) -S-(C! -C5 stretching base)-OR8 'Substituted by 1-3 _ primes, (21) -S(=0 )-(C] -C5 extended alkyl)-OR8, optionally substituted by 1-3 halogens, (22) -S(=0)2-(C丨-C5 extension base)-OR8 'as appropriate 1-3 halogen substitutions, (23) -(C--C5 alkylene)-N(R6)-C(=0)-(Cl _c5 alkyl)-R8, optionally substituted by 1-3 halogens , (24) -(C)alkylene)-N(R0)-C(=〇)-〇R8, optionally substituted by 1-3 halogens, (25) -(C! -C:5-alkylene Base)-N(R6)(R8) 'Replaced by _3 dentitions as appropriate, (26) -CKC〗-C5 alkyl)-C(R6)2-C(=〇)〇r8, as appropriate Being 13 143482-1 20 1111364 halogen substitutions, (27) -(C) -C5 alkylene)-C(R6)2-C(=0)-0R8, optionally substituted by 1-3 halo, (28) -0-( (:! -C5 alkyl)-morpholine, optionally substituted by 1-3 halogens, (29) -0C(=0)-morpholine, (30) -SR8, (31) -S( =0)-R8, (32) -S(=0)2-R8 (33) -N(R6)(R8), (34) -(C] -C5 alkylene)-C(R6)2- (R8), optionally substituted by 1-3 halogens, (35) -(R9)〇-iR10 5 (36) C2-C5 alkenyl-OR8 'Substituted by 1-3 halogens, (37) C2 -C5 alkynyl-OR8, optionally substituted with 1-3 halogens, (38) -(C! -C5alkyl-C5 alkylene)-R8, optionally substituted by 1-3 halo' ) -(C! -Q alkylene)-〇-C(=0)-(C丨-C5 alkyl)-R8, optionally substituted by 1-3 halogens '(40) _(CrC5) Base) -C(=0)-N(R6)(R8), optionally substituted by 1-3 halogens, (41) -(q -C5 alkylene)-0-C(=0)-N( R6)(R8), as the case may be replaced by 1-3 halogens, (42MQ _C5 alkylene group) - Zhang 8 'as replaced by 1-3 i elements as appropriate] 143482-1 •10- 201111364 (43) -( q -C:5 stretching base)-S(=〇)-R8 'Substituted by 1-3 halogens, and (44 -(q -C5alkylene)-S(=〇)2 -R8, optionally substituted by μ3 halogens, wherein R6 is selected from the group consisting of hydrogen, Cl _c6 alkyl, Qc: 8 ring An alkyl group, qc:6 alkenyl group, Q-C8 cycloalkenyl group and 匸2_匚6 alkynyl group, wherein each of the aforementioned alkyl, cycloalkyl, alkenyl, cycloalkenyl and alkynyl substituents is optionally taken 1 -3 halogen substitutions,

其中R7為鹵素, 其中R8係選自下列組成之組群:氫、q %烷基、 C3-Cs環烷基、(VC6烯基、C3_C8環烯基&C2_C6炔基,其中 各別述烷基、環烷基、烯基、環烯基及炔基取代基係視情 況被1-3個鹵素取代, 其中R9係選自下列組成之組群:_c(H)(〇H)、_c(=〇)_、 0C(-0)_、-C(=0)0_、_〇_、_〇c(=〇)〇、q Q伸烷基、C2_C5 伸烯基、-N(R6)-、-s-、-S(=0)_、养〇)2 _、_N(R6)_c(=〇)_、_c(=〇)_ _)-、-0C(=0)_N(R6)·、_N(R6)c(=〇)〇_、戰6)|_〇)2_、 、(〇)2-N(R )-,其中各前述伸燒基與伸稀基取代基係視情況 被1-3個鹵素取代,且其中沪係定義於上文,及 其中R10為五-或六-員飽和或不飽和雜環族或碳環 族環,其係視情況經單、二、三-、四-或五取代,其中 各取代基係獨立選自下列組成之組群:鹵素、-0H、-SR6、 N(R )(R )、c】_c5烧基、CrG環烧基、烯基 ' 匸…環 '土 c2-c5炔基、C丨-c5烷氧基、氰基及C1_C5_氰基,其中 143482-1 201111364 該雜環含有1至3個獨立選自N、〇及5之雜原子,其中各n 係視情況呈氧化物之形式’且各5係視情況呈氧化物之妒 式’選自下列組成之組群:s(=〇)或s(=〇)2,及其中%與助 係定義於上文。 於-項具體實施例中,本發明係提供式工化合物或其藥學 上可接受之鹽或其光學異構物,其中γ⑴或⑼之單環狀或 铜合環係個別選自下列:Wherein R7 is halogen, wherein R8 is selected from the group consisting of hydrogen, q% alkyl, C3-Cs cycloalkyl, (VC6 alkenyl, C3_C8 cycloalkenyl) and C2_C6 alkynyl, wherein each alkane The base, cycloalkyl, alkenyl, cycloalkenyl and alkynyl substituents are optionally substituted with from 1 to 3 halogens, wherein R9 is selected from the group consisting of: _c(H)(〇H), _c( =〇)_, 0C(-0)_, -C(=0)0_, _〇_, _〇c(=〇)〇, q Q alkyl, C2_C5 alkenyl, -N(R6)- , -s-, -S(=0)_, raise 〇) 2 _, _N(R6)_c(=〇)_, _c(=〇)_ _)-, -0C(=0)_N(R6) ·, _N(R6)c(=〇)〇_, war 6)|_〇)2_, , (〇)2-N(R)-, wherein each of the above-mentioned extended and extended substituents is as appropriate Substituted by 1-3 halogens, and wherein the Shanghai system is defined above, and wherein R10 is a five- or six-membered saturated or unsaturated heterocyclic or carbocyclic ring, which is singular, two or three depending on the situation. a tetra- or penta-substituted group in which each substituent is independently selected from the group consisting of halogen, -OH, -SR6, N(R)(R), c]-c5 alkyl, CrG cycloalkyl, alkene Base '匸...ring' soil c2-c5 alkynyl, C丨-c5 alkoxy, cyano and C1_C5_cyanide Wherein 143482-1 201111364 the heterocyclic ring contains 1 to 3 heteroatoms independently selected from N, fluorene and 5, wherein each n is optionally in the form of an oxide and each of the 5 systems is optionally an oxide 'Selected from the following group: s (= 〇) or s (= 〇) 2, and % and helper lines are defined above. In a specific embodiment, the present invention provides a compound of the formula, or a pharmaceutically acceptable salt thereof, or an optical isomer thereof, wherein the monocyclic or copper ring of γ(1) or (9) is individually selected from the following:

'43482-1 -12- 201111364 於另一項具體實施例中,本發明係提供式i化合物或其藥 學上可接$之鹽或其光學異構物’其中R2與R3係獨立選自 下列組成之組群:H、-〇ch2〇Ch3及_ch3。 於另項具體實施例巾’本發明係提供式丨化合物或其藥 學上可接受之鹽或其光學異構物,其中X為H、-〇H或.OCH3。 於另-項具體實施例中,本發明係提供式】化合物或其藥 學上可接受之鹽或其光學異構物,其中W為環丙基。 於另項具體實施例巾,本發明係提供式1化合物或其藥 學上可接受之鹽或其光學異構物,其中(Z)nl為-CH2-或鍵 結。 於另項具體實施例中,本發明係提供式1化合物或其藥 學上可接受之鹽或其光學異構物,其中: R為視情況被1-3個鹵素取代之_c2烷基, R與R3係獨立選自下列組成之組群:氫、鹵素、q -c5 烷基C1-c:5烷氧基及-CKC〗-c5伸烷基)-〇-(CH2 )0 _ 3 -CH3 ,其中 烷基、烷氧基及-CHCi -C5伸烷基)_〇_(CH2 )G · 3 _Ch3係視情況被 1-3個取代基取代’取代基獨立選自下列組成之組群:齒 素、視情況被1-3個鹵素取代之q 烷基及視情況被μ3個 鹵素取代之(^-(:5烷氧基, X係選自下列組成之組群:氫、_〇Η及q _c5烷氧基, 且 z為c】-c2伸烷基。 於另一項具體實施例中,本發明係提供式I化合物或其藥 學上可接受之鹽或其光學異構物,其中γ係 143482-1 •13- 201111364 視情況如式ϊ中所述 於另一項具體實 、—-、三_、四-或五取代。 藥學卜w e例中’本發明係提供式II化合物或其 接觉之鹽或其光學異構物,'43482-1 -12- 201111364 In another embodiment, the invention provides a compound of formula i or a pharmaceutically acceptable salt thereof or an optical isomer thereof wherein R2 and R3 are independently selected from the group consisting of Groups: H, -〇ch2〇Ch3 and _ch3. The present invention provides a hydrazine compound or a pharmaceutically acceptable salt thereof, or an optical isomer thereof, wherein X is H, -〇H or .OCH3. In another embodiment, the invention provides a compound of the formula: or a pharmaceutically acceptable salt thereof, or an optical isomer thereof, wherein W is cyclopropyl. In another embodiment, the invention provides a compound of formula 1, or a pharmaceutically acceptable salt thereof, or an optical isomer thereof, wherein (Z)nl is -CH2- or a bond. In another embodiment, the invention provides a compound of Formula 1, or a pharmaceutically acceptable salt thereof, or an optical isomer thereof, wherein: R is _c2 alkyl optionally substituted with 1-3 halo, R Independent of the R3 series selected from the group consisting of hydrogen, halogen, q-c5 alkyl C1-c:5 alkoxy and -CKC--c5 alkyl)-〇-(CH2)0 _ 3 -CH3 Wherein alkyl, alkoxy and -CHCi-C5 alkylene)_〇_(CH2)G · 3 _Ch3 are optionally substituted by 1-3 substituents. The substituents are independently selected from the group consisting of: A dentate, optionally substituted with 1-3 halogens, and optionally substituted by μ3 halogens (^-(:5 alkoxy, X is selected from the group consisting of hydrogen, _〇Η) And q _c5 alkoxy, and z is c]-c2 alkyl. In another specific embodiment, the invention provides a compound of formula I, or a pharmaceutically acceptable salt thereof, or an optical isomer thereof, wherein Γ-ray 143482-1 •13- 201111364 Depending on the case, it is described in the formula 于 in another specific, --, three-, four- or five-substituted. In the pharmaceutical case, the invention provides a compound of formula II or Its salt or its optics Isomer,

IIII

A係選自下列組成之組群: ⑴氫, (2)鹵素, ⑶Ci -C5院基, (4) q-Cs烷氧基,及 (5) -S-(CH2)〇.3-CH3 . · 其中⑶與⑷係視情況被1_3個函素取代’ B係選自下列組成之組群: ⑴氫, ⑵鹵素, ⑶CVCs烷基, ⑷CVC5烷氧基, (5) -OH » ^3482-1 14 201111364 ⑹-CF3, ⑺-c(:o)-ch3, ⑻-o-A -c5伸烷基)-〇-環丙基, ⑼-〇-(c 丨-C5 伸烷基)-〇-(CH2 )0 - 2 -CH3, (10) -(C丨-C5 伸烧基)-〇-(ch2 )0 - 2 -CH3, (11) -0C(=0)-嗎福啉, (12) -CKq -C5伸烷基)-嗎福啉, (13) -0-((:, -c5 伸烷基)-c(ch3)2-c(=o)oh, (14) -0-((:[ -C5 伸烷基)-C(CH3 )2 -C(=0)0CH3, (15)Group A is selected from the group consisting of: (1) hydrogen, (2) halogen, (3) Ci-C5, (4) q-Cs alkoxy, and (5) -S-(CH2)〇.3-CH3. · Where (3) and (4) are replaced by 1_3 elements as appropriate. 'B is selected from the group consisting of: (1) hydrogen, (2) halogen, (3) CVCs alkyl, (4) CVC5 alkoxy, (5) -OH » ^3482-1 14 201111364 (6)-CF3, (7)-c(:o)-ch3, (8)-oA-c5 alkylene)-oxime-cyclopropyl, (9)-〇-(c 丨-C5 alkylene)-〇-(CH2 ) 0 - 2 -CH3, (10) -(C丨-C5 stretching group)-〇-(ch2)0 - 2 -CH3, (11) -0C(=0)-morpholine, (12) - CKq-C5 alkylene)-morpholine, (13) -0-((:, -c5 alkyl)-c(ch3)2-c(=o)oh, (14) -0-(( :[ -C5 alkylene)-C(CH3)2 -C(=0)0CH3, (15)

(16)(16)

其中(3),(4),(8),(9),(10),(12),(13),(14),(15)及(16)係視 情況被1-3個鹵素取代, C係選自下列組成之組群: ⑴氫, (2) ci -C:5院基,視情況被13個鹵素取代,及 ⑶Cl七5院氧基’視情況被1-3個鹵素取代,立 D係選自下列組成之組群: ⑴氫, (2) 1¾ 素, 143482-1 -15- 201111364 (3) (:丨-(:5烷基, (4) Ο! -C5烧氧基, (5) C丨-C5 -亂基’ ⑹ C2 -C5 伸烯基-〇-(CH2 )〇 - 2 -CH3, ⑺-(q -c5 伸烷基)-n(h)-c(=o)-o-(ch2 )〇. 2 -CH3, ⑻-(c! -c5 伸烷基)-n(h)-c(=o)-(ch2 )0.2 -CH3, (9) -(Ci -C5 伸烷基)-0-CHF2, (10) -(Ci -C5 伸烧基)-〇-(CH2 )〇 - 2 -CH3 ’ (11) -CKq -c5 伸烷基)-o-(ch2 )〇 - 2 -CH3, (12) -((^-(:5 伸烷基)-OH, (13) 4-((^-C5 伸烷基)-OH, (14) -SCF3 (15) -风11)-((:1-(:5伸烷基)-0-(〇12)()_2-〇13,及 (16)Where (3), (4), (8), (9), (10), (12), (13), (14), (15) and (16) are replaced by 1-3 halogens as appropriate , C is selected from the group consisting of: (1) hydrogen, (2) ci - C: 5 fen, optionally substituted by 13 halogens, and (3) Cl VII 5 oxime 'as replaced by 1-3 halogens The D system is selected from the group consisting of: (1) hydrogen, (2) 13⁄4, 143482-1 -15- 201111364 (3) (: 丨-(:5 alkyl, (4) Ο! -C5 burning oxygen Base, (5) C丨-C5 - chaotic base '(6) C2 -C5 alkenyl-anthracene-(CH2)〇- 2 -CH3, (7)-(q -c5 alkylene)-n(h)-c( =o)-o-(ch2 )〇. 2 -CH3, (8)-(c! -c5 alkyl)-n(h)-c(=o)-(ch2 )0.2 -CH3, (9) -( Ci-C5 alkyl)-0-CHF2, (10) -(Ci-C5 alkyl)-〇-(CH2)〇-2 -CH3 ' (11) -CKq -c5 alkyl)-o- (ch2)〇- 2 -CH3, (12) -((^-(:5 alkyl)-OH, (13) 4-((^-C5 alkyl)-OH, (14) -SCF3 ( 15) - wind 11) - ((: 1-(:5 alkyl)-0-(〇12)()_2-〇13, and (16)

其中F、G及H係獨立選自下列組成之組群:氫、 鹵素及視情況被1-3個鹵素取代之q -C3院基,且 其中.R11係選自下列組成之組群:-CH2 -、-C(H)(OH)-及-C(=0)-, 其中(3),(4),(5),(6),(7),(8),(9),(10), (11),(12),(13)及(15) 係視情況被1-3個鹵素取代,及 其中R1,R2, R3, X及(Z)n丨均如式I中所述。 於另一項具體實施例中,本發明係提供式I化合物或其藥 143482-1 •16- 201111364 學上可接受之鹽或其光學異構物,其中丫係Wherein F, G and H are independently selected from the group consisting of hydrogen, halogen and q-C3, optionally substituted by 1-3 halogens, and wherein R11 is selected from the group consisting of: - CH2 -, -C(H)(OH)- and -C(=0)-, where (3), (4), (5), (6), (7), (8), (9), (10), (11), (12), (13) and (15) are replaced by 1-3 halogens, and R1, R2, R3, X and (Z)n丨 are as in Formula I Said. In another embodiment, the invention provides a compound of formula I or a medicament thereof, 143482-1 • 16-201111364, a salt which is acceptable or optically isomer thereof, wherein the lanthanide

三-、四_、五-或六取代’如上文式I 視情況經單 中所述。 ;另項具體貫施例中,本發明係提供式in化合物或其 藥學上可接受之鹽或其光學異構物,The three-, four-, five- or six-substituted ' is as described above for the formula I. In another specific embodiment, the present invention provides a compound of the formula in or a pharmaceutically acceptable salt thereof or an optical isomer thereof,

其中: A係選自下列組成之組群: ⑴氫, ⑵_素, (3) ⑷ (5) C! -C5烧基’視情況被μ3個鹵素取代, ci 烧氧基’視情況被w個鹵素取代,及 氱基,且 B係選自下列組成之組群:氫與!|素, C係選自下列組成之組群: ⑴氫, ⑵_素, (3) -Q烷基’視情況被i_3個鹵素取代, (4) ci -A烷氧基’視情況被1_3個鹵素取代,及 143482-1 -17- 201111364 ⑶氰基, D係選自下列組成之組群: ⑴氫, ⑵鹵素, ⑶c! -C5炫基,視情況被μ3個鹵素取代, (4) C! -C5烷氧基’視情況被μ3個鹵素取代, ⑶-(c〗-c5伸烷基)_a(CH2)〇-2_CH3,視情況被υ個 鹵素取代,及 ⑹氰基,且 籲 E係選自下列組成之組群: ⑴氫, ⑵鹵素, ⑶CVq烷基, ⑷Q-Cs烯基, (5) C^-Cs烧氧基’ ⑹氰基, | ⑺-(c】-C5 伸烷基)-C(CF3 )2 (H), (8) -(Q -C5 伸烷基)-N(H)-C(=0)-(CH2 )〇 · 2 -CH3, ⑼-(q -c5 伸烷基)-〇-(CH2 )〇 - 2 -CH3, (10)Wherein: A is selected from the group consisting of: (1) hydrogen, (2) _, (3) (4) (5) C! -C5 burnt base 'substituted by μ3 halogens, ci alkoxy' as the case may be a halogen substituted, and a fluorenyl group, and B is selected from the group consisting of: hydrogen and !|, C, selected from the group consisting of: (1) hydrogen, (2) _, (3) -Q alkyl Depending on the case, i_3 halogens are substituted, (4) ci-A alkoxy group is optionally substituted by 1_3 halogens, and 143482-1 -17- 201111364 (3) cyano group, D is selected from the group consisting of: (1) hydrogen , (2) halogen, (3) c! -C5 炫, which is optionally substituted by μ3 halogens, (4) C! -C5 alkoxy' is optionally substituted by μ3 halogens, (3)-(c--c5 alkyl)_a (CH2)〇-2_CH3, optionally substituted by a halogen, and (6) a cyano group, and the E is selected from the group consisting of: (1) hydrogen, (2) halogen, (3) CVq alkyl, (4) Q-Cs alkenyl, (5) C^-Cs alkoxy' (6) cyano, | (7)-(c)-C5 alkyl)-C(CF3)2 (H), (8) -(Q -C5 alkyl)-N ( H)-C(=0)-(CH2)〇· 2 -CH3, (9)-(q -c5 alkyl)-〇-(CH2 )〇-2 -CH3, (10)

143482-1 -18- (12) 201111364143482-1 -18- (12) 201111364

其'中(3),⑷,(5),(7),⑻及⑼係視情況被ι_3個鹵素取Its 'zhong (3), (4), (5), (7), (8) and (9) are taken by ι_3 halogens as the case may be

代,且 其中(1〇),(11),(12)及(13)係視情況被1_3個取代基取 代,取代基獨立選自下列組成之組群:鹵素、q -C5烷基、 匸】-<:5烷氧基及氰基, 其中R1,R2,R3,X及(Z)n丨均如式I中所述。 於另一項具體實施例中,本發明係提供式I化合物或其藥 學上可接受之鹽或其光學異構物,其中γ係選自下列組成 之組群:And wherein (1〇), (11), (12) and (13) are optionally substituted by 1 to 3 substituents, the substituents being independently selected from the group consisting of halogen, q-C5 alkyl, hydrazine 】-<:5 alkoxy and cyano, wherein R1, R2, R3, X and (Z)n丨 are as described in formula I. In another embodiment, the invention provides a compound of formula I, or a pharmaceutically acceptable salt thereof, or an optical isomer thereof, wherein the gamma is selected from the group consisting of:

視情况經單-、二-、三-、四-或五取代,如上文式I中所述。 143482-1 19 201111364 於另-項具體實施例中,本發明係提供具有下列化 之下,】列式1化合物或其藥學上可接受之鹽或其光學異構:勿 riSubstituted by mono-, di-, tri-, tetra- or penta, as described above in Formula I. 143482-1 19 201111364 In another embodiment, the present invention provides a compound of the formula 1 or a pharmaceutically acceptable salt thereof or an optical isomer thereof:

R RR R

其中A係選自下列組成之組群: ⑴氫,Wherein A is selected from the group consisting of: (1) hydrogen,

(2) ii 素, ⑶C〗-C5烧基, ⑷q-Cs烷氧基, ⑶氰基, ⑹Ci-cv氰基, ⑺-(C】-c5 伸烷基)-N(H)-C(=0)-(CH2 )〇 - 2 -CH3, ⑻-(q -C5 伸烷基)-〇-(CH2 )〇. 2 -CH3,及 143482-1 •20- 201111364 ⑼-NCHHCi -c5 伸烷基)-〇_(Ch2 2 _CH3, 其中(3),(4),⑹,(7),⑻及⑼係視情況被μ3個_素取 代,且 其中R1,R2,R3,Χ及(Ζ)η 1均如上文式I中所述。 於另一項具體貫施例中,本發明係提供式丨化合物或其藥 學上可接受之鹽或其光學異構物,其中¥係(2) ii, (3) C--C5 alkyl, (4) q-Cs alkoxy, (3) cyano, (6) Ci-cv cyano, (7)-(C)-c5 alkyl)-N(H)-C(= 0)-(CH2)〇- 2 -CH3, (8)-(q-C5 alkylene)-〇-(CH2)〇. 2 -CH3, and 143482-1 •20- 201111364 (9)-NCHHCi -c5 alkylene )-〇_(Ch2 2 _CH3, where (3), (4), (6), (7), (8) and (9) are replaced by μ3 _ primes, and wherein R1, R2, R3, Χ and (Ζ) η 1 is as described in the above formula I. In another specific embodiment, the present invention provides a hydrazine compound or a pharmaceutically acceptable salt thereof or an optical isomer thereof, wherein

視情況經單-或二取代,如上文關於式〗所述。 於另一項具體實施例中,本發明係提供下列式I化合物或 其藥學上可接受之鹽或其光學異構物,其係為It is mono- or di-substituted as appropriate, as described above with respect to Formula. In another embodiment, the invention provides a compound of formula I or a pharmaceutically acceptable salt thereof, or an optical isomer thereof, which is

其中: Α係選自下列組成之組群: ⑴氫, (2) 鹵素, (3) C] -C5 烧基, (4) 烷氧基,及 (5) -(q -C5 伸烷基)-〇_(CH2 )〇 _ 2 -CH3, 其中(3),(4)及(5)係視情況被1-3個卤素取代,真 B係選自下列組成之組群: 143482-1 •21 - 201111364 ⑴氫, ⑵齒素, (3) CVC5烷基, (4) (^-(:5烷氧基, (5) -(C丨-C5 伸烷基)-0-(CH2 )〇. 2 -CH3,及 (6) -NOHMq -C5 伸烷基)-0-(CH2 )〇 _ 2 -CH3, 其中(3),⑷,(5)及⑹係視情況被1-3個齒素取代,且 其中R1,R2,R3,X及(Z)n!均如上文式I中所述。 本發明亦關於式I之結晶形式。在特定具體實施例中,本 發明係關於被定義為(3S,4R)-N-({3-漠基-4-曱基_5_[3-(曱氧基) 丙基]苯基}曱基)-N-環丙基-4-(1-曱基-2-酮基-i,2-二氫-4-吡啶 基)-3-六氫ρ比咬缓醯胺鹽酸鹽之結晶形式〗或其藥學上可接 受之水合物。在其他具體實施例中,本發明係關於式丨之結 晶形式(例如上文所述之形式〗),其係藉*13CSSNMR被特 徵鑒定為具有化學位移吸收峰,具有至少一或多個以每百 萬份之份數表示之下列化學位移:12〇丄31 2,17丄43 5, 41 6, 29.4, 58.5, 71.4, 28.7, 42.5, 138.3 及 143.6。特殊具體實施例係具有 至。'一 一、四、五'六、七、八、九、十或十一個上述 化學位移。其他具體實施例係具有全部12個化學位移。在 其他具體實_巾’本發明係關於式i之結晶形式(例如上 文所述之形式〇 ’其特徵為圖2之固態13C-SSNMR CPMAS核 磁共振光6香。在其他具體實施例中,本發明係關於式I之結 晶形式(例如上文所述之形式〗),其特徵為圖3之熱重分析 曲線。在其他具體實施例中,本發明係關於式I之結晶形式 143482-1 -22- 201111364 (例如上文所述之形式Ϊ),其特徵為圖4之示差掃描卡計法 曲線°在其他具體實施例中,本發明係關於式I之結晶形式 (例如上文所述之形式I) ’其係藉由X射線粉末繞射被特徵 赛定為具有一或多個相應於d-間距之下列反射:10.59,7,04, 4.24, 4.22, 3.88, 3.58’ 3.51,3.31 及 3.08。特殊具體實施例係具有 至夕、 —四、五、六、七、八、九、十或Η—個上述 反射。其他具體實施例係具有全部九個反射。在其他具體 貫施例中,本發明係關於式I之結晶形式(例如上文所述之 形式I),其特徵為圖5之X-射線繞射圖樣。 上文式I化合物及其藥學上可接受之鹽係為腎素抑制劑。 4化口物可用於抑制腎素,及治療譬如高血壓之症狀。 對式(I)化合物之任何指稱,應明瞭亦指稱此種化合物之 光學上純對掌異構物,對掌異構物之混合物,譬如外消旋 物,非對映異構物,非對映異構物之混合物’非對映異構 外消旋物、,非對映異構外消旋物之混合物,内消旋形式, 以及孤(尤其是藥學上可接受之鹽)與溶劑合物(包括水合 物)’及形態學形式,按適t與權宜方式。本發明係涵蓋所 t :W合物係以本質上已知之方式分離,例如藉 官柱層析法、镇爲麻k ,g曰析法(TLC)、高性能液相層析法(hplc) 或結晶化作用0太欲 本發明化合物可具有對掌中心,例如-個 對掌中心(提供兩種 粗異構物,⑻與⑶)或兩個對掌中心 (徒供至向四種立駚 發明包括所右 (R,R)、(S,S)、(R,W,R))。本 二斤有此等光學異構物及其混合物。除非另有明確 0 則對一種異構物之指稱係適用於任何可能之里 143482-1 -23- 201111364 構物。無論何時未指定異構物組成’例如當對於對掌性舻 之鍵結係被描繪為直線時,應明瞭的是,係表示該: 碳之㈣㈣態兩者’及因此是兩種對掌異構物及其混合 此外’具有碳-碳雙鍵之化合物可以Z-與E-形式存在’其 中該化合物之所有異構形式均被包含在本發明中。 〃 本發明化合物亦包括亞硝化之式(I)化合物,其已經過一 或多個位置譬如氧(經基縮合)、硫(氫硫基縮幻及/或= 被亞硝化。本發明之亞硝化化合物可使用熟諳此藝者已知 之習用方法製備。例如,關於使化合物亞;E肖化之已知方法 係描述於美國專利 5,38〇,758, 5,7〇3 〇73, 5 994,294, 632 432 及 6,218,4Π ; W0 规9672 ;及 〇此等人,〇租 prep : 165-198 (1983)中。 鹽類在特殊具體實施例中係為式(1)化合物之藥學上可接 受鹽。措辭"㈣上可接受之鹽"係涵蓋與無機酸類或有機 酸類之鹽’該酸類例如鹽酸、氫溴酸、氫碘酸、硫酸、胺 基石黃酸、峨酸、石肖酸、亞磷酸、亞錢、棒樣酸、甲酸、 :酸、草酸、順丁稀二酸、乳酸、酒石酸、反丁烯二酸' 本甲酸、苯乙醇酸、桂皮酸、棕櫚酸、硬脂酸、麩胺酸、 天門冬胺酸、甲烷磺酸、乙烷磺酸、乙烷二磺酸、對-甲苯 嶒酸、柳酸、琥珀酸、三氟醋酸等,其對有生命之生物體 為無t性,或在式(I)化合物於本性上為酸性之情況下,係 為與無機鹼之鹽,該無機鹼例如鹼金屬或鹼土金屬鹼,例 如氫氧化鈉、氫氧化鉀、氫氧化鈣等。關於藥學上可接受 143482-1 -24- 201111364 鹽之其他實例’可特別參考,,驗性藥物 尸Awm. (1986),33, 201-217。 伴,·, 亦包括充作前體藥物之式τ化合物之衍生物。此等 則體樂物,在對病患投藥後’係於身體中,藉由正常代謝 過私被轉化成幻化合物。此種前體藥物包括會展現增強之 用率、組織專—性及/或細胞傳輸,以改良式ι化合 物之樂物吸收作料。此種前體藥物之作用可由於物理化Wherein: the lanthanide is selected from the group consisting of: (1) hydrogen, (2) halogen, (3) C]-C5 alkyl, (4) alkoxy, and (5) - (q -C5 alkyl) -〇_(CH2)〇_ 2 -CH3, wherein (3), (4) and (5) are replaced by 1-3 halogens as appropriate, and true B is selected from the group consisting of: 143482-1 • 21 - 201111364 (1) Hydrogen, (2) dentate, (3) CVC5 alkyl, (4) (^-(:5 alkoxy, (5) -(C丨-C5 alkyl)-0-(CH2)〇 . 2 -CH3, and (6) -NOHMq -C5 alkylene)-0-(CH2 )〇_ 2 -CH3, wherein (3), (4), (5) and (6) are 1-3 teeth depending on the situation. Substituted, and wherein R1, R2, R3, X and (Z)n! are as described above in Formula I. The invention also relates to the crystalline form of Formula I. In particular embodiments, the invention is defined (3S,4R)-N-({3-Molyl-4-indenyl_5_[3-(indolyl)propyl]phenyl}indolyl)-N-cyclopropyl-4-(1 - fluorenyl-2-keto-i,2-dihydro-4-pyridyl)-3-hexahydrop-pyrase as a crystalline form of the chitosan hydrochloride or a pharmaceutically acceptable hydrate thereof. In other specific embodiments, the invention relates to a crystalline form of the formula (example) The form as described above, which is characterized by *13 CSS NMR as having a chemical shift absorption peak, having at least one or more of the following chemical shifts expressed in parts per million: 12〇丄31 2, 17丄43 5, 41 6, 29.4, 58.5, 71.4, 28.7, 42.5, 138.3 and 143.6. Specific embodiments have to. 'One, four, five 'six, seven, eight, nine, ten or eleven The above chemical shifts. Other embodiments have all 12 chemical shifts. In other embodiments, the invention relates to a crystalline form of formula i (such as the form described above) which is characterized by the solid state of Figure 2. 13C-SSNMR CPMAS Nuclear Magnetic Resonance Light 6. In other specific embodiments, the invention relates to a crystalline form of Formula I (such as the form described above), which is characterized by the thermogravimetric analysis curve of Figure 3. In a specific embodiment, the present invention is directed to the crystalline form 143482-1 -22-201111364 of Formula I (such as the form 上文 described above), which is characterized by the differential scanning card gauge curve of FIG. 4 in other specific embodiments. The present invention relates to a crystalline form of Formula I (eg, The form I) 'is characterized by X-ray powder diffraction as having one or more of the following reflections corresponding to d-spacing: 10.59, 7, 04, 4.24, 4.22, 3.88, 3.58' 3.51 , 3.31 and 3.08. Particular embodiments have the above-described reflections of up to, - four, five, six, seven, eight, nine, ten or ten. Other embodiments have all nine reflections. In other specific embodiments, the invention is directed to a crystalline form of Formula I (e.g., Form I as described above) characterized by the X-ray diffraction pattern of Figure 5. The compound of formula I above, and pharmaceutically acceptable salts thereof, are renin inhibitors. 4 mouth can be used to inhibit renin, and to treat symptoms such as high blood pressure. Any reference to a compound of formula (I) shall be understood to also refer to the optically pure palmar isomer of such a compound, a mixture of palmomers, such as racemates, diastereomers, non-pairs a mixture of enantiomers, a diastereomeric racemate, a mixture of diastereomeric racemates, a meso form, and an orphan (especially a pharmaceutically acceptable salt) in combination with a solvent (including hydrates)' and morphological forms, in accordance with the appropriate t and expedient means. The present invention encompasses that the t:W compound is isolated in a manner known per se, such as by column chromatography, town k, g decantation (TLC), high performance liquid chromatography (hplc). Or crystallization 0 too. The compound of the present invention may have a center of the palm, for example, a pair of palm centers (providing two crude isomers, (8) and (3)) or two pairs of palm centers. The invention includes the right (R, R), (S, S), (R, W, R)). The two kilograms have such optical isomers and mixtures thereof. Unless otherwise specified 0, the reference to an isomer is applicable to any possible 143482-1 -23- 201111364 structure. Whenever the isomer composition is not specified 'for example, when the bond system for the palm of the hand is depicted as a straight line, it should be understood that the system indicates that: the carbon (four) (four) states are both 'and therefore two Structures and mixtures thereof In addition, 'compounds having a carbon-carbon double bond may exist in the Z- and E-forms' wherein all isomeric forms of the compound are included in the present invention. 〃 The compounds of the invention also include nitrosated compounds of formula (I) which have been subjected to one or more positions such as oxygen (transcondensation via a base), sulfur (hydrosulfide-based and/or = nitrosated). Nitrifying compounds can be prepared by conventional methods known to those skilled in the art. For example, the known methods for making compounds sub-E are described in U.S. Patent Nos. 5,38,758, 5,7, 3, 7, 73, 994, 294. , 632 432 and 6,218,4Π; W0 reg. 9672; and 〇 人 pre pre pre pp 165-198 (1983). Salts in a particular embodiment are pharmaceutically acceptable compounds of formula (1) Salt. The word "(4) acceptable salt" encompasses salts with inorganic acids or organic acids such as hydrochloric acid, hydrobromic acid, hydroiodic acid, sulfuric acid, aminic acid, citric acid, tartaric acid. , phosphite, arsenic, bar acid, formic acid, acid, oxalic acid, cis-succinic acid, lactic acid, tartaric acid, fumaric acid, benzate, phenylglycolic acid, cinnamic acid, palmitic acid, stearic acid , glutamic acid, aspartic acid, methanesulfonic acid, ethanesulfonic acid, ethane disulfonic acid, p-toluene Acid, salicylic acid, succinic acid, trifluoroacetic acid, etc., which are not t-sexual to living organisms, or in the case where the compound of formula (I) is acidic in nature, is a salt with an inorganic base, Inorganic bases such as alkali metal or alkaline earth metal bases, such as sodium hydroxide, potassium hydroxide, calcium hydroxide, etc. Other examples of pharmaceutically acceptable 143482-1 -24-201111364 salts can be specifically referred to, test drug colonies Awm. (1986), 33, 201-217. Companion, ·, also includes derivatives of τ compounds that are used as prodrugs. These body music are 'lined in the body after administration to the patient. It is converted into a phantom compound by normal metabolism. This prodrug includes a substance that exhibits enhanced use, tissue specificity, and/or cell transport to improve the absorption of the compound of the formula. The role of drugs can be due to physicalization

學之改變所造成’譬如親脂性、分子量、電荷及其他 測疋藥物滲透性質之物理化學性質。 於前文幻中及後文所使用之—般術語,在本揭示内容 係具有下述意義’除非另有指明。在對化合物、鹽、 醫樂組合物、疾病等使用複數形式之情況下,其亦意謂單 一化合物、鹽等。 ,,除非另有指明,否則m,單獨或與其他基團合 併,係意謂具有-至六個碳原子之飽和、直鍵及分枝鍵基 團。、可以Cl·6烷基或Ά烷基"表示)。當所意欲之意義 為此項日寺命j如當碳原子數係在一至四個碳原子之範圍 内時’此意義係以類似方式’以” Ci4烷基”或"c】_c4烷基" 表示。烷基之實例為甲基、乙基、正·丙基、異丙基正_ 丁基、異丁基、第二-丁基、第三_丁基、戊基、己基及庚基。 甲基、乙基及異丙基健使詩本文特殊具體實施例中。 化合物之結構描繪可以"_CH3 ,,、,,CH3 ”、"_Me”、,,Me„或”卜,, (^即此等具有相當之意義)顯示末端甲基。末端乙基可被 描繪為 ”-CH2CH3"、”CH2CH3,,' "_Et"、”Et"或"卜(意即此等 143482-1 •25· 201111364 具有相當之意義)。 伸烷基” 一詞係指任何二價線性或分枝鏈脂族烴基,具 有在所指定範圍内之碳原子數。因此,例如"_Ci<:6伸烷基 係私任何q至C:6線性或分枝狀伸烷基,而„_Ci 伸烷基」, 2私任何q至q線性或分枝狀伸烷基。關於本發明,特別 令人感興趣之-種伸烧基為仰2)16_,且特別令人感興趣 之亞組包括-(CH2)h-、_(CH2)1 3_、_(CH2)卜 2 及 _CH2_。吾人 感興趣之另一亞組為伸烷基,選自下列組成之組群: 2 CH(CH3 及-C(CH3 )2 -。一些措辭,譬如"C, -c4伸烷美 -笨基"與”被苯基取代之 1 4_烷基 土 π π n, Uj烷基,係具有相同意義,且 可交換使用。 π非另有指明 极 * Τ -叫%六六他悉圈. 個二、思、明具有二至六個碳原子之不飽和(意即具有至少 ^建)直鍵與分枝鏈基團(其可以,,c2 6稀基,,或,,C2 C6烯基 Θ所意奴之意義不為此項時’例如當碳原子數係一 :四個碳原子之範圍内時’此意義係以 稀基,,或,,C2-C4烯基"表示。 L2 伸縣”—㈣餘何二價線性或分枝鏈㈣單不心 二土,具有在所指定範圍内之碳原子數。 除非另有指明,否則•丨炔其” _ Μ 。。 併,俜咅相1亡 、土 3,早獨或與其他基團4 個^^有二至六個碳原子之不飽和(意即具有至少_ 在二至。:所意欲之意義不為此項時,例如當碳原子畫“ -四個碳原子之範圍内時,此意義係以類似方式” 143482-1 -26- 201111364 Ά·4快基”或”c2-c4块基”表示。 装基”―詞’單獨或與其他基團☆併’係指R-〇-基團, 、 為烷基。烷氧基之實例為曱氧基、乙氡武 異丙氧基、異丁氧基、第二_ 丁氧基及第三^基丙乳基、 A:基:Γ—詞,單獨或與其他基團合併,係指鮮 …基。…基之實例為叫、 2 2、HaCH2CH2CH2-及 CH3CH(OH)-。 中,詞係意謂氟、氣、溴或破。在特殊具體實施例 或氣 鼠、氯或漠。在特定具體實施例中,函素為氣 人:'另!指明,否則,’環烧基”-詞,單獨或與其他基團 二有3至8個碳原子之飽和環狀烴環系統,例 Α二r、^丁基、環戊基、環己基、環庚基及環辛基。 義:C3’8%烧基或”c3_q環院基’·表示。當所意欲之意 =此項時’例如當碳原子數係在三至六個碳原子之範 机卷表不。 除非二有指出’否則於本文中使用之"碳環,,(及其變型, ;料族%V’碳環基")_詞,係指cjq單環狀飽和或 匕和環。碳環可在任何碳原子上連接至分子之其餘部份, =造成安定化合物。飽和《族環亦被稱為環烧基環, 例如環丙基、環丁基等。 於本文中使用之”單環”(及其變型,譬如’,單環狀”)一詞 系指I-環,其可被-或多個如本文中所述之取代基取代 143482-1 -27- 201111364 或為未經_取代。 ”雜環,,(及其變型,譬如"雜環族"或,,雜環基,,)一詞係廣 義也私稱女疋4-至8-員飽和或不飽和單環狀環,其含有—或 夕個選自N、〇及S之雜原子(例如丨至6個雜原子或1至4個 雜原子),及其餘為碳原子(典型上為至少一個碳原子);其 中任-個或多個氮與硫雜原子係視情況被氧化,且任—個 或^固氮雜原子係視情況被四級化。除非另有指明,否則 =料被連接在任何雜原子或碳原子上,其條件是連接會 :文疋’”。構之產生。除非另有指明’否則當雜環具有取 4、土時’應明瞭的是取代基可被連接至環中之任何原 無^原子或碳原子,其條件是會造成安定化學結構: 在詞,單獨或併用,係關於苯基、苯基或氣印基。 體貫施例中,”芳基”為苯基。縮寫’.Ph”表干笨其 ”雜芸茸,,w 仏小本暴。 子之’单獨或併用,係意謂含有-至四個氮原 …八有一至三個氮原子之苯并稠合六員芳 方矢環,含有—貝方 人右㈣ 氮或一個硫原子之五員芳族環· 3有一個氧、-個氮或-個硫原子之笨并稠合五員芳: 含有兩個獨立選自氧、氮及硫之雜原子之貝:, 種環之苯并稠合衍生物;含有三個氮原子之及此 其苯并祠合衍生物;四唾基環;“基環;環及 種;系統之實例為咬喃基、,塞吩基力各基此 ,基、如林基、異料基、味唾基、^ 1 唾基、異“基、塔呼基”比哇基、,錢、二:;基”塞 苯并違吩基、❹《及4„基。▲ 坐基、 143482-1 -28- 201111364 式i化合物及其藥學上可接受鹽之特殊實例係包括下文 所列示者: 反式-N-環丙基-N-[(2,3-二氣苯基)甲基]-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺(實例1) 反式-N-[{5-氯基-2-[3-(甲氧基)丙基]-4-咐啶基}曱基]-N-環丙 基-4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺(實 例2) 反式-N-({2-氣基-5-[3-(曱氧基)丙基]苯基}曱基)_N-環丙基-4-(1-甲基-2-酮基-1,2-二氩-4-ρ比咬基)-3-六氫说咬缓醢胺(實例3) 反式-N-({2-氯基-5-[2-(曱氧基)乙基]苯基}曱基)·ν_環丙基-4-(1-甲基-2-酮基-1,2-二氫-4-ρ比β定基)-3-六氫(7比咬叛醯胺(實例4) 反式-Ν-環丙基-Ν-({2,3-二氣-5-[3-(曱氧基)丙基]苯基}甲 基)-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡咬羧醯胺 (實例5) 反式-Ν-環丙基-Ν-({2,3-二氣-5-[2-(曱氧基)乙基]苯基}曱 基)-4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺 (實例6) 反式-Ν-環丙基-Ν-({2-曱基-5-[3-(甲氧基)丙基]苯基}曱 基)-4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)_3-六氫吡啶羧醯胺 (實例7) 反式-Ν-環丙基-Ν-({2-曱基-5-[2-(曱氧基)乙基]苯基}曱 基)-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺 (實例8) 反式-Ν-環丙基-Ν-({2,3-二氤-5-[3-(曱氧基)丙基]苯基)曱 143482-1 -29- 201111364 基)-4-(1-曱基-2-酮基-1,2-二氫-4-ρ比咬基)-3-六氫p比咬緩醯胺 (實例9) 反式-Ν-ί哀丙基-4-(1-甲基-2-嗣基-1,2-二氮-4-p比σ定基)_n_({3_ (甲氧基)-5-[3-(曱氧基)丙基]苯基}曱基)-3-六氫P比咬幾^酿胺 (實例10) 反式-N-環丙基-4-(1-曱基-2-酮基-1,2-二氫-4-P比咬基)_ν_({3· {[2-(曱氧基)-乙基]氧基}-5-[3-(曱氧基)丙基]苯基}曱基)_3•六氮 吡啶羧醯胺(實例11) 反式-Ν-環丙基-4-(1-乙基-2-酮基-1,2-二氫-4-ρ比咬基)_n_({3_ {[2-(曱氧基)-乙基]氧基}-5-[3-(甲氧基)丙基]苯基}甲基)_3_六氫 吡啶羧醯胺(實例12) 反式-Ν-環丙基-Ν-({3-{[2-(曱氧基)乙基]氧基卜5-[3-(曱氧基) 丙基]笨基}曱基)-4-(1,5,6-三曱基-2-酮基-1,2-二氫-4-ρ比。定基)-3— 六氫吡啶羧醯胺(實例13) 反式-Ν-環丙基-4-(1-曱基-5-{[(甲氧基)曱基]氧基•酮基 -1,2-二氫-4-吡咬基)-Ν-({3-{[2-(曱氧基)乙基]氧基}-5-[3-(曱氧基) 丙基]苯基}甲基)-3-六氫吡啶羧醯胺(實例14) 反式-Ν-環丙基-Ν·{[2,3-二氣-5-(3-氰基丙基)苯基]曱基卜4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺(實例15) 反式-Ν-{[5-(3-氰基丙基)-2,3-二氟苯基]甲基}-Ν-環丙基-4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺(實例16) 反式-Ν-環丙基-Ν-{[2,3-二氯-5-(4-羥丁基)苯基]曱基}-4-(1-曱 基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺(實例17) 反式-Ν-環丙基-4-(1-甲基_2-酮基-1,2-二氫-4-吡啶基)-Ν-({3- 143482-1 •30- 201111364 [3-(甲氧基)丙基]-1-莕基}甲基)-3-六氫吡啶羧醯胺(實例18) 反式-(2-{3,4-二氣-5-[(環丙基{[4-(1-甲基-2-酮基-1,2-二氫-4-吡 啶基)-3-六氫吡啶基]幾基}胺基)甲基]苯基}乙基)胺基甲酸甲 酯(實例19) 反式-N-壤丙基-4-(1-曱基-2-嗣基-1,2-二風-4-p比°定基)-N-(8-p奎 0林基甲基)-3-六氫ρ比咬緩醯胺(實例20) 反式-N-環丙基-N-(8-異4啉基甲基)-4-(1-甲基-2-酮基-1,2-二 氫-4-吡啶基)-3-六氫吡啶羧醯胺(實例21) 反式-N-環丙基-N-(5-異喳啉基曱基)-4-(1-曱基-2-酮基-1,2-二 氫-4-吡啶基)-3-六氫吡啶羧醯胺(實例22) 反式-N-環丙基-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)-N-(5-喹 啉基曱基)-3-六氫吡啶羧醯胺(實例23) 反式-N-環丙基-N-(l-異喹啉基曱基)-4-(1-曱基-2-酮基-1,2-二 氫-4-吡啶基)-3-六氫吡啶羧醯胺(實例24) 反式-N-環丙基-4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)-N-({2-P-(曱氧基)丙基]-4-喹啉基}甲基)-3-六氫吡啶羧醯胺(實例25) 反式-N-環丙基-4-(1-甲基-2-酮基-1,2-二氩-4-吡啶基)-N-({6-[3-(甲氧基)丙基]-8-p奎啉基}曱基)-3-六氫吡啶羧醯胺(實例26) 反式-N-[(5-溴基-2,3-二氯苯基)曱基]環丙基_4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧酿胺(實例27) 反式-N-({3-氣基-5-[3-(曱氧基)丙基]苯基}甲基)_N-環丙基-4-(1-甲基-2-酮基-1,2-二氩-4-吡啶基)_3-六氫吡啶羧醯胺(實例28) 反式-N-環丙基-4-(1-曱基-2-酮基_ι,2-二氫-4-吡啶基)-Ν-({1-[3-(曱氧基)丙基HH-啕哚-3-基丨甲基)_3_六氫吡啶羧醯胺(實 143482-1 •31 . 201111364 例29) 反式-N-環丙基-N-{[2,3-二氣-5-(2-氰基乙基)苯基]甲基}-4-(l-曱基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺(實例30) 反式-(2-{3,4-二氣-5-[(環丙基{[4-(1-曱基-2-酮基-1,2-二氫-4-吡 啶基)-3-六氫吡啶基]幾基}胺基)曱基]苯基}乙基)胺基曱酸乙 酯(實例31) 反式-N-({3-漠基-5-[3-(甲氧基)丙基]苯基}甲基)_N_環丙基_4_ (1-曱基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺(實例32) 反式-N-環丙基-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)-N-({5-[3-(甲氧基)丙基]-3-聯苯基}曱基)-3-六氫吡啶羧醯胺(實例33) 反式-N-環丙基-4-(1-曱基-2-酮基-1,2-二氫-4-叶1:咬基)-N-{[[3-(曱氧基)丙基]-5-(3-吡啶基)苯基]甲基卜3-六氫吡啶羧醯胺(實 例34) 反式-N-環丙基-N-[(2,3-二氣-5-{[2-(甲氧基)乙基]胺基}笨基) 甲基]-4-(1-甲基-2-酮基-1,2-二氫-4-峨咬基)-3-六氫p比咬叛醯胺 (實例35) 反式-N-環丙基-4-(1-曱基-2-酮基-1,2-二氫-4-ρ比。定基)_N-[(3- {[2-(曱氧基)乙基]胺基}-l-萘基)曱基]-3-六氫峨。定幾醢胺(實 例36) 反式-N-{[6-(2-氰基乙基)-8-p奎'•林基]甲基}-N-環丙基-4-(1-曱 基-2-酮基-1,2-二氫-4-ρ比。定基)-3-六氫p比。定叛醯胺(實例37) 反式-N-環丙基-4-(1-甲基-2-酮基-1,2-二氩-4-p比。定基)_n_({3_ [2-(甲氧基)乙基]-1-莕基}甲基)-3-六氫p比。定叛醯胺(實例38) 反式-N-({3-[2-(乙醯胺基)乙基]-1-茶基}曱基)_N-環丙基斗(1_ 143482-1 •32· 201111364 甲基-2-_基- l,2-二氫-4-ρ比咬基)_3_六氫ρ比咬缓醯胺(實例39) 反式-N-[(2-漠笨基)甲基]_N_環丙基_4-(1-曱基-2-酮基-1,2-二 氫-4-吡啶基)-3-六氫吡啶羧醯胺(實例40) 反式-N-環丙基·4-(1-曱基_2_酮基·ι,2-二氫-4-吡啶基⑼-⑴-[2-(甲氧基)乙基]-1Η-叫丨哚-3-基}曱基)-3-六氫毗啶羧醯胺(實 例41) 反式-Ν-環丙基-4-(1-甲基_2-酮基-1,2-二氫-4-吡咬基)·Ν-{[1-(2,2,2-三氟乙基)-1Η-吲哚_3-基]曱基}-3-六氫吡。定羧醯胺 ® (實例42) 反式-Ν-環丙基-4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)-Ν-{[1-(4,4,4-三氟丁基)-1Η-吲嗓-3-基]曱基}-3-六氫口比咬缓醢胺 (實例43) 反式-N-[(l-丁基-1Η-啕哚-3-基)曱基]-Ν-環丙基-4-(1-甲基-2-酮基二氫-4-吡啶基)-3-六氣吡啶羧醯胺(實例44) 反式-Ν-環丙基-Ν-({1-[3-(乙氧基)丙基]_1Η_吲哚各基}曱 _ 基)-4-(1-曱基酮基-1,2-二氫-4_ρ比。定基)各六氫ρ比。定緩醯胺 (實例45) 反式-Ν-環丙基-4-(1-曱基-2-酮基-1,2-二氫斗吡啶基)-Ν-({1-[3,3,3-三氟-2-(三氟甲基)丙基]-1Η-吲哚-3-基}曱基)_3_六氫吡啶 羧醯胺(實例46) 反式-Ν-({Η3-(乙醯胺基)丙基]-1Η-吲哚_3-基}曱基)_Ν_環丙 基曱基-2-酮基-1,2-二氫斗吡啶基)-3-六氫吡啶羧醯胺(實 例47) 反式-Ν-環丙基-4-(1-甲基-2-酮基-1,2-二氫_4_吡啶基 143482-1 -33· 201111364 [3-(丙醯基胺基)丙基]-ΙΗ-叫丨p朵-3-基}曱基)-3-六氫p比。定叛醢胺 (實例48) 反式-Ν-({1-[2-(乙醯胺基)乙基]-1Η-Η丨嗓-3-基}曱基)·ν_環丙 基-4-(1-甲基-2-酮基-1,2-二氫-4-ρ比。定基)-3-六氫峨。定緩醯胺(實 例49) 反式-Ν-環丙基-4-(1-曱基-2-酮基-1,2-二氫-4-ρ比咬基)-Ν-({ 1-[2-(丙醯基胺基)乙基]-1Η-啕哚-3-基}曱基)-3-六氫吡啶羧醯胺 (實例50) 反式-Ν-環丙基-4-(1-甲基-2-酮基-1,2-二氫·4-Ρ比啶基)-Ν-{[1-(2-丙稀-1-基)-1Η-吲嗓-3-基]曱基}-3-六氫η比咬叛胺(實例51) 反式-N-環丙基-4-(1-甲基-2-酮基-1,2-二氫-4-P比咬基)-Ν-{[1-(苯基甲基丨嗓-3-基]曱基}-3-六氫p比咬叛醯胺(實例52) 反式-N-環丙基-4-(1-曱基-2-酮基-1,2-二氫-4-P比。定基)-Ν-{[1-(2-p比咬基甲基)-1Η-吲嗓-3-基]甲基}-3-六氫吡啶羧醯胺(實例53) 反式-N-環丙基_4-(1_曱基-2-酮基-1,2-二氫-4-吡啶基)-N-{ [1-(3-p比咬基甲基)-1Η-吲哚-3-基]甲基}-3-六氫吡啶羧醯胺(實例54) 反式-N-環丙基·4-(ι_甲基_2_酮基-i,2-二氫_4_吡啶基)-Ν-{[1-(4-对匕°定基甲基)-1Η-吲哚-3-基]甲基}-3-六氫吡啶羧醯胺(實例55) 反式-N-環丙基_n-({1-[(4-氟苯基)曱基]-1H-十朵-3-基}曱基)-4-(1-曱基-2-酮基-i,2-二氫-4-吡啶基)各六氫吡啶羧醯胺(實例 56) 反式-N-({i-[(4-氣苯基)甲基]_1Η_Ρ?|哚各基丨甲基)_N環丙基 -4-(1-曱基-2-酮基·1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺(實例 57) 143482-1 •34· 201111364 反式-N-環丙基-N_(U-[(3_氟苯基)甲基]·1Η叫丨哚_3基}甲基> 4-(1-甲基-2-酮基-U-二氫冰吡啶基)_3_六氫吡啶羧醯胺(實例 58) 反式-Ν-({1-[(3-氯苯基)曱基]_1H-吲哚_3D甲基環丙基 -4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺(實例 59) 反式-Ν-({1-[(3-氰基苯基)曱基]_1H_吲哚_3基)甲基)n環丙 基-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)各六氫吡啶羧醯胺(實 例60) 反式-N-環丙基-4-(1-甲基-2-酮基-u—二氫斗吡啶基)N_ ({H(3-曱基苯基)甲基HH,嗓-3-基}曱基)_3•六氫吡啶羧醯胺 (實例61) 反式-N-環丙基-N-({5-氟基-1-[3-(曱氧基)丙基]_m_十朵_3基} 曱基)-4-(1-甲基-2,基-1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺 (實例62) 反式-N-{[6-溴基-1-(苯基曱基)-iH-吲嗓_3_基]曱基卜N_環丙 基-4-(1-曱基-2-酮基-1,2-二氫-4-吨啶基)各六氫吡啶羧醯胺(實 例63) 反式-N-環丙基-N-UH(3-氟苯基)甲基]_6_(曱氧基)_1Η·Ρ引哚 -3-基]甲基)-4-(1-曱基-2-酮基-1,2-二氫_4_吡啶基)_3_六氫吡啶羧 醯胺(實例64) 反式-Ν-環丙基-4-(1-曱基-2-_基],2_二氫_4^比π定基)_ν_{[4-甲 基-1-(苯基曱基)-1Η-吲哚-3-基]甲基卜3-六氫吡啶羧醯胺(實例 65) 143482-1 •35· 201111364 反式-N-{[4-氰基-1-(苯基曱基)_1H_吲哚各基]曱基卜N_環丙 基_4-α-曱基-2-酮基-1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺(實 例66) 反式-Ν-環丙基-Ν-{[4-氟基-1-(苯基曱基)_爪_吲哚_3_基]甲 基甲基-2-闕基-1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺 (實例67) 反式-Ν-環丙基-Ν-({4-氟基-1-[(3_氟苯基)曱基]_1Η吲哚_3基] 甲基M-(l-甲基-2-綱基-1,2-二氫-4-吡啶基)各六氫吡啶羧醯胺 (實例68) 反式-Ν-環丙基-Ν-({4-氟基-1-[3-(甲氧基)丙基]_1Η吲哚_3_基) 甲基)-4-(1-曱基-2-酮基-1,2-二氫斗吡啶基)各六氫吡啶羧醯胺 (實例69) 反式-Ν-({4-氣基-1-[3-(曱氧基)丙基]_出_吲哚_3基}甲基 環丙基-4-(1-甲基-2-酮基-1,2-二氫斗吡啶基)冬六氫吡啶羧醯 胺(實例70) 反式-N-U4-氣基-1-(笨基甲基)_1Η_吲哚_3基]甲基}_Ν環丙 基斗(1-曱基-2-酮基-1,2-二氫斗吡啶基)_3_六氫吡啶羧醯胺(實 例Ή) 反式-Ν-{[4-溴基-1-(苯基曱基)_此吲哚_3基]甲基卜Ν環丙 基-4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)_3-六氫吡啶羧醯胺(實 例72) 反式-Ν-({4-溴基-1-[(3-氟苯基)曱基ΗΗ•吲哚_3•基}甲基)& 環丙基-4-(1-甲基-2-酮基4,2-二氫-4-吡啶基)_3_六氫吡啶羧醯 胺(實例73) 143482-1 -36· 201111364 反式-N-({〉臭基-1-[3-(甲氧基)丙基HH-啕哚-3-基}曱基)-N-環 丙基-4-(1-甲基_2-酮基4,2_二氫_冬吡啶基)_3_六氫吡啶羧醯胺 (實例74) 反式-N_環丙基-Ν·[(4-氟基-1H-啕哚-3-基)甲基]-4-(1-甲基-2-_基-1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺(實例75) 反式-Ν-ί辰丙基_N_{[4_氟基小(3_吡啶基甲基)_1H-啕哚_3基] 曱基}-4-(1-甲基-2-酮基-i,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺 (實例76) ® 反式-N-環丙基-N-{[4-氟基-1-(4-吡啶基甲基)_ih-W哚-3-基] 曱基}-4-(1-甲基-2-酮基-1,2-二氳-4-吡啶基)-3-六氫吡啶羧醯胺 (實例77) 反式-N-({3-乙醯基-5-[3-(曱氧基)丙基]苯基}甲基)-N-環丙基 -4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺(實例 78) 反式-N-({1,3-雙[3-(甲氧基)丙基]-2,4-二酮基-1,2,3,4-四氫-5-嘧 ^ 啶基}甲基)-N-環丙基-4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺(實例79) 反式-N-環丙基-N-({2,3-二甲基-5-[3-(甲氧基)丙基]苯基}甲 基)-4-(1-曱基-2-酮基-1,2-二氫冬被°定基)-3-六氫p比。定叛醯胺 (實例80) 反式-N-[(2-氣基-5-{[2-(曱乳基)乙基]乳基}苯基)曱基]-N-環 丙基_4-(1_甲基-2-S同基-1,2-·鼠σ疋基)-3-六氮p比。定叛酿胺 (實例81) 反式_Ν-環丙基-4-(1·甲基酮基_1,2- —虱-4-ρ比。定基)-Ν-(2-各 143482-1 -37- 201111364 基曱基)-3-六氫吡啶羧醯胺(實例82) 反式-N-環丙基-4-(1-曱基-2-酮基-1,2-二氫-4-p比咬基)_n_({3-[(三氟曱基)硫基]苯基丨甲基)-3-六氫吡啶羧醯胺(實例83) 反式-N-環丙基-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基 (甲氧基)丙基]-2-(曱硫基)苯基]甲基}-3-六氫p比。定敌醯胺(實 例84) 反式-N-({3-溴基-4-甲基-5-[3-(甲氧基)丙基]苯基}甲基)環 丙基-4-(1-曱基-2-酮基-1,2-二氫-4-ρ比咬基)-3-六氫p比咬緩酿胺 (實例85) # 反式-N-[3,5-雙(3-曱氧基丙基)卞基]-N-環丙基-4-(1-甲基_2_酉同 基二氫-4-p比咬基)-3-六氫p比咬緩gi胺(實例86) 反式-N-環丙基-N-[3-(3-甲氧基丙基)-5-曱芊基]-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)各六氫吡啶羧醯胺(實例87) 反式-N-[2-漠基-3,5-雙(3-甲氧基丙基)亨基]-N-環丙基_4-(1_曱 基-2-酮基-1,2-二氫-4-p比咬基)-3-六氫峨咬叛醯胺(實例88) 反式-N-[2-氣基-3,5-雙(3-曱氧基丙基)爷基]_N_環丙基斗(1_曱 基-2-酮基-1,2-二氫-4-P比咬基)_3-六氫?比D定叛醯胺(實例89) ® 反式-N-環丙基_n_[2-甲氧基-3,5-雙(3-甲氧基丙基)爷基]-4-(1-甲基-2-酮基-1,2-二氫冰吡啶基)·3-六氫吡啶羧醯胺(實例9〇) 反式-N-環丙基-N_[3_(3_甲氧基丙基)_5_(三氟曱基)节基]_4_(1_ 甲基-2-酮基-1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺(實例91) 反式-N-環丙基_N_[3_羥基_5·(3甲氧基丙基)节基]_4 (1甲基 -2-酮基-1’2-一氫-4-吡啶基)_3-六氫吡啶羧醯胺(實例92) 反式-Ν-(3-苯甲醯基_5_溴基芊基環丙基_4 (1甲基_2_酮 143482-1 •38- 201111364 基-1’2-二氫-H定基)-3-六氫峨σ定竣醯胺(實例93) 反式-N-{3-溴基-5-[(1Ε)-3-曱氧基小丙烯小基]字基卜N•環丙 基-4-(1-曱基-2-酮基-1,2-二氫斗吡啶基)_3_六氫吡啶羧醯胺(實 例94) 反式-N-{3-溴基-5-[(2-羥乙基)硫基]爷基}善環丙基冰(1_曱 基-2-酮基-1,2-二氫-4-P比啶基)_3_六氫吡咬羧醯胺(實例95) 反式-N-環丙基-N-[3-[2-(環丙基氧基)乙氧基>5_(3_曱氧基丙 基)爷基]-4-(1-甲基-2-酮基-l,2-二氫_4-吡啶基)各六氫吡啶羧醯 胺(實例96) 反式-N-環丙基-N-{3-(3-甲氧基丙基)_5_[2_(4_嗎福啉基)乙氧 基]节基}-4-(1-甲基-2-酮基-i,2-二氫_4-吡啶基)-3-六氫吡啶缓 醯胺(實例97) 反式-3-[(環丙基{[4-(1-曱基_2·酮基二氫_4_吡啶基)3六 氫吡啶基]羰基丨胺基)甲基]-5-(3-甲氧基丙基)苯基4-嗎福啉羧 酸酯(實例98) 反式-N-環丙基-N-[6-(3-甲氧基丙基)_2,3_二氫-1H-雖-1-基]_4_ (1-曱基-2-酮基-1,2-二氫-4-p比咬基)_3_六氫?比咬缓酸胺(實例99) 反式-N-環丙基-N-[7-(3-曱氧基丙基)_ι,2,3,4-四氫-1-茶基]-4-(1-曱基-2-酮基-1,2-二氫-4-吡咬基)-3-六氫吡咬羧醯胺(實例 100) 反式-N-[3-溴基-5-(3-羥丙基)-4-曱苄基]-N-環丙基-4-(1-甲基 -2-酮基-1,2-二氫-4-?比α定基)-3-六氫p比咬緩醯胺(實例1〇].) 反式-Ν-[3-溴基-5-(3-乙氧基丙基)-4-曱芊基]-Ν-環丙基-4-(1-甲基-2-酮基-1,2-二氫-4-ρ比。定基)-3-六氫ρ比υ定缓醯胺(實例1〇2) 143482-1 -39- 201111364 反式-N-{3-溴基-5-[3-(二氟曱氧基)丙基]_4_曱芊基ρΝ_環丙 基-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺(實 例 103) 反式-Ν-(3-字基-5-甲芊基)_Ν_環丙基冰(1_甲基_2_酮基^ 氫-4-吡咬基)-3-六氫p比咬羧醯胺(實例1〇4) 反式-N-[3-漠基-5-(3-氟芊基)_4_曱苄基]_N_環丙基_4-(l-曱基 -2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺(實例1〇5) 反式-N-[3-溴基-5-(3-氟苯曱醯基)_4-曱芊基]_Ν·環丙基冬(1_ 曱基-2-酮基-1,2-二風-4-ρ比。定基)-3-六氫?比D定緩醯胺(實例1〇6) 反式-N-{3-溴基-5-[(3-氟苯基)(羥基)曱基]_4_曱苄基}_N_環丙 基-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺(實 例 107) 反式-N-[2-氣基-5-(2-曱氧基乙基)节基]環丙基_4_羥基_4_ (1-曱基-2-酮基-1,2-二氫-4-p比咬基)-3-六氫?比π定叛g篮胺(實例 108) 反式-N-[2-氣基-5-(2-甲氧基乙基)节基]_n_環丙基_4_曱氧基 -4-(1-甲基-2-酮基-1,2-二氫-4-ρ比咬基)-3-六氫p比咬緩酸胺(實例 109) 反式-N-環丙基-4-羥基-N-[3-(2-曱氧基乙氧基)_5_(3_曱氧基 丙基)辛基]-4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)各六氫吡啶缓 醯胺(實例110) 反式-N-環丙基-4-曱氧基-N-[3-(2-甲氧基乙氧基)_5_(3_甲氧 基丙基)亨基]-4-(1-曱基-2-酮基-l,2-二氫-4-?比。定基)_3_六氫P比咬 羧醯胺(實例111) 143482-1 -40- 201111364 本發明亦涵蓋一種醫藥配方,其包含藥學上可接受之載 劑與式I化合物或其藥學上可接受之結晶形式或水合物。特 定具體實施例為式I化合物之醫藥組合物,其係另外包含第 二種藥劑。 縮寫之清單: BINAP 2,2’-雙(二苯基膦基)-1,Γ-聯莕 BOC 第三-丁氧羰基 BSA 牛血清白蛋白 _ COD 1,5-環辛二烯 DBU 1,8-二氮雙環并[5.4.0]十一 -7-稀 DCM 二氣曱烷 DIBA1-H 氫化二異丁基鋁 DMAP 4-二甲胺基吡啶 DME 1,2-二曱氧基乙烷 DMF Ν,Ν-二曱基曱醯胺 • DMP Dess-Martin 過換烧 DMSO 二曱亞石風 DPPB 1,4-雙(二笨基膦基)丁烷 DPPF 1,Γ-雙(二苯基膦基)二環戊二烯鐵 EDTA 乙二胺四醋酸 EIA 酶免疫檢測 Et20 乙 EtOAc 醋酸乙酯 HATU 六氟磷酸〇-(7-氮苯并三唑-1-基)-Ν,Ν,Ν',Ν’-四曱基錁 143482-1 -41 - 201111364The physicochemical properties resulting from changes in the properties such as lipophilicity, molecular weight, charge, and other infiltration properties of the test drug. The general terms used in the previous illusions and the following texts have the following meanings in the present disclosure unless otherwise indicated. In the case of using a plural form for a compound, a salt, a medical composition, a disease, or the like, it also means a single compound, a salt or the like. , unless otherwise indicated, m, alone or in combination with other groups, means saturated, straight-bonded, and branched bond groups having from - to six carbon atoms. It can be represented by Cl·6 alkyl or decyl ". When the intended meaning is this Japanese temple, such as when the number of carbon atoms is in the range of one to four carbon atoms, 'this meaning is similar to 'Ci4 alkyl' or "c]_c4 alkyl " said. Examples of alkyl groups are methyl, ethyl, n-propyl, isopropyl-n-butyl, isobutyl, second-butyl, tert-butyl, pentyl, hexyl and heptyl. Methyl, ethyl and isopropyl groups are described in this particular embodiment. The structure of the compound can be characterized by "_CH3,,,,,CH3", "_Me",,,Me, or "b," (where ^ is equivalent) to display the terminal methyl group. The terminal ethyl group can be described as "-CH2CH3", "CH2CH3,, ' "_Et", "Et" or " (meaning that these 143482-1 •25·201111364 have considerable significance). The term refers to any divalent linear or branched chain aliphatic hydrocarbon group having a number of carbon atoms within the specified range. Thus, for example, "_Ci<:6 alkylene is any q to C:6 linear or branched alkyl, and „_Ci alkyl”, 2 private q to q linear or branched alkyl base. With regard to the present invention, a particularly interesting type of excipient is 2) 16_, and a particularly interesting subgroup includes -(CH2)h-, _(CH2)1 3_, _(CH2) 2 and _CH2_. Another subgroup of interest to us is an alkylene group selected from the group consisting of: 2 CH(CH3 and -C(CH3)2 -. Some words, such as "C, -c4 alkylene-styl "and the 1-4 π-alkyl π π n, Uj alkyl substituted by phenyl, have the same meaning, and can be used interchangeably. π does not specify the pole * Τ - called % six or six. Two, two or six carbon atoms are unsaturated (meaning having at least one) direct bond and branched chain groups (which can, c2 6 dilute, or, C2 C6 alkenyl) The meaning of Θ 奴 slave is not the case when 'for example, when the number of carbon atoms is one: four carbon atoms', this meaning is represented by a dilute base, or, C2-C4 alkenyl.伸县"—(4) Yu Di valence linear or branched chain (4) Single unconstrained soil, with the number of carbon atoms within the specified range. Unless otherwise specified, 丨 alkyne" _ Μ 。 。咅 phase 1 death, soil 3, early alone or with other groups 4 ^ ^ have two to six carbon atoms of unsaturated (meaning that there is at least _ in two to.: the intended meaning is not this, For example when carbon atoms are drawn - In the case of - four carbon atoms, this meaning is expressed in a similar manner "143482-1 -26- 201111364 Ά·4 fast base" or "c2-c4 block base". Mounting "" word alone or with other The group ☆ and 'refers to the R-〇- group, and is an alkyl group. Examples of the alkoxy group are a decyloxy group, an oxime isopropoxy group, an isobutoxy group, a second _butoxy group and the first Trisylpropionyl, A:yl: Γ-word, alone or in combination with other groups, means fresh base. Examples of bases are, 2, HaCH2CH2CH2- and CH3CH(OH)-. The word system means fluorine, gas, bromine or broken. In a specific embodiment or gas rat, chlorine or desert. In a specific embodiment, the element is gas: 'other! indicate, otherwise, 'ring-burning base' a word, a saturated cyclic hydrocarbon ring system having 3 to 8 carbon atoms, alone or in combination with other groups, such as ruthenium, butyl, cyclopentyl, cyclohexyl, cycloheptyl and cyclooctyl. : C3 '8% burnt base or "c3_q ring yard base" · expressed. When the intended meaning = this item 'for example, when the number of carbon atoms is in the range of three to six carbon atoms, the machine does not. Point out 'otherwise in this article The use of "carbocycle,, (and its variants; ; family %V'carbocyclyl")_, means cjq monocyclic saturated or oxime and ring. The carbocyclic ring can be attached to any carbon atom to The rest of the molecule, = causing a stable compound. Saturated "family ring is also known as a cycloalkyl ring, such as cyclopropyl, cyclobutyl, etc. As used herein, "monocyclic" (and its variants, such as ' The term "monocyclic" refers to an I-ring which may be substituted by - or a plurality of substituents as described herein 143482-1 -27- 201111364 or may be unsubstituted. "Heterocycle,, (and its variants, such as "heterocyclic" or "heterocyclyl,") is a broad term also known as a female 疋4- to 8-membered saturated or unsaturated monocyclic ring. , which contains - or a hetero atom selected from N, hydrazine and S (for example, to 6 heteroatoms or 1 to 4 heteroatoms), and the remainder being a carbon atom (typically at least one carbon atom); Any one or more of the nitrogen and sulfur heteroatoms are oxidized as appropriate, and any or a nitrogen-fixing hetero atom is optionally quaternized. Unless otherwise indicated, the material is attached to any heteroatom or carbon. On the atom, the condition is that the connection will be: 疋'. The formation of the structure. Unless otherwise indicated 'otherwise when the heterocyclic ring has taken 4, soil' it is understood that the substituent may be attached to any of the original atoms or carbon atoms in the ring, provided that it will result in a stable chemical structure: Used alone or in combination, with respect to phenyl, phenyl or amphoteric. In the embodiment, the "aryl group" is a phenyl group. The abbreviation '.Ph' table is dull and sloppy. The 'individually or in combination, means that there are - to four nitrogen atoms... eight benzo-fused six-membered aromatic ring of one or three nitrogen atoms, containing - Bayer's right (four) nitrogen or a sulfur atom Aromatic ring 3 has an oxygen, a nitrogen or a sulfur atom stupid and fused five-membered aromatic: a shell containing two heteroatoms independently selected from oxygen, nitrogen and sulfur: a fused derivative; a benzopyrene derivative containing three nitrogen atoms; a tetras-silacyclyl ring; a "base ring; a ring and a species; an example of a system is a thiol group, and a thiophene group , base, such as forest base, heterogeneous base, taste sulphate, ^ 1 sulphate, hetero-yl, tahki, wow, w, ke, ke, ke, ke, ke, ke, ke, ke, ke 4 „基.▲ 坐基, 143482-1 -28- 201111364 Specific examples of the compound of formula i and its pharmaceutically acceptable salts include those listed below: trans-N-cyclopropyl-N-[(2 ,3-diphenylphenyl)methyl]-4-(1-indol-2-one-1,2-dihydro-4-pyridyl)-3-hexahydropyridinecarboxamide (Example 1) trans-N-[{5-Chloro-2-[3-(methoxy)propyl]-4-acridinyl}indenyl]-N-cyclopropyl- 4-(1-Methyl-2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide (Example 2) trans-N-({2- gas-based- 5-[3-(indolyl)propyl]phenyl}indenyl)_N-cyclopropyl-4-(1-methyl-2-keto-1,2-diar-ar--4-p ratio ))-3-hexahydro said biting slow amide (Example 3) trans-N-({2-chloro-5-[2-(decyloxy)ethyl]phenyl}fluorenyl)·ν_ Cyclopropyl-4-(1-methyl-2-keto-1,2-dihydro-4-ρ ratio β-decyl)-3-hexahydro (7-bit retinoylamine (Example 4) trans- Ν-cyclopropyl-hydrazine-({2,3-dioxa-5-[3-(indolyl)propyl]phenyl}methyl)-4-(1-indol-2-yl-- 1,2-dihydro-4-pyridyl)-3-hexahydropyridylcarboxamide (Example 5) trans-Ν-cyclopropyl-Ν-({2,3-digas-5-[2 -(decyloxy)ethyl]phenyl}indolyl-4-(1-methyl-2-keto-1,2-dihydro-4-pyridyl)_3_hexahydropyridine carboxamide ( Example 6) trans-Ν-cyclopropyl-fluorene-({2-mercapto-5-[3-(methoxy)propyl]phenyl}indolyl)-4-(1-methyl-2 -keto-1,2-dihydro-4-pyridyl)_3-hexahydropyridine carboxamide (Example 7) trans-Ν-cyclopropyl-Ν-({2-mercapto-5-[2 -(decyloxy)ethyl]phenyl}indolyl-4-(1-mercapto-2-keto-1,2-dihydro-4- Pyridyl)_3_hexahydropyridine carboxamide (Example 8) trans-Ν-cyclopropyl-fluorene-({2,3-diox-5-[3-(decyloxy)propyl]phenyl )曱143482-1 -29- 201111364 base)-4-(1-mercapto-2-keto-1,2-dihydro-4-ρ ratio octyl)-3-hexahydrop than biting decylamine (Example 9) trans-Ν-ί propyl-4-(1-methyl-2-indolyl-1,2-diaza-4-p ratio σ-based)_n_({3_(methoxy) -5-[3-(decyloxy)propyl]phenyl}indolyl)-3-hexahydro-P is a bit of a chiral amine (Example 10) trans-N-cyclopropyl-4-(1- Mercapto-2-keto-1,2-dihydro-4-P ratio bite)_ν_({3·{[2-(decyloxy)-ethyl]oxy}-5-[3-(曱oxy)propyl]phenyl}indenyl)_3•hexazapyridine carboxamide (Example 11) trans-Ν-cyclopropyl-4-(1-ethyl-2-keto-1,2 -dihydro-4-ρ ratio bite)_n_({3_ {[2-(decyloxy)-ethyl]oxy}-5-[3-(methoxy)propyl]phenyl}methyl _3_ hexahydropyridine carboxamide (Example 12) trans-Ν-cyclopropyl-fluorene-({3-{[2-(decyloxy)ethyl)oxy b-[3-(曱) Oxy) propyl] phenyl} fluorenyl)-4-(1,5,6-tridecyl-2-keto-1,2-dihydro-4-ρ ratio. Benzyl)-3-hexahydropyridine carboxamide (Example 13) trans-Ν-cyclopropyl-4-(1-indolyl-5-{[(methoxy)indolyl]oxy]keto- 1,2-dihydro-4-pyridyl)-indole-({3-{[2-(decyloxy)ethyl)oxy}-5-[3-(decyloxy)propyl]benzene }}methyl)-3-hexahydropyridine carboxamide (Example 14) trans-Ν-cyclopropyl-Ν·{[2,3-dioxa-5-(3-cyanopropyl)phenyl ] 曱基卜 4-(1-methyl-2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide (Example 15) trans-Ν-{[5 -(3-cyanopropyl)-2,3-difluorophenyl]methyl}-indole-cyclopropyl-4-(1-methyl-2-keto-1,2-dihydro-4 -pyridyl)-3-hexahydropyridine carboxamide (Example 16) trans-indole-cyclopropyl-indole-{[2,3-dichloro-5-(4-hydroxybutyl)phenyl]indole }-4-(1-mercapto-2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide (Example 17) trans-hydrazine-cyclopropyl- 4-(1-Methyl-2-keto-1,2-dihydro-4-pyridyl)-indole-({3- 143482-1 •30- 201111364 [3-(methoxy)propyl] -1-mercapto}methyl)-3-hexahydropyridine carboxamide (Example 18) trans-(2-{3,4-digas-5-[(cyclopropyl{[4-(1- Methyl-2-keto-1,2-dihydro-4-pyridyl)-3 - hexahydropyridyl]methyl}amino)methyl]phenyl}ethyl)carbamic acid methyl ester (Example 19) trans-N-Lactylpropyl-4-(1-indolyl-2-indole Base-1,2-two wind-4-p ratio °-based)-N-(8-p-quinoline-methyl)-3-hexahydro-p-butanylamine (Example 20) trans-N- Cyclopropyl-N-(8-iso-4-linylmethyl)-4-(1-methyl-2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridinecarboxylate Amine (Example 21) trans-N-cyclopropyl-N-(5-isoindolyl fluorenyl)-4-(1-indol-2-yl-1,2-dihydro-4-pyridine Benzyl-3-hexahydropyridine carboxamide (Example 22) trans-N-cyclopropyl-4-(1-indol-2-one-1,2-dihydro-4-pyridyl)- N-(5-quinolinylfluorenyl)-3-hexahydropyridine carboxamide (Example 23) trans-N-cyclopropyl-N-(l-isoquinolinylfluorenyl)-4-(1 - mercapto-2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide (Example 24) trans-N-cyclopropyl-4-(1-methyl -2-keto-1,2-dihydro-4-pyridyl)-N-({2-P-(decyloxy)propyl]-4-quinolinyl}methyl)-3-hexahydro Pyridinium Carboxamide (Example 25) trans-N-Cyclopropyl-4-(1-methyl-2-keto-1,2-di-aryl-4-pyridyl)-N-({6-[ 3-(methoxy)propyl]-8-p quinolyl X-yl)-3-hexahydropyridine carboxamide (Example 26) trans-N-[(5-bromo-2,3-dichlorophenyl)indenyl]cyclopropyl_4-(1- Mercapto-2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine Carboxamide (Example 27) trans-N-({3-气基-5-[3- (decyloxy)propyl]phenyl}methyl)_N-cyclopropyl-4-(1-methyl-2-keto-1,2-diar-aryl-4-pyridyl)-3-hexahydropyridine Carboxylamidine (Example 28) trans-N-cyclopropyl-4-(1-indol-2-oneyl-ι,2-dihydro-4-pyridyl)-indole-({1-[3 -(decyloxy)propylHH-indole-3-ylindolemethyl)_3_hexahydropyridinecarboxamide (Im 143482-1 •31 . 201111364 Example 29) trans-N-cyclopropyl-N -{[2,3-dioxa-5-(2-cyanoethyl)phenyl]methyl}-4-(l-nonyl-2-keto-1,2-dihydro-4-pyridine ))-3-hexahydropyridine carboxamide (Example 30) trans-(2-{3,4-dioxa-5-[(cyclopropyl{[4-(1-mercapto-2-)yl) -1,2-dihydro-4-pyridyl)-3-hexahydropyridyl]amino}amino)indenyl]phenyl}ethyl)amino decanoic acid ethyl ester (Example 31) trans-N -({3-Molyl-5-[3-(methoxy)propyl]phenyl}methyl)_N_cyclopropyl_4_(1-indol-2-yl-1,2-di Hydrogen-4-pyridyl)-3-hexahydropyridinecarboxylate Indoleamine (Example 32) trans-N-cyclopropyl-4-(1-indol-2-one-1,2-dihydro-4-pyridyl)-N-({5-[3- (Methoxy)propyl]-3-biphenyl}indenyl)-3-hexahydropyridinecarboxamide (Example 33) trans-N-cyclopropyl-4-(1-indolyl-2- Ketol-1,2-dihydro-4-leaf 1: dimethyl)-N-{[[3-(indolyl)propyl]-5-(3-pyridyl)phenyl]methyl b 3 - hexahydropyridine carboxamide (Example 34) trans-N-cyclopropyl-N-[(2,3-dioxa-5-{[2-(methoxy)ethyl]amino}} ) methyl]-4-(1-methyl-2-keto-1,2-dihydro-4-indole)-3-hexahydrop ratio biting retinoic acid (Example 35) trans-N - cyclopropyl-4-(1-mercapto-2-one-1,2-dihydro-4-p ratio. Stationary)_N-[(3-{[2-(indolyl)ethyl]amino}-l-naphthyl)indolyl]-3-hexahydroindole.醢 醢 ( (Example 36) trans-N-{[6-(2-Cyanoethyl)-8-p-quino-•indolyl]methyl}-N-cyclopropyl-4-(1- Mercapto-2-keto-1,2-dihydro-4-p ratio. Azide)-3-hexahydrop ratio. Detamine (Example 37) trans-N-cyclopropyl-4-(1-methyl-2-keto-1,2-di-argon-4-p ratio. Base)_n_({3_[2 -(Methoxy)ethyl]-1-indenyl}methyl)-3-hexahydrop ratio. Detamine (Example 38) trans-N-({3-[2-(ethylamino)ethyl]-1-teayl} fluorenyl)_N-cyclopropyl phenyl (1_ 143482-1 • 32· 201111364 methyl-2-yl-l,2-dihydro-4-ρ ratio bite base)_3_hexahydro-p ratio to biting guanamine (Example 39) trans-N-[(2-ami Methyl]_N_cyclopropyl-4-(1-mercapto-2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide (Example 40) -N-cyclopropyl·4-(1-indolyl-2-keto-I,2-dihydro-4-pyridyl(9)-(1)-[2-(methoxy)ethyl]-1Η-丨哚-3-yl}mercapto)-3-hexahydropyridinium carboxamide (Example 41) trans-Ν-cyclopropyl-4-(1-methyl-2-keto-1,2 -Dihydro-4-pyridyl)·Ν-{[1-(2,2,2-trifluoroethyl)-1Η-吲哚_3-yl]indolyl}-3-hexahydropyrryl. Carboxylamidine® (Example 42) trans-Ν-cyclopropyl-4-(1-methyl-2-keto-1,2-dihydro-4-pyridyl)-Ν-{[1- (4,4,4-Trifluorobutyl)-1Η-indol-3-yl]indolyl}-3-hexahydroport than biting decylamine (Example 43) trans-N-[(l-butyl) Η-1Η-啕哚-3-yl) fluorenyl]-indole-cyclopropyl-4-(1-methyl-2-ketodihydro-4-pyridyl)-3-hexapyridine carboxy guanamine (Example 44) trans-Ν-cyclopropyl-indole-({1-[3-(ethoxy)propyl]_1Η_吲哚}}}}})) Base-1,2-dihydro-4_ρ ratio. Base) each hexahydro ρ ratio. Hydrazine (Example 45) trans-Ν-cyclopropyl-4-(1-indol-2-one-1,2-dihydropyridinyl)-indole-({1-[3, 3,3-Trifluoro-2-(trifluoromethyl)propyl]-1Η-indol-3-yl}indenyl)_3_hexahydropyridine carboxamide (Example 46) trans-Ν-({ Η3-(Ethylamino)propyl]-1Η-吲哚_3-yl}indenyl)_Ν_cyclopropylindol-2-one-1,2-dihydropyridinyl)-3- Hexahydropyridine carboxamide (Example 47) trans-Ν-cyclopropyl-4-(1-methyl-2-keto-1,2-dihydro-4-pyridyl 143482-1 -33· 201111364 [3-(Propylamino)propyl]-oxime-called 丨p-3-yl}fluorenyl)-3-hexahydrop ratio. Detamine (Example 48) trans-Ν-({1-[2-(ethylamino)ethyl]-1Η-indol-3-yl}fluorenyl)·ν_cyclopropyl- 4-(1-Methyl-2-keto-1,2-dihydro-4-ρ ratio. Azide)-3-hexahydroindole. Hydrazine (Example 49) trans-Ν-cyclopropyl-4-(1-mercapto-2-keto-1,2-dihydro-4-ρ ratio)-Ν-({ 1 -[2-(Propylamino)ethyl]-1Η-indol-3-yl}indenyl)-3-hexahydropyridinecarboxamide (Example 50) trans-indole-cyclopropyl-4 -(1-methyl-2-keto-1,2-dihydro-4-pyridinyl)-indole-{[1-(2-propan-1-yl)-1Η-吲嗓-3 -yl]mercapto}-3-hexahydron-rheptin (Example 51) trans-N-cyclopropyl-4-(1-methyl-2-keto-1,2-dihydro-4 -P ratio bite)-Ν-{[1-(phenylmethylindol-3-yl)indolyl}-3-hexahydrop ratio biting retinoic acid (Example 52) trans-N-cyclopropane 4-(1-mercapto-2-keto-1,2-dihydro-4-P ratio. Stationary)-Ν-{[1-(2-p ratio dimethyl)-1Η-吲Indole-3-yl]methyl}-3-hexahydropyridine carboxamide (Example 53) trans-N-cyclopropyl_4-(1_mercapto-2-keto-1,2-dihydro -4-pyridyl)-N-{ [1-(3-p-Bitylmethyl)-1Η-indol-3-yl]methyl}-3-hexahydropyridine Carboxamide (Example 54) -N-cyclopropyl·4-(ι_methyl_2-keto-i,2-dihydro-4-pyridyl)-indole-{[1-(4-pair 匕°-decylmethyl) -1Η-indol-3-yl]methyl}-3-hexahydropyridinecarboxamide (Example 55) trans-N-cyclopropane __n-({1-[(4-Fluorophenyl)indolyl]-1H-decaol-3-yl}indolyl)-4-(1-indol-2-ylyl-i,2- Dihydro-4-pyridyl) each hexahydropyridine carboxamide (Example 56) trans-N-({i-[(4-Phenylphenyl)methyl]_1Η_Ρ?|哚 丨 丨 methyl)_N Cyclopropyl-4-(1-indol-2-one-1,2-dihydro-4-pyridyl)_3_hexahydropyridine carboxamide (Example 57) 143482-1 •34· 201111364 Trans -N-cyclopropyl-N_(U-[(3-fluorophenyl)methyl]·1Η丨哚丨哚_3yl}methyl> 4-(1-methyl-2-keto-U- Dihydropyridinyl)_3_hexahydropyridine carboxamide (Example 58) trans-Ν-({1-[(3-chlorophenyl)indolyl]_1H-indole_3D methylcyclopropyl- 4-(1-mercapto-2-keto-1,2-dihydro-4-pyridyl)_3_hexahydropyridine carboxamide (Example 59) trans-Ν-({1-[(3- Cyanophenyl)indenyl]_1H_吲哚_3yl)methyl)ncyclopropyl-4-(1-indol-2-one-1,2-dihydro-4-pyridyl) Hexahydropyridine carboxamide (Example 60) trans-N-cyclopropyl-4-(1-methyl-2-keto-u-dihydropyridinyl) N_ ({H(3-mercaptobenzene) Methyl HH, ind-3-yl}fluorenyl)_3•hexahydropyridine carboxamide (Example 61) trans-N-cyclopropyl-N-({5- -1-[3-(decyloxy)propyl]_m_decadet-3-yl} fluorenyl-4-(1-methyl-2,yl-1,2-dihydro-4-pyridyl )_3_hexahydropyridine carboxamide (Example 62) trans-N-{[6-bromo-1-(phenylindenyl)-iH-indole_3_yl]indolyl N-cyclopropane 4-(1-mercapto-2-keto-1,2-dihydro-4-tonidyl)-hexahydropyridine carboxamide (Example 63) trans-N-cyclopropyl-N- UH(3-fluorophenyl)methyl]_6_(decyloxy)_1Η·Ρ 哚-3-yl]methyl)-4-(1-mercapto-2-keto-1,2-dihydro _4_pyridyl)_3_hexahydropyridine carboxamide (Example 64) trans-Ν-cyclopropyl-4-(1-indolyl-2-yl), 2_dihydro_4^ ratio π Stationary)_ν_{[4-methyl-1-(phenylindenyl)-1Η-indol-3-yl]methylidene 3-hexahydropyridinecarboxamide (Example 65) 143482-1 •35· 201111364 Trans-N-{[4-cyano-1-(phenylindenyl)_1H_indole)]indolyl N-cyclopropyl_4-α-mercapto-2-one-1, 2-Dihydro-4-pyridyl)_3_hexahydropyridine carboxamide (Example 66) trans-Ν-cyclopropyl-hydrazine-{[4-fluoro-1-(phenylindenyl)-plaw _吲哚_3_yl]methylmethyl-2-mercapto-1,2-dihydro-4-pyridyl)_3_hexahydropyridine carboxamide (Example 67) trans-Ν-ring Propyl-indole-({4-fluoro-1-[(3-fluorophenyl)indolyl]_1Η吲哚_3yl]methyl M-(l-methyl-2-yl-1,2 -dihydro-4-pyridyl) hexahydropyridine carboxamide (Example 68) trans-Ν-cyclopropyl-fluorene-({4-fluoro-1-[3-(methoxy)propyl) ]_1Η吲哚_3_yl)methyl)-4-(1-mercapto-2-keto-1,2-dihydropyridinyl) each hexahydropyridine carboxamide (Example 69) trans- Ν-({4-Alkyl-1-[3-(oximeoxy)propyl]_出_吲哚_3yl}methylcyclopropyl-4-(1-methyl-2-keto- 1,2-dihydropyridylpyridyl) winter hexahydropyridine carboxamide (Example 70) trans-N-U4-carbyl-1-(stylmethyl)_1Η_吲哚_3yl]methyl} _Νcyclopropyl phenyl (1-mercapto-2-keto-1,2-dihydropyridinyl)_3_hexahydropyridine carboxamide (example Ή) trans-Ν-{[4-bromo- 1-(phenylindenyl)_this 吲哚3-yl]methyldiphenylcyclopropyl-4-(1-methyl-2-keto-1,2-dihydro-4-pyridyl)_3 - hexahydropyridine carboxamide (Example 72) trans-Ν-({4-bromo-1-[(3-fluorophenyl)indolyl]ΗΗ_3•yl}methyl)& Propyl-4-(1-methyl-2-keto 4,2-dihydro-4-pyridyl)_3_hexahydropyridine carboxamide (Example 73) 143482-1 -36· 201111364 trans-N-({>Smellyl-1-[3-(methoxy)propylHH-indol-3-yl}indenyl)-N-cyclopropyl-4-(1 -Methyl-2-keto 4,2-dihydro-t-pyridyl)_3_hexahydropyridine carboxamide (Example 74) trans-N-cyclopropyl-oxime [(4-fluoro-1H) -Indol-3-yl)methyl]-4-(1-methyl-2-yl-1,2-dihydro-4-pyridyl)_3_hexahydropyridine carboxamide (Example 75) -Ν-ί辰propyl_N_{[4_Fluoro-small (3_pyridylmethyl)_1H-indole-3-yl] fluorenyl}-4-(1-methyl-2-keto- i,2-Dihydro-4-pyridyl)-3-hexahydropyridine carboxamide (Example 76) ® trans-N-cyclopropyl-N-{[4-fluoro-1-(4-pyridine) Methyl)_ih-W哚-3-yl] fluorenyl}-4-(1-methyl-2-keto-1,2-diin-4-pyridyl)-3-hexahydropyridinecarboxylate Amine (Example 77) trans-N-({3-Ethyl-5-[3-(indolyl)propyl]phenyl}methyl)-N-cyclopropyl-4-(1-A Benz-2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide (Example 78) trans-N-({1,3-bis[3-(methoxy) Propyl]-2,4-dione-1,2,3,4-tetrahydro-5-pyrimidinyl}methyl)-N-cyclopropyl-4-(1-methyl- 2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide (Example 79) trans-N-cyclopropyl-N-({2,3-dimethyl-5-[3-(methoxy)propyl]phenyl}methyl)-4-(1- Mercapto-2-keto-1,2-dihydrobutyric is determined by the ratio of 3-hexahydrop. Detamine (Example 80) trans-N-[(2-carbyl-5-{[2-(indolyl)ethyl]))}phenyl)indolyl]-N-cyclopropyl 4-(1_methyl-2-S-iso-1,2-.murine σ-yl)-3-hexanitro-p ratio. Derivatives (Example 81) trans _ Ν-cyclopropyl-4-(1·methyl ketone_1,2- 虱-4-ρ ratio. 定)-Ν-(2- each 143482- 1 -37- 201111364 hydrazino)-3-hexahydropyridine carboxamide (Example 82) trans-N-cyclopropyl-4-(1-mercapto-2-keto-1,2-dihydro -4-p ratio bite)_n_({3-[(trifluoromethyl)thio]phenylindolemethyl)-3-hexahydropyridine carboxamide (Example 83) trans-N-cyclopropyl 4-(1-mercapto-2-keto-1,2-dihydro-4-pyridyl(methoxy)propyl]-2-(indolyl)phenyl]methyl}-3- Hexahydro-p ratio. Detergent amine (Example 84) trans-N-({3-bromo-4-methyl-5-[3-(methoxy)propyl]phenyl}methyl) ring Propyl-4-(1-mercapto-2-keto-1,2-dihydro-4-ρ ratio octyl)-3-hexahydrop ratio biting slowing amine (Example 85) #trans-N -[3,5-bis(3-decyloxypropyl)indenyl]-N-cyclopropyl-4-(1-methyl-2-indoleyldihydro-4-p ratio) 3-hexahydrop to bite giamine (Example 86) trans-N-cyclopropyl-N-[3-(3-methoxypropyl)-5-mercapto]-4-(1- Mercapto-2-keto-1,2-dihydro-4-pyridyl) hexahydropyridine carboxamide (Example 87) trans-N-[2-Molyl-3,5-bis(3- Methoxypropyl)henyl] -N-cyclopropyl_4-(1_mercapto-2-keto-1,2-dihydro-4-p ratio octyl)-3-hexahydroindole retinoic amine (Example 88) trans -N-[2-carbyl-3,5-bis(3-decyloxypropyl)-yl]_N_cyclopropylidene (1_mercapto-2-keto-1,2-dihydro- 4-P ratio bite)_3-hexahydro? than D-denidamine (Example 89) ® trans-N-cyclopropyl_n_[2-methoxy-3,5-bis(3-methoxy Propyl)-4-(1-methyl-2-keto-1,2-dihydropyridinyl)·3-hexahydropyridinecarboxamide (Example 9〇) trans-N- Cyclopropyl-N_[3_(3-methoxypropyl)_5_(trifluoromethyl)]]]4_(1_methyl-2-keto-1,2-dihydro-4-pyridyl)_3 _ hexahydropyridine carboxamide (Example 91) trans-N-cyclopropyl_N_[3_hydroxy_5·(3methoxypropyl)]]4 (1 methyl-2-keto- 1'2-monohydro-4-pyridyl)_3-hexahydropyridine carboxamide (Example 92) trans-indole-(3-benzhydryl-5-bromodecylcyclopropyl-4) Methyl-2-ketone 143482-1 •38- 201111364 yl-1'2-dihydro-H-decyl)-3-hexahydroindole sigmaamine (Example 93) trans-N-{3-bromo group -5-[(1Ε)-3-decyloxypropenyl small group]-based group N•cyclopropyl-4-(1-mercapto-2-keto-1,2-dihydrogen Pyridyl)_3_hexahydropyridinium carboxamide (Example 94) trans-N-{3-bromo-5-[(2-hydroxyethyl)thio]-yl}}-cyclopropyl ice (1_ Mercapto-2-keto-1,2-dihydro-4-Ppyridyl)_3_hexahydropyridylcarboxamide (Example 95) trans-N-cyclopropyl-N-[3-[ 2-(cyclopropyloxy)ethoxy>5-(3-methoxypropyl)-yl]-4-(1-methyl-2-keto-l,2-dihydro-4- Pyridyl) each hexahydropyridine carboxamide (Example 96) trans-N-cyclopropyl-N-{3-(3-methoxypropyl)_5_[2_(4_morpholinyl) ethoxylate ]]}}(1-methyl-2-keto-i,2-dihydro-4-pyridyl)-3-hexahydropyridine decylamine (Example 97) trans-3-[ (cyclopropyl {[4-(1-indolyl-2-keto)dihydro-4-pyridyl)3 hexahydropyridyl]carbonylguanidinyl)methyl]-5-(3-methoxypropane Phenyl 4-morpholine carboxylate (Example 98) trans-N-cyclopropyl-N-[6-(3-methoxypropyl)_2,3-dihydro-1H- though- 1-yl]_4_(1-mercapto-2-keto-1,2-dihydro-4-p than dimethyl)_3_hexahydro? Tough acid amine (Example 99) trans-N-cyclopropyl-N-[7-(3-methoxypropyl)_ι, 2,3,4-tetrahydro-1-chalyl-4 -(1-mercapto-2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridylcarboxamide (Example 100) trans-N-[3-bromo- 5-(3-Hydroxypropyl)-4-indolebenzyl]-N-cyclopropyl-4-(1-methyl-2-keto-1,2-dihydro-4-? ratio α-based) -3-hexahydrop is more than a chitosamine (Example 1〇).) trans-Ν-[3-bromo-5-(3-ethoxypropyl)-4-indenyl]-oxime- Cyclopropyl-4-(1-methyl-2-keto-1,2-dihydro-4-ρ ratio. Alkyl)-3-hexahydrop-pyridine hydrazide (Example 1〇2) 143482 -1 -39- 201111364 trans-N-{3-bromo-5-[3-(difluorodecyloxy)propyl]_4_indolyl ρΝ_cyclopropyl-4-(1-indenyl) 2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide (Example 103) trans-Ν-(3-ylyl-5-methylindenyl)_Ν_ Cyclopropyl ice (1_methyl-2-keto^hydro-4-pyridyl)-3-hexahydrop ratio carboxy carbamide (Example 1〇4) trans-N-[3-Momot -5-(3-fluoroindolyl)_4_曱benzyl]_N_cyclopropyl_4-(l-fluorenyl-2-keto-1,2-dihydro-4-pyridyl)-3- Hexahydropyridine carboxamide (Example 1〇5) trans-N-[3-bromo-5-(3- Fluorobenzoyl)_4-mercapto]_Ν·cyclopropyl winter (1_ decyl-2-keto-1,2-dipho-4-pyr ratio. Stationary)-3-hexahydro? Ratio D to slow amine (Example 1〇6) trans-N-{3-bromo-5-[(3-fluorophenyl)(hydroxy)indenyl]_4_曱benzyl}_N_cyclopropyl 4-(1-mercapto-2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide (Example 107) trans-N-[2- gas-based- 5-(2-decyloxyethyl)benzyl]cyclopropyl-4_hydroxy_4_(1-indol-2-one-1,2-dihydro-4-p ratio) - Hexahydrogen? Determining g-amine by ratio π (Example 108) trans-N-[2-carbyl-5-(2-methoxyethyl)]]-n-cyclopropyl_4_decyloxy-4- (1-Methyl-2-keto-1,2-dihydro-4-ρ ratio octyl)-3-hexahydrop to chiral acid amine (Example 109) trans-N-cyclopropyl-4 -hydroxy-N-[3-(2-decyloxyethoxy)_5_(3-methoxypropyl)octyl]-4-(1-methyl-2-keto-1,2-di Hydrogen-4-pyridyl) each hexahydropyridine slow oxime (Example 110) trans-N-cyclopropyl-4-methoxy-N-[3-(2-methoxyethoxy)_5_( 3-methoxypropyl)henyl]-4-(1-indolyl-2-keto-l,2-dihydro-4-? ratio. Stationary)_3_hexahydro-P ratio Example 111) 143482-1 -40- 201111364 The invention also encompasses a pharmaceutical formulation comprising a pharmaceutically acceptable carrier and a compound of formula I or a pharmaceutically acceptable crystalline form or hydrate thereof. A specific embodiment is a pharmaceutical composition of a compound of formula I which additionally comprises a second agent. List of abbreviations: BINAP 2,2'-bis(diphenylphosphino)-1, hydrazine-hydrazine BOC tert-butoxycarbonyl BSA bovine serum albumin _ COD 1,5-cyclooctadiene DBU 1, 8-Diazabicyclo[5.4.0]unde-7-dilute DCM Dioxane DIBA1-H Diisobutylaluminum hydride DMAP 4-Dimethylaminopyridine DME 1,2-dimethoxy ethane DMF Ν, Ν-dimercaptoamine • DMP Dess-Martin over-fired DMSO 曱 曱 曱 D DPPB 1,4-bis(diphenylphosphino)butane DPPF 1, Γ-bis (diphenyl Phosphyl) Dicyclopentadienyl Iron EDTA Ethylenediaminetetraacetic Acid EIA Enzyme Immunoassay Et20 Ethyl Acetate Ethyl Acetate HATU Hexafluorophosphonium Phosphate-(7-Nitrobenzotriazol-1-yl)-Ν,Ν,Ν ',Ν'-四曱基锞143482-1 -41 - 201111364

Hex 己烧 IPA 異丙醇 KHMDS 六曱基二矽氮化鉀 mCPBA 間-氣過苯曱酸 MeOH 曱醇 NBS N-溴基琥珀醯亞胺 NMO N-甲基嗎福啉-N-氧化物 n-PrOH 正-丙醇 PBS 填酸鹽緩衝之鹽水 PG 保護基 PPh3 三苯膦 RT 室溫 TBAF 氟化四丁基銨 TFA 三氟醋酸 THF 四氫p夫喃 TMEDA Ν,Ν,Ν·,Ν'-四曱基乙二胺 Tol 曱苯 MTBE 甲基第三-丁基醚 COD 環辛二烯 c.HCl 濃HC1 除非明確地相反陳述,否則於本文中引用之所有範圍均 為内含。例如,被描述為q -c6烷基之烷基係意謂該烷基可 含有1, 2, 3, 4, 5或6個碳原子。 當特定範圍包含〇時(例如(CH2)0-3),0係意謂直接共價鍵。 143482-1 -42- 201111364 當任何變數於任何組成中’或於描繪與描述本發明化合 物之任何化學式中出現超過—次時,其在各存在處之定義 係與其在每一個其他存在處之定義無關。 而且’取代基及/或變數之組合,只有在此種組合會造成 安定化合物下才可允許。 左取代一詞(例如在”視情況被一或多個取代基取代之 芳基··.”中)包括被所指稱取代基之單_與多取代,達此種單 與夕重取代(包括在相同位置上之多重取代)係於化學上 被允终且造成安定化合物之程度。 安定"化合物為一種化合物,其可經製備與單離,且其 結構與性質仍然保肖’或可被造成保持基本上不變,歷經 丰又足以允5午使用g亥化合物以達本文中所述目的(例如對 病患之治療或預防投藥)之時間。 在具有吡啶基N-氧化物部份基團之本發明化合物中,吡 啶基-N-氧化物部份係於結構上使用習用表示圖描嬖 _ 乂 N—0 Ο"'0' 其具有相當之意義。 本發明係關於一種治療及/或預防疾病之方法,該疾病係 關於高血壓、鬱血性心衰竭、肺高血壓、收縮高血壓 '腎 機能不全、腎絕血、腎衰竭、腎纖維變性、心臟機能不全、 心臟肥大、心臟纖維變性、心肌絕血、心肌病、絲球體性 腎炎、腎絞痛,由於糖尿病所造成之併發症,譬如腎病、 脈管病及神經病,青光眼、高眼球内壓力、動脈粥瘤硬化、 血管造形術後之再狹窄、在血管或心臟手術後之併發症、 143482-1 ,43- 201111364 勃起機能障礙、醛固酶過多症、肺纖維變性、硬皮病、焦 慮、認知病症、以免疫壓抑劑治療之併發症及其他已知與 腎素-血管收縮素系統有關聯之疾病,此方法包括對人類或 動物投予如上文定義之化合物。 於另一項具體實施例中,本發明係關於一種治療及/或預 防疾病之方法,該疾病係關於高血壓、鬱血性心衰竭、肺 高血壓、腎機能不全、腎絕血、腎衰竭、腎纖維變性、心 臟機能不纟、心臟肥大、心臟纖維變性、心肌絕血、心肌 病’由於糖尿病所造成之併發症,譬如腎病、脈管病及神 經病。於另-項具體實施例中,本發明係關於—種治療及/ 或預防與腎素-血管收縮素系統之調節功能障礙有關聯之 疾病,以及治療上文所提及疾病之方法。 /本發明亦關於式(1)化合物於藥劑製備上之用*,該藥劑 係用於治療及/或預防上文所提及之疾病。 式①化合物或上文所提及之醫藥組合物亦可合併使用其 他樂理學活性化合物’包括ACE,制劑、中性内肽酶抑制 劑、血管收縮素11受體拮抗劑、内皮肽受體拮抗劑、血管 擴張劑' @拮抗劑、鉀活化劑 '利尿劑、抑交感劑、錢 上腺素能拮抗劑、㈣上腺素能拮抗劑或其他有利於預防 或治療上文所提及疾病之藥物。 ' 關於式I化合物,”投筚”— 巧及其變型(例如,,投予,,化合 係意謂對需要治療或預防之個體提供化合物或該化人 =體樂物。當本發明之化合物或其前體藥物; 夕種其他活性劑(例如—種藥劑,譬如血管受= 143482-1 201111364 4 d ACE抑制劑或其他已知會降低血壓之活性劑)人併提 供時,應明瞭,,投藥"及其變型係各包括在㈣時时或在 不同時間下提供該化合物或前體藥物及其他藥劑。去組人 之藥劑係同時投予時,其可在單一組合物中一起投二 其可個別地投予。 予或 於本文中使用之”組合物 旦 冲心队叫盈—種以特定Hex hexane IPA isopropanol KHMDS hexamethylene dihydrazine potassium hydride mCPBA m-gas perbenzoic acid MeOH sterol NBS N-bromo amber quinone imine NMO N-methylmorpholine-N-oxide n -PrOH n-propanol PBS sulphate buffered saline PG protecting group PPh3 triphenylphosphine RT room temperature TBAF tetrabutylammonium fluoride TFA trifluoroacetic acid THF tetrahydropuffan TMEDA Ν, Ν, Ν·, Ν' - Tetradecylethylenediamine Tol Benzene MTBE Methyl Third-Butyl Ether COD Cyclooctadiene c. HCl Concentrated HC1 All ranges quoted herein are inclusive unless explicitly stated to the contrary. For example, an alkyl group described as a q-c6 alkyl group means that the alkyl group may contain 1, 2, 3, 4, 5 or 6 carbon atoms. When a specific range contains 〇 (for example, (CH2) 0-3), the 0 system means a direct covalent bond. 143482-1 -42- 201111364 When any variable appears in any composition' or occurs in any chemical formula that describes and describes a compound of the invention, its definition at each occurrence is defined in each of its other places of existence. Nothing. Moreover, combinations of substituents and/or variables are permissible only if such combinations result in a stability compound. The term "replacement of the left" (for example, in the "aryl group substituted by one or more substituents as appropriate") includes the single- and multiple-substituted substitutions of the indicated substituents, Multiple substitutions at the same position are chemically terminated and result in a degree of stability of the compound. The stability of a compound is a compound that can be prepared and isolated, and its structure and properties remain intact or can be kept substantially unchanged, and it is sufficient to allow the use of g-shell compounds at 5 noon. The time of the purpose (eg, administration to a patient for treatment or prevention). In the compound of the present invention having a pyridyl N-oxide moiety, the pyridyl-N-oxide moiety is structurally represented by a conventional representation _ 乂 N - 0 Ο " '0' The meaning. The present invention relates to a method for treating and/or preventing diseases related to hypertension, septic heart failure, pulmonary hypertension, systolic hypertension, renal insufficiency, renal blood loss, renal failure, renal fibrosis, heart Insufficiency, cardiac hypertrophy, cardiac fibrosis, myocardial ischemia, cardiomyopathy, spheroid nephritis, renal colic, complications caused by diabetes, such as kidney disease, vascular disease and neuropathy, glaucoma, high intraocular pressure, Atherosclerosis, restenosis after angioplasty, complications after vascular or cardiac surgery, 143482-1, 43- 201111364 Erectile dysfunction, aldosteronism, pulmonary fibrosis, scleroderma, anxiety, Cognitive disorders, complications treated with immunosuppressive agents, and other diseases known to be associated with the renin-angiotensin system include administering a compound as defined above to a human or animal. In another embodiment, the invention relates to a method of treating and/or preventing a disease, relating to hypertension, septic heart failure, pulmonary hypertension, renal insufficiency, renal ischemia, renal failure, Renal fibrosis, cardiac dysfunction, cardiac hypertrophy, cardiac fibrosis, myocardial ischemia, cardiomyopathy 'complications due to diabetes, such as kidney disease, vascular disease and neuropathy. In another embodiment, the invention relates to a method of treating and/or preventing a disorder associated with the regulation of dysfunction of the renin-angiotensin system, and a method of treating the above mentioned diseases. / The present invention also relates to the use of a compound of the formula (1) for the preparation of a medicament for the treatment and/or prevention of the diseases mentioned above. The compound of formula 1 or the pharmaceutical composition mentioned above may also be combined with other music active compounds including ACE, formulation, neutral endopeptidase inhibitor, angiotensin 11 receptor antagonist, endothelin receptor antagonist Agent, vasodilator ' @ antagonist, potassium activator' diuretic, antisympathetic agent, adrenergic antagonist, (iv) adrenergic antagonist or other beneficial to prevent or treat the above mentioned diseases drug. 'About the compound of formula I, "injection" - and its variants (for example, administration, compounding means providing a compound or a human body to a subject in need of treatment or prevention. When the compound of the invention Or its prodrug; other active agents (such as a drug, such as blood vessels = 143482-1 201111364 4 d ACE inhibitors or other active agents known to lower blood pressure) and provided, should be clear,, dosing " and its variants each include providing the compound or prodrug and other agents at (iv) or at different times. When the de-grouped agents are administered simultaneously, they may be administered together in a single composition. Can be administered individually. The composition used in this article

^ 3特&成份之產物,以及任何直接或間接由於以特定 置合併特定成份所造成之產物。 所明藥學上可接受”係指醫藥組合物之成份必項可啮 相容,且不會有害於其接受者。 可彼此 於本文中使用之”病患"一詞係指動物,在 例中為哺乳動物,而在特殊具體實施例中為人類 是治療、觀察或實驗之目標。 ’、'' 於本文中使用之’·有效量"或”醫藥活性量,,一詞係音* 活性化合物或藥劑之量’其會引出研究人員、 床家所正在尋求之組織、系統 '動物或人類中之 生物干或醫藥回應。於一項具體實施例中,有 減輕被治療疾病或症狀之徵候之,•治療上有效量·,里於二 ==1V有效量為關於預防被阻止疾病或症狀: 且 效量"。此術語於本文中亦包括足以抑制 月素且错以引出被尋求之回應之守,w外 制有效量·>當活性化合物(意:物:u、即抑 稱係針對化合物之自由態形式(意即非 皿 特殊具體實施例中,此量係包括每天!毫克與 143482-1 -45- 201111364 1000毫克之間。在其他具體竇竑办丨ώ 八體貫%例中,此量係包括每天i 克與500毫克之間。在其他呈體音 天^ 3 products of the & components, and any products directly or indirectly due to the specific combination of specific components. It is understood that the pharmaceutically acceptable ingredients mean that the ingredients of the pharmaceutical composition are compatible and not deleterious to the recipient. The term "patient" as used herein refers to an animal, in the case It is a mammal, and in a particular embodiment is a human being, a target for treatment, observation or experimentation. ','' used in this article '·effective amount' or 'medical activity amount, the word sound * the amount of active compound or agent' will lead to the researcher, the organization that the bed is seeking, system' A biologically dry or medicinal response in an animal or human. In one embodiment, there is a symptom of amelioration of the disease or condition being treated, • a therapeutically effective amount, and an effective amount in the second = =1 V is prevented from being prevented Disease or Symptoms: and the dose ". The term also includes herein sufficient to inhibit the monthly element and the wrong to lead to the response sought, w externally effective amount ·> when the active compound (meaning: substance: u, That is, the inhibition system is directed to the free form of the compound (meaning that it is not specifically described in the specific embodiment, this amount includes between daily milligrams and 143482-1 -45-201111364 1000 mg. In other specific sinus 竑 丨ώ 八In the case of body%, this amount includes between i and 500 mg per day.

/、體貫靶例中,此量係包括备 1毫克與200毫克之間。 I 在本發明之方法中(意即抑制腎素),式!化合物,視情..兄 呈鹽形式,可藉會產生活性劑與藥劑作用位置接觸之任何 方式投藥。如所述之此種投藥方法係形成本發明之特定且 體實施例。該化合物可藉㈣可用於.搭配醫藥之習用方:气 投藥,作成個別治療劑或在治療劑組合卜其可單獨投:, 但典型上係與輯選擇之投藥途徑及標準㈣實務為基礎 作選擇之醫藥載劑-起投藥。本發明化合物可例如以經口 方式、黏膜方式(包括舌下、面夹員 '直腸、鼻或陰道投藥)、 非經腸方式(包括皮下注射、大丸劑注射,動脈内、靜脈内、 肌内、胸骨内注射,或灌注投藥技術)、藉由吸入喷霧,經 皮,譬如被冑或離子電渗傳冑,或局部才史藥,w含有有效 3:之化合物與習用無毒性藥學上可接受之載劑、佐劑及媒 劑之醫藥組合物之單位劑量形式投藥。上述使用如本文中 所 意 述化合物之投藥技術係形成本發明之重要具體實施例。 欲被涵蓋作為本發明一部份之劑型之實例係包括但不限 於:片劑、小藥囊,膠囊,譬如軟彈性明膠膠囊,扁囊劑、 錠劑、糖錠、分散液、栓劑、軟膏、泥敷劑(粥劑)、糊劑、 私末、敷料 '乳膏、石膏、溶液 '貼藥、氣溶膠(例如鼻喷 霧劑或吸入|§ )、凝膠,適用於口腔或黏膜投予病患之液體 劑型,包括懸浮液(例如水性或非水性液體懸浮液、油在水 中型乳化液或水在油中型液體乳化液)、溶液及酏劑,適合 143482-1 -46- 201111364 非經腸投予病患之液體劑型,及盔菌 …、困固體(例如結晶性或非 曰曰曰質固體),其可被重配以提供適合非經腸投予病患之液體 劑型。適於口服投藥之液體製劑(例如懸浮液、糖激、醜劑 等)可根據此項技藝中已知之技術製成,且可採用任何常用 媒質,譬如水、二醇類、油類、醇類等。適於口服投藥之 固體製劑(例如粉末、丸劑 '膠囊及片劑)可根據此項技藝 中已知之技術製成,且可採用一些固體賦形劑,譬如澱粉、 •糖類、高嶺土、潤滑劑、黏合劑、崩解劑等。非經腸組合 物可根據此項技藝中已知之技術製成,且典型上係採用作 為载劑之無菌水,與選用之其他成份,譬如溶解助劑。可 /主射’合液可根據此項技藝中已知之方法製成,纟中載劑包 $鹽水溶液、葡萄糖溶液或含有鹽水與葡萄糖之混合物之 '合液。適用於製備供使用於本發明中之醫藥組合物之方法, 及適用於該組合物中之成份之進一步說明,係提供於/, in the body target, this amount includes between 1 mg and 200 mg. I In the method of the invention (meaning to inhibit renin), formula! The compound, as the case may be, is in the form of a salt which can be administered by any means which produces an active agent in contact with the site of action of the agent. Such administration methods as described form a particular embodiment of the invention. The compound can be used in conjunction with the prescription of the medicine: gas administration, individual treatment or combination of therapeutic agents: it can be administered separately, but it is usually based on the selection route and standard (4) practice. The selected pharmaceutical carrier - from the drug. The compounds of the present invention can be administered, for example, orally, mucosally (including sublingual, face-clamped 'rectal, nasal or vaginal administration), parenteral (including subcutaneous injection, bolus injection, intra-arterial, intravenous, intramuscular). , intrathoracic injection, or perfusion medication technology), by inhalation spray, percutaneous, such as by sputum or iontophoresis, or local history, w contains effective 3: compound and conventional non-toxic pharmaceutically acceptable The pharmaceutical composition of the carrier, adjuvant and vehicle is administered in unit dosage form. The above-described administration techniques using the compounds as described herein form an important embodiment of the invention. Examples of dosage forms to be encompassed as part of the present invention include, but are not limited to, tablets, sachets, capsules, such as soft elastic gelatin capsules, cachets, lozenges, lozenges, dispersions, suppositories, ointments. , cataplasm (porridge), paste, blister, dressing 'cream, plaster, solution' patch, aerosol (eg nasal spray or inhalation | §), gel, suitable for oral or mucosal cast Liquid dosage forms for patients, including suspensions (such as aqueous or non-aqueous liquid suspensions, oil-based emulsions or water-based liquid emulsions), solutions and elixirs, suitable for 143482-1 -46- 201111364 Liquid dosage forms for enteral administration, and Helmets, trapped solids (e.g., crystalline or non-steroidal solids), which can be reconstituted to provide a liquid dosage form suitable for parenteral administration. Liquid preparations suitable for oral administration (e.g., suspensions, glycolics, ugly agents, etc.) can be made according to techniques known in the art, and any conventional medium such as water, glycols, oils, alcohols can be employed. Wait. Solid preparations suitable for oral administration (e.g., powders, pills 'capsules and tablets) can be made according to techniques known in the art, and can employ solid excipients such as starch, sugar, kaolin, lubricants, Adhesives, disintegrators, etc. The parenteral compositions can be made according to techniques known in the art, and typically employ sterile water as a vehicle, together with other ingredients such as dissolution aids. The /priming' solution can be made according to methods known in the art, and the carrier is a solution of saline solution, dextrose solution or a mixture of saline and glucose. A method suitable for the preparation of a pharmaceutical composition for use in the present invention, and further description of the ingredients suitable for use in the composition, is provided

Remmgt()n氏醫藥科學,第18版,由A.R.Gennaro編著,Mack出 • 版公司,1990中。 發月亦關於製備本文中所述化合物之方法。在特定具 &實^例中’本發明係關於製備下式化合物之方法: R1Remmgt () N Medical Science, 18th Edition, edited by A.R. Gennaro, Mack, Ltd., 1990. The method of preparing the compounds described herein is also known. In the specific & embodiment, the invention relates to a method for preparing a compound of the formula: R1

其中:· U3482-1 -47- 201111364 R1為視情況被1-3個鹵素取代之Q -C2烷基, R2與R3係獨立選自下列組成之組群:氫、鹵素、q -C5 烧基、C】-C5院氧基及-0-(C丨-C5伸烧基)-0-(CH2 )〇 - 3 -CH3 ’其中 烷基、烷氧基及-0-((:! -C5伸烷基)-0-(CH2 )〇 - 3 -CH3係視情況被 1-3個取代基取代,取代基獨立選自下列組成之組群:鹵 素、視情況被1-3個鹵素取代之q -C5烷基及視情況被1-3個 鹵素取代之C! -C5烷氧基, X係選自下列組成之組群:氫、-OH及C, -C5烷氧基, (Z)n丨為C丨-C2伸烷基, A係選自下列組成之組群: ⑴氫, (2) 鹵素, (3) CVC5烷基, (4) CVCs烷氧基,及 (5) -S-(CH2 )〇. 3 "CHj > 其中(3)與⑷係視情況被μ3個鹵素取代’ Β係選自下列組成之組群: ⑴氫, (2)鹵素, ⑶烷基, (4) CVC5烷氧基, ⑶-OH, ⑹-CF3, (7) _c(=0)-CH3, 143482-1 201111364 (8) -0-(C丨-C5 伸烷基)-0-(CH2 )〇 — 2 -CH3, (9) -(C】-C5 伸烷基)-0-(CH2 )0.2 -CH3, (10) -0-(C丨-c5 伸烷基)-C(CH3 )2 -C(=0)0H,及 (11) -O-CCrCs 伸烷基)-C(CH3)2-C(=0)0CH3, 其中(3),⑷,(8),(9)及(11)係視情況被1-3個鹵素取 代, C係選自下列組成之組群: ⑴氫, (2) q-Q烷基,視情況被1-3個鹵素取代,及 (3) Q -C5烷氧基,視情況被1-3個鹵素取代,且 D係選自下列組成之組群: ⑴氫, (2) 鹵素, (3) (VC5烷基, (4) Q-Q烷氧基, (5) 氰基, (6) C2 -C5 伸烯基-0-(CH2 )〇. 2 -CH3, (7) -(q -C5 伸烷基)_N(H)-C(=0)-0-(CH2 )0 - 2 -CH3, (8) -(C! -C5 伸烷基)-N(H)-C(=0)-(CH2 )〇 - 2 -CH3, (9) -(q -C5 伸烷基)-0-CHF2, (10) -(C〗-C5 伸烷基)-O-(CH2)0.2-CH3, (11) -0-(Ci-C5 伸烷基)-O-(CH2)0-2-CH3, (12) -((VC5伸烷基)-OH, (13) -S-A-Cs 伸烷基)-OH, 143482-1 -49- 201111364 (14) -SCF3,及 (15) -NCHHq -C5 伸烷基)-0-(CH2 )〇 _ 2 -CH3, 其中(3),(4),(5),(6),(7),(8),(9),(10),(11),(12),(13)及(15) 係視情況被1-3個鹵素取代, 其係包括下列步驟: (1)使式⑻化合物或其鹽於溶劑存在下偶合至式⑻化合 物或其鹽:Wherein: · U3482-1 -47- 201111364 R1 is a Q-C2 alkyl group optionally substituted by 1-3 halogens, and R2 and R3 are independently selected from the group consisting of hydrogen, halogen, q-C5 alkyl , C]-C5, alkoxy and -0-(C丨-C5 extended alkyl)-0-(CH2)〇-3 -CH3 ' wherein alkyl, alkoxy and-0-((:! -C5 The alkylene group -0-(CH2)〇-3 -CH3 is optionally substituted with from 1 to 3 substituents independently selected from the group consisting of halogens, optionally substituted by 1-3 halogens. a C-C5 alkyl group and a C-alkoxy group substituted by 1-3 halogens, X is selected from the group consisting of hydrogen, -OH and C, -C5 alkoxy, (Z) n丨 is C丨-C2 alkylene, and A is selected from the group consisting of: (1) hydrogen, (2) halogen, (3) CVC5 alkyl, (4) CVCs alkoxy, and (5)-S -(CH2 )〇. 3 "CHj > where (3) and (4) are replaced by μ3 halogens as appropriate. ' Β is selected from the group consisting of: (1) hydrogen, (2) halogen, (3) alkyl, ( 4) CVC5 alkoxy, (3)-OH, (6)-CF3, (7) _c(=0)-CH3, 143482-1 201111364 (8) -0-(C丨-C5 alkyl)-0-(CH2 )〇— 2 -CH3, (9) -(C -C5 alkylene)-0-(CH2)0.2 -CH3, (10) -0-(C丨-c5 alkylene)-C(CH3)2 -C(=0)0H, and (11)- O-CCrCs alkyl)-C(CH3)2-C(=0)0CH3, wherein (3), (4), (8), (9) and (11) are optionally substituted by 1-3 halogens, Group C is selected from the group consisting of: (1) hydrogen, (2) qQ alkyl, optionally substituted with 1-3 halogens, and (3) Q-C5 alkoxy, optionally substituted with 1-3 halogens And D is selected from the group consisting of: (1) hydrogen, (2) halogen, (3) (VC5 alkyl, (4) QQ alkoxy, (5) cyano, (6) C2 - C5 Base-0-(CH2)〇. 2 -CH3, (7) -(q -C5 alkylene)_N(H)-C(=0)-0-(CH2 )0 - 2 -CH3, (8) -(C! -C5 alkylene)-N(H)-C(=0)-(CH2)〇- 2 -CH3, (9) -(q -C5 alkylene)-0-CHF2, (10 -(C--C5 alkylene)-O-(CH2)0.2-CH3, (11)-0-(Ci-C5 alkylene)-O-(CH2)0-2-CH3, (12) -((VC5 alkylene)-OH, (13) -SA-Cs alkylene)-OH, 143482-1 -49- 201111364 (14) -SCF3, and (15) -NCHHq -C5 alkylene) -0-(CH2 )〇_ 2 -CH3, where (3), (4), (5), (6), (7), (8), (9), (10) (11), (12), (13) and (15) are optionally substituted by 1 to 3 halogens, which comprise the following steps: (1) Coupling a compound of the formula (8) or a salt thereof in the presence of a solvent to the formula (8) Compound or its salt:

以形成式⑹化合物或其鹽To form a compound of the formula (6) or a salt thereof

(2)藉由移除Boc使化合物⑹去除保護。 在特殊具體實施例中,溶劑係為/包括一或多種化合物, 選自下列組成之組群:DMF、氣化草醯及/Pr2Net。在特殊 具體實施例中,去除保護步驟係以一或多種化合物進行, 該化合物選自下列組成之組群:HC1、IPA及MTBE。 在特定具體實施例中,本發明係關於一種製備下式化合 物之方法: 143482-1 -50- 201111364(2) The compound (6) is removed from the protection by removing Boc. In a particular embodiment, the solvent is/comprising one or more compounds selected from the group consisting of DMF, gasified grass mash, and /Pr2Net. In a particular embodiment, the removal protection step is carried out with one or more compounds selected from the group consisting of HC1, IPA, and MTBE. In a particular embodiment, the invention is directed to a method of preparing a compound of the formula: 143482-1 -50- 201111364

其係包括下列步驟: (1)使具有Boc基團之式⑻化合物與下文式(b),於DMF、 氯化草醯及zPr2NEt存在下偶合:It comprises the following steps: (1) coupling a compound of formula (8) having a Boc group to formula (b) below, in the presence of DMF, chlorinated mash and zPr2NEt:

以形成式(c)化合物To form a compound of formula (c)

MeMe

(C); 與(C); with

(2)使所形成之化合物經過Boc基團之移除,於HCL、IPA 及MTBE存在下去除保護。 合成方法 本發明之化合物可藉由下文所示與描述之說明性合成反 應圖式中描繪之多種方法製成,其係形成本發明之特定具 143482-1 201111364 體實施例。用於製備此等化合物之起始物質與試劑,通常 係為可得自市售供應商,譬如Aldrich化學公司’或藉由熟 諳此藝者已知之方法,按照參考資料中所提出之程序製備, 譬如有機合成之Fieser與Fieser氏試劑;Wiley & Sons : New York, 第1-21卷;R. C. LaRock,綜合有機轉變,第2補充版Wiley-VCH, New York 1999 ;综合有機合成,B. Trost 與 I. Fleming (編著)第 1-9 卷 Pergamon,Oxford, 1991 ;綜合雜環化學,A. R. Katritzky 與 C. W. Rees (編著)Pergamon,Oxford, 1984,第 1-9 卷;综合雜環化學 II, A. R. Katritzky 與 C. W. Rees (編著)Pergamon,Oxford 1996,第 1-11 卷;及有機反應,Wiley & Sons : New York, 1991,第 1-40 卷。下 述合成反應圖式與實例僅只是本發明化合物可藉以合成之 一些方法之說明例而已,並可施行此等合成反應圖式之各 種修正,且對於已參考本申請案中所包含揭示内容之熟諳 此藝者係為由然心生。 合成反應圖式之起始物質與中間物,若需要可使用習用 技術單離與純化,包括但不限於過濾、蒸餾 '結晶化作用、 層析等。此種物質可使用習用方式作特徵鑒定,包括物理 常數與光譜數據。 除非另有特別敘述,否則實驗程序係在下述條件下進行。 溶劑之蒸發係使用迴轉式蒸發器,在減壓(600-4000巴斯卡: 4.5-30毫米Hg)下,以至高60°C之浴溫進行。若未另有指出, 則反應典型上係在氮大氣下,於環境溫度下操作。無水溶 劑’譬如THF、DMF、Et2 Ο、DME及曱笨,係為商用級。試 劑係為商用級,且使用之而無需進一步純化。急驟式層析 143482-1 -52- 201111364 係於石夕膠(雛網目)上操作。反應過料㈣層層析法 (TLC)或核磁共振(NMR)光譜測定法追蹤,且所予之反應時 間係僅為說明而已。所有最後產物之結構與純度係藉 TLC、質#光譜法、加·及高壓液相層析法(Η·)確定。 化學符號具有其常用意義。下列縮寫亦已被使用:v(體積), W(重量),b.P.(沸點),m.P.(熔點),L(升),乱(毫升),g (克),mg(毫克)’ mol(莫耳),聰〇1(毫莫耳),叫(當量)。(2) The formed compound is removed by removal of the Boc group and the protection is removed in the presence of HCL, IPA and MTBE. Synthetic Methods The compounds of the present invention can be made by a variety of methods depicted in the illustrative synthetic reaction schemes shown below and in the description, which form the specific embodiment of the invention 143482-1 201111364. Starting materials and reagents for the preparation of such compounds are generally prepared by commercially available suppliers, such as Aldrich Chemical Company, or by methods known to those skilled in the art, in accordance with the procedures set forth in the references. For example, Fieser and Fieser's reagents for organic synthesis; Wiley & Sons: New York, Vol. 1-21; RC LaRock, Integrated Organic Transformation, 2nd Supplement Wiley-VCH, New York 1999; Integrated Organic Synthesis, B. Trost And I. Fleming (eds.), Volumes 1-9, Pergamon, Oxford, 1991; Integrated Heterocyclic Chemistry, AR Katritzky and CW Rees (eds.) Pergamon, Oxford, 1984, vol. 1-9; Integrated Heterocyclic Chemistry II, AR Katritzky and CW Rees (ed.) Pergamon, Oxford 1996, vol. 1-11; and Organic Reactions, Wiley & Sons: New York, 1991, vol. 1-40. The following synthetic schemes and examples are merely illustrative of some of the methods by which the compounds of the present invention can be synthesized, and various modifications of such synthetic schemes can be performed, and reference is made to the disclosure contained in the present application. Those who are familiar with this art are born out of heart. The starting materials and intermediates of the synthetic reaction scheme can be isolated and purified using conventional techniques, including but not limited to filtration, distillation, crystallization, chromatography, and the like. Such materials can be characterized using conventional methods, including physical constants and spectral data. Unless otherwise stated, the experimental procedure was carried out under the following conditions. The evaporation of the solvent was carried out using a rotary evaporator under reduced pressure (600-4000 kPa: 4.5-30 mm Hg) at a bath temperature of 60 ° C. Unless otherwise indicated, the reaction is typically carried out under nitrogen atmosphere at ambient temperature. Anhydrous solvents such as THF, DMF, Et2®, DME and sputum are commercially available. The reagents were commercial grade and used without further purification. Rapid-type chromatography 143482-1 -52- 201111364 is operated on Shishijiao (collar net). The reaction is traced by (tetra) layer chromatography (TLC) or nuclear magnetic resonance (NMR) spectrometry, and the reaction time is merely illustrative. The structure and purity of all final products were determined by TLC, mass spectrometry, and high pressure liquid chromatography (Η·). Chemical symbols have their usual meanings. The following abbreviations have also been used: v (volume), W (weight), bP (boiling point), mP (melting point), L (liter), chaos (ml), g (g), mg (mg) 'mol (mo Ear), Congyi 1 (millimeter), called (equivalent).

除非另有指明’否則下文所提及之全部變數均具有如上文 所提供之意義。All variables mentioned below have the meaning as provided above unless otherwise indicated.

盥一般而言,本發明化合物可經由經適當取代之吡啶酮工 與經適當官能基化之胺π之偶*,接著自醯胺m移除B〇c_ 保護基而製成(圖式1)。 圖式1In general, the compounds of the present invention can be prepared via the appropriately substituted pyridone and the appropriately functionalized amine π, followed by the removal of the B〇c_ protecting group from the guanamine m (Figure 1). . Figure 1

必要吨。定酮I之合成可例如按圖式2中所舉例進行。典型 上’製自已知三氟曱烷磺酸鹽V之二羥基硼烷酯刃(例如 1434S2-1 .53- 201111364Necessary tons. The synthesis of the ketone I can be carried out, for example, as exemplified in Scheme 2. Typically, it is prepared from a dihydroxy borane ester blade of known trifluorosulfonate V (e.g., 1434S2-1.53-201111364)

Ujjarnwalla 等人,Bioorg. Med. Chem. Lett. ; 15 (18),2005,第 4〇23- 4028頁)與鹵化物vn之金屬催化Suzuki偶合,可提供a,沒_不 飽和酯VIII ^雙鍵之還原作用;最合宜地使用鎂或釤碘化 物達成,及後續鹼所媒介之平衡,係接著獲得飽和酯IX, 為單一非對映異構物。其轉化成相應之吡啶酮x可在兩步 驟中,經由酯IX以mCPBA;或等量氧化劑,接著為所形成 之吡啶N-氧化物與TFAA在三乙胺中之反應;或等量重排促 進劑之最初處理而實現。或者,對於酯ιχ之v基團為〇Bn 之情況,在典型條件下之簡單氫化作用係直接獲得吡啶酮 而且’對於酯IX之V基團為OMe之情況,於蛾化納存在 下’與烧基鹵化物之反應係獲得吡啶酮χι。事實上吾人 亦可經由吡啶酮X以適當試劑之N烷基化作用獲取沿。最 谈’ 11比啶酮XI之皂化作用係獲得吡啶酮j。 143482-1 -54· 201111364 F3c- ,s* 圖式2 M^^Me ΊνUjjarnwalla et al., Bioorg. Med. Chem. Lett.; 15 (18), 2005, pp. 4-23- 4028) Metal-catalyzed Suzuki coupling with halide vn provides a, non-unsaturated ester VIII ^ double The reduction of the bond; the most convenient use of magnesium or hydrazine iodide to achieve the equilibrium of the subsequent base, followed by the acquisition of the saturated ester IX as a single diastereomer. Conversion to the corresponding pyridone x can be carried out in two steps, via ester IX with mCPBA; or an equivalent amount of oxidizing agent, followed by reaction of the formed pyridine N-oxide with TFAA in triethylamine; or equivalent rearrangement This is achieved by the initial treatment of the accelerator. Alternatively, in the case where the v group of the ester oxime is 〇Bn, the simple hydrogenation under typical conditions is the direct obtaining of the pyridone and the case where the V group of the ester IX is OMe, in the presence of moth The reaction of the alkyl halide is obtained as a pyridone oxime. In fact, we can also obtain the edge via the alkylation of pyridone X with an appropriate reagent. The most important saponification of 11 is pyridine ketone to obtain pyridone j. 143482-1 -54· 201111364 F3c- ,s* Figure 2 M^^Me Ίν

Ό O (^V^OEtΌ O (^V^OEt

.Λ Me N#ΛΛ) V 〇、B'〇0.Λ Me N#ΛΛ) V 〇, B'〇0

OEt VII VI R2v.Ns R2^NsOEt VII VI R2v.Ns R2^Ns

RiRi

OEtOEt

Me NίίΛΛ) XIMe N ίίΛΛ) XI

R3 γ 〇 Me^O^OR3 γ 〇 Me^O^O

X R2^N^V U = Br, I V = H,OMe, OBn V = H, OBnX R2^N^V U = Br, I V = H,OMe, OBn V = H, OBn

V = OMe 關於I製備中所使用之鹵化物VII,其中v為0Me或〇Bn, 其合成可極其容易地自其相應之吡啶酮XIV達成。例如, 此轉變可經由使吡啶酮XIV與曱基或芊基鹵化物,於碳酸 銀存在下反應而達成(圖式3)。對於吡啶酮XIV既非市購可 知亦非文獻上已知之情況,此必要化合物可經由峨。定义氧 化物XIII之中介,製自其相應之p比咬ΧΙΙ。 圖式3V = OMe Regarding the halide VII used in the preparation of I, wherein v is 0Me or 〇Bn, the synthesis can be achieved extremely easily from its corresponding pyridone XIV. For example, this transformation can be achieved by reacting pyridone XIV with a mercapto or fluorenyl halide in the presence of silver carbonate (Figure 3). For the case where pyridone XIV is neither commercially available nor known in the literature, the essential compound can be passed via hydrazine. Define the intermediary of oxide XIII, made from its corresponding p-bite. Figure 3

R2\^NR2\^N

U XII 〇㊀U XII 〇一

u XIII R2^n^ou XIII R2^n^o

u XIV U = Br,l V = OMe, OBn r2^n.u XIV U = Br, l V = OMe, OBn r2^n.

uu

VII 在大部份情況中,關於製備圖中所使用之胺n之途徑 143482-1 •55· 201111364 已被揭示於已公告之專利申請案w〇2〇〇7/〇〇925〇ai中。非已 知者可根據例如圖式4中所舉例之方法合成。在適當情況 下’醛XV係首先以區域選擇性方式漠化。然後,使所形成 之溴化物XVI接受一般還原胺化條件,而得胺。若必 要,則胺XVI1可接著被保護成其相應之N.BQC衍生物XVIII。 使用典型金屬所媒介之偶合,譬如Suzuki或Bu—触吨 U 1使胺ιι中之R鍵附加至胺χνπ或胺χνιπ上。於必 要時’可進行簡單化學改質’譬如氫化作用、·啦稀化作 用、還原作用、醯化作用、臭氧分解、氧化作用及其他作# 用,以達成胺II中之所要R基團。最後,關於胺χιχ,係需 要簡單去除保護步驟。VII In most cases, the route for the preparation of the amines used in the figures 143482-1 • 55· 201111364 has been disclosed in the published patent application w〇2〇〇7/〇〇925〇ai. Non-known persons can be synthesized according to, for example, the method exemplified in Fig. 4. Where appropriate, the aldehyde XV system first desertified in a regioselective manner. The resulting bromide XVI is then subjected to general reductive amination conditions to yield an amine. If necessary, the amine XVI1 can then be protected as its corresponding N.BQC derivative XVIII. Coupling using a typical metal medium, such as Suzuki or Bu-Ten U1, allows the R bond in the amine to be attached to the amine χνπ or amine χνιπ. When necessary, 'simple chemical modification' can be performed, such as hydrogenation, thinning, reduction, deuteration, ozonolysis, oxidation, and other processes to achieve the desired R group in amine II. Finally, with regard to amine χιχ, it is necessary to simply remove the protective step.

R" FT XVR" FT XV

圖式4Figure 4

«為胺π中所見及之另一種常見骨架。此等胺 在八型反應條件下,製自+朵XXI之烧基化作用 寺可再_入進行簡單化學改質,譬如氫化作用 稀化作用、還原作用、酿化作用、臭氧分解、氧化 /、作用以達成胺n中之所要R基團。最後,X紐 143482-1 •56- 201111364 月女化作用係皞得所要之胺n。若啕哚χχι不為市購可得,則 其可經由例如4哚xx之簡單甲醯基化作用獲取,該作于用係 最合宜地以P〇Cl3,在DMF中達成。 ’、«Another common skeleton seen in the amine π. Under the eight-type reaction conditions, these compounds can be re-introduced by a simple chemical modification, such as hydrogenation thinning, reduction, brewing, ozonolysis, oxidation/ And act to achieve the desired R group in the amine n. Finally, X New Year 143482-1 • 56- 201111364 The feminization of the month is the desired amine. If 啕哚χχι is not commercially available, it can be obtained via a simple formazanization of, for example, 4 xx, which is most conveniently achieved with P〇Cl3 in DMF. ’,

關於在六氫吡啶環之位置4上帶有烷氧基之本發明化合 物,其係最合宜地經由胺Π與片酮酯ΧΧΠΙ間之最初醯胺形 成,接著添加衍生自經適當保護及經適當取代之羥基吡啶 之Gignard試劑而獲取。若必要,則所形成醇χχν之官能基 化作用係先於經保護之羥基吡啶XXVI使用前文所述之化 學轉化成所要之吡啶酮XXVII。最後,B〇C移除可在典型條 件下達成(圖式6)。With respect to the compounds of the invention having an alkoxy group at position 4 of the hexahydropyridine ring, which is most conveniently formed via the initial guanamine between the amine oxime and the ketone ester oxime, followed by addition from appropriate protection and appropriate Obtained as a Gignard reagent substituted with hydroxypyridine. If necessary, the functionalization of the alcohol oxime formed is prior to the conversion of the protected hydroxypyridine XXVI to the desired pyridone XXVII using the chemical techniques previously described. Finally, B〇C removal can be achieved under typical conditions (Figure 6).

143482-1 57- 201111364 圖式6 〇〇143482-1 57- 201111364 Figure 6 〇〇

R2^n_opgR2^n_opg

OEt + ΗΝ,(Ζ)ηΐΥA R3 Ξ〇 r4〇Aa Me^H L Me^J L Me入〇人〇OEt + ΗΝ,(Ζ)ηΐΥA R3 Ξ〇 r4〇Aa Me^H L Me^J L Me into the 〇人〇

N'(Z)n1YAN'(Z)n1YA

XXVIXXVI

XXVII xxvm 代表性環丙基胺結構單位係示於表1中。 表1 化合物 結構 胺1 Άα 胺2 Η ψ OMeThe representative cyclopropylamine structural unit of XXVII xxvm is shown in Table 1. Table 1 Compound Structure Amine 1 Άα Amine 2 Η ψ OMe

143482-1 -58- 201111364143482-1 -58- 201111364

化合物 結構 胺3 A.Compound structure amine 3 A.

CICI

胺7 胺8 胺9 胺10 胺11 胺12 143482-1Amine 7 amine 8 amine 9 amine 10 amine 11 amine 12 143482-1

MeMe

A.A.

MeMe

OMe A.OMe A.

OMe s 〇 A.OMe s 〇 A.

ClCl

Cl 〇Me OMe OMe H OMe OMe CN 化合物 結構 胺6 、兮°' ^OMe 胺14 Me〇2C> 胺15 Ί OMe 胺16 HN 丫。 OMe 胺17 Ά 胺18 胺19 ΆΝ -59- 201111364Cl 〇Me OMe OMe H OMe OMe CN Compound Structure Amine 6, 兮°' ^OMe Amine 14 Me〇2C> Amine 15 Ί OMe Amine 16 HN 丫. OMe amine 17 Ά amine 18 amine 19 ΆΝ -59- 201111364

化合物 結構 胺20 Άν 胺30 匕CN 胺31 ^^〇Me 胺32 k^N^Me 〇 胺33 胺34 A Nn—,〇Me 胺35 人XV V-CF3 胺36 HN^Y\J A Vy^CF3 143482-1 ·60· 201111364Compound structure amine 20 Άν amine 30 匕CN amine 31 ^^〇Me amine 32 k^N^Me guanamine 33 amine 34 A Nn-, 〇Me amine 35 human XV V-CF3 amine 36 HN^Y\JA Vy^CF3 143482-1 ·60· 201111364

化合物 結構 胺28 ^K^nrBr OMe 胺29 HN—OMe 胺39 入 Nv^cf3 cf3 胺40 A ^NH 胺41 Ηϊ^χΡ A ^NH 〇^Et 胺42 Axv HN-f〇 Me 胺43 HN^rrO 人 HN--f〇 Et 胺44 A 化合物 結構 胺37 ηγτΡ Δ ^s^y^Me 胺38 A L.Vy-〇Et 胺47 A 胺48 \^N 胺49 ηϊΎΡ A Ns> 胺50 HrtP Ns>c 胺51 κ ^ F 胺52 λ 4 Cl 143482-1 • 61 - 201111364 化合物 結構 化合物 結構 胺45 胺53 ΗΝ^ττΟ CN 胺46 胺54 A^q Me 胺55 F AXn^ ^-〇Me 胺63 Cl. HN^VV^ ΑχΝζ V〇Me 胺56 A^o 胺64 Cl, 胺57 A n-q F 胺65 BrV\ hn^yv) A^o 胺58 Mev^\ 胺66 BrV\ HN^TV) F 胺59 NCWx HN^rAJ A^o 胺67 h〇cP A ^-~〇Me 胺60 hn^AJ^ 胺68 A ΙνΓ 143482-1 -62- 201111364Compound structure amine 28 ^K^nrBr OMe amine 29 HN-OMe amine 39 into Nv^cf3 cf3 amine 40 A ^NH amine 41 Ηϊ^χΡ A ^NH 〇^Et amine 42 Axv HN-f〇Me amine 43 HN^rrO Human HN--f〇Et Amine 44 A Compound Structure Amine 37 ηγτΡ Δ ^s^y^Me Amine 38 A L.Vy-〇Et Amine 47 A Amine 48 \^N Amine 49 ηϊΎΡ A Ns> Amine 50 HrtP Ns> c amine 51 κ ^ F amine 52 λ 4 Cl 143482-1 • 61 - 201111364 Compound structure compound structure amine 45 amine 53 ΗΝ^ττΟ CN amine 46 amine 54 A^q Me amine 55 F AXn^ ^-〇Me amine 63 Cl HN^VV^ ΑχΝζ V〇Me Amine 56 A^o Amine 64 Cl, Amine 57 A nq F Amine 65 BrV\ hn^yv) A^o Amine 58 Mev^\amine 66 BrV\ HN^TV) F Amine 59 NCWx HN^rAJ A^o Amine 67 h〇cP A ^-~〇Me Amine 60 hn^AJ^ Amine 68 A ΙνΓ 143482-1 -62- 201111364

化合物 結構 胺61 F 胺62 ΑχΝζ V〇Me 胺71 Me HN 八YVMe A y 胺72 Cl hn^yS A V 〇-v^OMe 胺73 HpDO 胺74 ΗΓΡ scf3 胺75 SMe HN 〜 A Y 胺76 HN^^V¾γBr A γΜβ ^^OMeCompound structure amine 61 F amine 62 ΑχΝζ V〇Me amine 71 Me HN 八 YVMe A y amine 72 Cl hn^yS AV 〇-v^OMe amine 73 HpDO amine 74 ΗΓΡ scf3 amine 75 SMe HN ~ AY amine 76 HN^^V3⁄4γBr A γΜβ ^^OMe

143482-1 63- 201111364143482-1 63- 201111364

化合物 結構 化合物 結構 胺77 〇Me ΗΝ^Τ^Γ a y ^^OMe 胺86 HN W/ )> ^OMe 胺78 A Y . ^^OMe 胺87 ΗΝ^τί^νΒΓ A Vmo 胺79 〇Me Br p a y ^^OMe 胺88 HN^T^TBr A ^Me ^^OEt 胺89 HN^ri^VBr A γΜβ ochf2 胺91 TO: l〇rF 胺90 % 胺92 TO! °^aF 【實施方式】 胺1 N-(2,3-二氣苄基)環丙胺 胺1係根據已公告之專利申請案WO 2007/009250 A1中所述 之程序製成。 胺2 N-{[5-氣基-2-(3-曱氧基丙基)-4-吡啶基]甲基}環丙胺 胺2係根據已公告之專利申請案WO 2007/009250 A1中所述 之程序製成。 143482-1 • 64- 201111364 胺3 N-({2-氣基-5-[3-(甲氧基)丙基]苯基}甲基)環丙胺 胺3係根據已公告之專利申請案w〇 2〇〇7/〇〇925〇 A1中所述 之程序製成。 胺4 N-({2-氣基-5-[2-(曱氧基;)乙基]苯基}甲基)環丙胺 胺4係根據已公告之專利申請案w〇 2007/009250 A1中所述 之程序製成。 ®胺5 N-({2,3-二氣-5-[3-(曱氧基丙基)丙基]苯基)曱基)環丙胺 步驟1 : 5-溴基-2,3-二氣苯曱醛 於2,3-二氣苯曱醛(1當量)之TFA溶液(0.38M)中,添加硫酸 (5當量)。歷經3小時期間,在室溫下分次添加队溴基琥珀 醯亞胺(1.5當量)’最終獲得黃橘色溶液。於%小時後,將 粗製反應混合物以9:1 (v/v)己燒:趟稀釋,然後以水、in NaOH φ 水溶液、水及鹽水相繼洗滌。使有機萃液以Na2S04脫水乾 燥,過濾’並使濾液在真空中濃縮,而得標題化合物,為 白色固體。 步驟2 : N-[(5-溴基-2,3-二氣笨基)曱基]環丙胺 將得自前一步驟之5-溴基-2,3-二氣苯曱醛(1當量)與環丙 基胺(2當量)合併於CH2C12(0.1M)中。然後,於其中添加Compound Structure Compound Amine 77 〇Me ΗΝ^Τ^Γ ay ^^OMe Amine 86 HN W/ )> ^OMe Amine 78 AY . ^^OMe Amine 87 ΗΝ^τί^νΒΓ A Vmo Amine 79 〇Me Br pay ^ ^OMe Amine 88 HN^T^TBr A ^Me ^^OEt Amine 89 HN^ri^VBr A γΜβ ochf2 Amine 91 TO: l〇rF Amine 90 % Amine 92 TO! °^aF [Embodiment] Amine 1 N- (2,3-Dimethylbenzyl)cyclopropylamine 1 is made according to the procedure described in the published patent application WO 2007/009250 A1. Amine 2 N-{[5-Alkyl-2-(3-decyloxypropyl)-4-pyridyl]methyl}cyclopropylamine 2 is according to the published patent application WO 2007/009250 A1. The program is made. 143482-1 • 64- 201111364 Amine 3 N-({2-carbyl-5-[3-(methoxy)propyl]phenyl}methyl)cyclopropylamine 3 is based on the published patent application w It is made by the procedure described in 〇2〇〇7/〇〇925〇A1. Amine 4 N-({2-carbyl-5-[2-(decyloxy))ethyl]phenyl}methyl)cyclopropylamine 4 is according to the published patent application w〇2007/009250 A1 The program is made. ®amine 5 N-({2,3-dioxa-5-[3-(methoxypropyl)propyl)phenyl)indolyl)cyclopropylamine Step 1: 5-bromo-2,3-di Gasbenzaldehyde was added to a solution of 2,3-dioxabenzaldehyde (1 equivalent) in TFA (0.38 M) with sulfuric acid (5 eq.). Over a period of 3 hours, the bromo amber imine (1.5 equivalents) was added in portions at room temperature to finally obtain a yellow orange solution. After % hours, the crude reaction mixture was diluted with 9:1 (v/v) hexane: hydrazine and washed successively with water, in NaOH φ aqueous solution, water and brine. The organic extract was dried with EtOAc (EtOAc m. Step 2: N-[(5-Bromo-2,3-dioxa)indolyl]cyclopropylamine will be obtained from the previous step of 5-bromo-2,3-dibenzoquinone (1 equivalent) Combined with cyclopropylamine (2 equivalents) in CH2C12 (0.1 M). Then add it to it

(1當量),並將所形成之懸浮液在室溫下攪拌18小時。接著, 將不溶物經由過濾’經過矽藻土墊移除,且使渡液在真空 中濃縮。然後’使如此獲得之粗製亞胺再溶於THF : MeOH 143482-1 -65· 201111364 之2.1 (v/v)混合物(0.17M)中。於此;谷液中’分次添加硼氫化 鈉(10當量),並將所形成之混合物在室溫下攪拌48小時。 以IN HC1水溶液使反應淬滅,以IN NaOH水溶液中和,且以 醚萃取。接著’將合併之有機萃液以水與鹽水洗務,以 NasSO4脫水乾燥,過濾,及使濾液在真空中濃縮。如此獲 得之粗產物經由急驟式層析之純化(Si〇2,己烷—1:1 (v/v)己 烷:EtOAc),獲得標題化合物,為無色油。 步驟3 : N-({2,3-二氣-5-[(1E)-3_(甲氧基H•丙烯·Η]苯基}甲基) 環丙胺 將得自前一步驟之Ν-[(5-漠基·2,3_二氣苯基)甲基]環丙胺(1 當量)與4,4,5,5_四甲基_2_[(1Ε)各(曱氧基Η丙烯]基] 氧侧伍園α.5當量)合併於DMF: n_Pr〇H之5:1 (v/v)混合物 (0.17M)中。然後’於此溶液中,添加反式雙(三苯鱗鳩化 鈀量),並將容器重複抽氣,且以氮逆充填。最後, 添加2NNa2C〇3水料(2當量),並將㈣成之兩相懸浮液在 9(TC下加熱8小時。使目前黑色懸浮液冷卻至室溫以水稀 釋且以驗十取。接著,將合併之有機萃液以以Na〇H水溶 液、水及鹽水進一步法游·。妙' 祕 ..^ 无心然後,使其以Na2S04脫水乾燥, 過;慮及使;慮液在真空中濃縮,而得黏稠紅色油。如此押 得之粗產物經由急驟式層析之純化(Si〇2,己炫—3:7(v/v)己 烷:EtOAc),獲得標題化合物,為黃色油。 步驟4 :胺5 便付目刖一步驟之N-(丨2,3- 、1 --肌·J-LUt)-3-(甲氧基)-1-丙太 基]本基}曱基)-環丙胺(1告吾〉1Λ^ U田置)與10% w/w鈀/炭(0.1當量 143482-1 -66- 201111364 浮於EtOAc (0.03M)中。然後’將容器抽氣,並以h2蘇氣。在 經充填H2大氣之氣瓶下,將反應懸浮液於室溫下授拌2小 時。接著’以CI^Cl2使反應淬滅’經過矽藻土床過據,且 使濾液在真空中濃縮。如此獲得之粗產物經由急驟式層析 之純化(Si〇2 ’己烧—1:1 (v/v)己烧:EtOAc),獲得標題化合 物,為無色油。 胺6 1^-({2,3-二氯-5-[2-(曱氧基)乙基]苯基}甲基)環丙胺 * 步驟1 : [(5-漠基_2,3_二氯苯基)甲基]環丙基胺基甲酸u_二甲 基乙酯 將得自胺5步驟2之N-[(5-漠基-2,3-二氯苯基)甲基]環丙胺 (1 ‘里)與二碳酸二-第三_ 丁酯q J當量)合併於CH2Cl2 (〇’17M)中。然後,於此溶液中,添加Hunig氏驗(1.2當量), 並將所形成之黃色溶液在室溫下攪拌3小時。接著,將反應 混合物以醚稀釋,且以水與鹽水相繼洗滌。然後,使有機 • 層以Na2S〇4脫水乾燥,過濾’並使濾液在真空中濃縮,而 得汽色油。如此獲得之粗產物經由急驟式層析之純化 (Sl〇2,己烷―3:7 (v/v)己烷:EtOAc),獲得標題化合物,為 無色油。 v驟2 . %、丙基[ο二氣乙烯基苯基)曱基]胺基曱酸丨,丨二 曱基乙I旨 將得自前一步驟之[(5-漠基-2,3-二氯苯基)甲基]環丙基胺 基甲酸U-二曱基乙酯(1當量)與2-乙烯基-4,4,5,5-四曱基 1,3,2-_氧硼伍園(1當量)合併於: n_pr〇H之2:1 (v/v)混合 143482-1 -67- 201111364 物(0.1M)中。然後’於此溶液中,添加醋酸I巴(π) (〇 〇5當量) 與三笨膦(〇·15當量)’接著將容器重複抽氣,並以氮逆充填。 最後’添加2Ν NafO3水溶液(2當量),且將所形成之兩相懸 浮液在90°C下加熱18小時。使目前黑色懸浮液冷卻至室溫, 以水稀釋,並以1:1 (v/v)己烷:醚萃取。然後,將合併之有 機萃液以IN NaOH水溶液、水及鹽水進一步洗滌。接著,使 其以Na2S〇4脫水乾燥’過濾,及使濾液在真空中濃縮,而 得淡黃色油。如此獲得之粗產物經由急驟式層析之純化 (Si〇2,己烷—9:1 (Wv)己烷:Et0Ac),獲得標題化合物,為 無色油。 步驟3 :環丙基{[2,3-二氯-5-(2-羥乙基)苯基]甲基丨胺基曱酸u_ 一曱基乙画旨 將得自前一步驟之環丙基[(2,3_二氣乙烯基苯基)曱基] 胺基甲酸1,1-二甲基乙酯(1當量)、[Ir(c〇D)cl]2(〇 〇25當量)及 DPPB(〇.〇5當量)合併於THF(〇nM)中。然後,於此溶液中, 添加4,4,5,5-四曱基-l,3,2-二氧硼伍圜(1.3當量),並將所形成之 、,’工色〉谷液在室溫下攪拌12小時。最後,添加過硼酸鈉(〇.1M 水溶液,1當量),且將目前黑色兩相溶液於室溫下再激烈 攪拌12小時。分離水層,並以醚逆萃取。接著,將合併之 有機萃液以IN NaOH水溶液、水及鹽水進一步洗滌。然後, 使其以NasSO4脫水乾燥,過濾,及使濾液在真空中濃縮, 而得淡黃色油。如此獲得之粗產物經由急驟式層析之純化 (Si〇2,9:1 _ 己烷:Et〇Ac— 3:7 (v/v) Et〇Ac ··己烷),獲得標 題化合物,為無色油。 143482-1 •68- 201111364 步驟4 :環丙某(72 3 g c m ^ (丨氣·5_[2-(甲氧基)乙基]苯基}甲基)胺基 甲酸1,1-二甲基乙酯 使%丙基{[2,3-二氯!(2_羥乙基)苯基]甲基}胺基甲酸u_ 二甲基乙酉旨(1當量)溶於THF(〇3M)tj7。然後,於此溶液中, 添加氫化鈉(在油中之⑼% w/w分散液,i當量),並將所形 成之憨淨液在至/凰下攪拌5分鐘。最後,添加蛾曱炫(1〇當 罝)’且將目前淡黃色溶液在黑暗中,於室溫下再攪拌10 φ 小時。接著,於真空中移除揮發性物質,並使所形成之殘 留物於驗與1NHC1水溶液之間作分液處理。分離水層,並 以醚逆萃取。然後,將合併之有機萃液以in 水溶液、 水及鹽水進-步洗鲦。接著,使其以Na2S〇4脫水乾燥,過 濾,及使濾液在真空中濃縮,而得標題化合物(被油污染), 為淡黃色油。 步驟5 :胺6 使得自前一步驟之環丙基({2,3_二氣_5_[2_(甲氧基)乙基]苯 • 基}甲基)胺基甲酸U_二曱基乙酯(1當量)溶於CH2C12(0.1M) 中。然後,於此溶液中,添加HC1 (40m,在二氧陸園中, 30當量),並將所形成之溶液在室溫下攪拌2小時。接著, 以IN NaOH水溶液使反應淬滅,且以醚萃取。然後,將人併 之有機萃液以水與鹽水進一步洗滌,以Na2S〇4脫水乾燥, 過濾,及使濾液在真空中濃縮。如此獲得之粗產物經由急 驟式層析之純化(Si02,9:1 (ν/v)己烷:Et〇Ac— Et〇Ac),獲得 標題化合物’為無色油。 胺7 143482-1 -69- 201111364 N-(2-曱基-5-[3-(曱氧基)丙基]苯基}曱基)環丙胺 步驟1 : 5-氣-N-環丙基-2-甲基笨曱醯胺 在0C下,於5-氣基-2-曱基笨甲酸(1當量)與DMF(l2當量) 之曱苯溶液(1M)中,逐滴添加氣化草醯(ι 2當量),歷經丄小 時。將所形成之溶液於〇t下搜拌2小時,然後在真空中移 除揮發性物質。使所形成之殘留物溶於二氣甲烷⑽中, 冷卻至o°c,並相繼地逐滴添加環丙基胺(15當量)與Hunig 氏鹼(2當量)。將所形成之懸浮液在室溫下攪拌18小時。以 IN HC1水溶液使反應淬滅,且以二氯曱烷萃取。使合併之 有機萃液以MgS〇4脫水乾燥,過濾,及使濾液在真空中濃縮 至〜1/3份體積。於所形成之白色懸浮液中,添加相等體積 之己烧’並將標題化合物經由真空過濾單離。 步驟2 : N-[(5-氣基-2-曱基苯基)甲基]環丙胺 在〇°C下,於得自前一步驟之5_氯_N_環丙基_2_甲基苯甲醯 胺(1當量)在THF (0.4M)中之懸浮液内,添加硼烷(1 〇M,在 THF中,3當量)。使所形成之懸浮液溫熱至室溫,歷經工小 時,然後於回流下加熱1小時。使目前淡黃色溶液再冷卻至 〇 C,並以IN HC1水溶液小心地使反應淬滅。將所形成之混 合物於回流下加熱1小時,以確保胺_棚烷複合物之完全分 解。在以IN NaOH水溶液小心中和之後,分離水層,並以 EtOAc逆萃取。將合併之有機萃液以鹽水洗滌,以MgSa^ 水乾燥’及過濾。使濾液在真空中濃縮,並使如此獲得之 粗產物經由急驟式層析進一步純化(Si〇2,己烷—4:1 (v/v)己 烧:Et2 0),以顯示標題化合物,為無色油。 143482-1 ► 70- 201111364 步驟3 : [(5-氣基-2-甲基苯基)曱基]環丙基胺基曱酸ι,ΐ-二甲基 乙酯 在-78°C下,於得自前一步驟之N_[(5-氣基_2_甲基苯基)甲基] 環丙胺(1當量)之THF溶液(0.3M)中,添加六甲基二矽氮化鉀 (0.5M ’在曱苯中,1.2當量)。於-78°C下攪拌1小時後,添加 一奴• — -第二-丁自旨(1.1當1)’並使所形成之混合物慢慢溫 熱至室溫’歷經2小時。以飽和NH4C1水溶液使反應淬滅, φ 然後以醚萃取。將合併之有機萃液以鹽水洗滌,以MgS04 脫水乾燥’過濾,及使濾液在真空中濃縮。經由急驟式層 析之進一步純化(Si〇2,己烷—4:1 (v/v)己烷:Et20),獲得標 題化合物,為淡黃色油。 步驟4 :環丙基({2-曱基-5-[(1Ε)-3-(甲氧基)-1-丙烯-1-基]苯基} 甲基)胺基甲酸1,1-二曱基乙酯 將得自前一步驟之[(5-氣基-2-曱基苯基)甲基]環丙基胺基 .曱酸1,1-二曱基乙酯(1當量)與4,4 5,5_四曱基_2 [(1e) 3 (曱氧 • 基)小丙稀-1·基Η,3,2·二氧硼伍園(1當量)合併於n-BuOH (0.48M)中。然後,於此溶液中,添加參(二苯亞曱基丙酮) 二鈀(〇)氣仿加成物(0.02當量)、[2,,6,-雙(曱氧基)-2-聯苯基](二 環己基)碟烷(〇.〇8當量)及粉末狀磷酸鉀(2當量)。將容器重 複抽氣,並以氮逆充填,接著,將所形成之懸浮液在1〇〇。〇 下加熱16小時。使目前黑色懸浮液冷卻至室溫,以Et〇Ac 稀釋,且經過Si〇2塾片過渡。然後,使濾液在真空中濃縮, 並使如此獲得之粗產物經由急驟式層析直接地接受純化 (Si〇2,己烷—3:7 (v/v)己烷:Et〇Ac)。標題化合物係被單離 143482-1 -71 - 201111364 成淡黃色油。 步驟5.裱丙基({2-甲基·5_[3_(曱氧基)丙基]苯基}曱基)胺基曱 酸1,1_·一曱基乙酉旨 使付自前一步驟之環丙基({2甲基_5 [(1Ε)_3 (曱氧基H-丙 烯小基]苯基}曱基)胺基曱酸1,1-二曱基乙酯(1當量)與10% w/w鈀/炭(0.1當量)懸浮於Et〇Ac(〇〇8M)中。然後,將容器抽 氣,並以H2滌氣。在經充填%大氣之氣瓶下,將反應懸浮 液於室溫下攪拌2小時。接著,以CH2Cl2使反應淬滅,經過 矽藻土床過濾,及使濾液在真空中濃縮。如此獲得之粗產 物經由急驟式層析之純化(Si〇2,己烷—1:1 (v/v)己烷: EtOAc) ’獲得標題化合物,為無色油。 步驟6 :胺7 使得自前一步驟之環丙基({2_曱基_5_[3(曱氧基)丙基]苯 基}曱基)胺基曱酸1,1_二曱基乙酯(1當量)溶於CH2Cl2(〇1M) 中。然後,於此溶液中,添加HC1 (4 〇M,在二氧陸園中, 30當量),並將所形成之溶液在室溫下攪拌2小時。接著, 以INNaOH水溶液使反應淬滅,且以醚萃取。然後,將合併 之有機萃液以水與鹽水進一步洗滌,以Na2S04脫水乾燥, 過濾’及使濾液在真空中濃縮。如此獲得之粗產物經由急 驟式層析之純化(Si〇2 ’ 9:1 (v/v)己烷:EtOAc— EtOAc),獲得 標題化合物,為無色油。 胺8 N-({2-甲基-5-[2-(甲氧基)乙基]笨基}甲基)環丙胺 胺8係根據胺6中所述之程序製成,但替代地使用得自胺 143482-1 -72- 201111364 7步驟3之[(5-氣基-2-曱基笨基)甲基]環丙基胺基曱酸以-二 曱基乙酯作為受質,n-BuOH作為溶劑,參(二苯亞曱基丙酮) 二鈀⑼氣仿加成物作為鈀來源,[2,,6,-雙(甲氧基)_2-聯笨 基](二環己基)填烷作為配位體,及粉末狀磷酸鉀作為鹼, 用於Suzuki偶合(步驟2)。 胺9 N-({2,3-二氟-5-[3-(甲氧基)丙基]苯基丨曱基)環丙胺 鲁 胺9係根據胺5中所述之程序製成,但替代地使用2,3_二氟 苯曱醛作為起始物質。 胺10 N-({3-(曱氧基)-5-[3-(甲氧基)丙基]笨基丨曱基)環丙胺 步驟1 : 3-溴基-5-羥基苯曱醛 在-10 C下,於正-丁基鋰(2.5M,在己烷中,2.1當量)之甲 苯溶液(1.6M)中,添加正-丁基氣化鎂(2 〇M ’在THF中,〇 6 當i )。將反應混合物在-l〇°C下授拌3〇分鐘,然後於下, % 逐滴添加3,5_二溴酚(1當量)之曱苯溶液(0.7M),歷經35分鐘 期間。於-10 C下再攪拌30分鐘後,使反應混合物冷卻至_4〇 C,接著逐滴添加DMF (20當量),歷經2〇分鐘《然後,使 反應混合物慢慢地溫熱至室溫,並將其在室溫下攪拌i小 時。於〇°C下,以1ΝΗα水溶液小心地使反應淬滅,且以醚 卒取。將合併之有機萃液以水與鹽水洗滌,以MgS〇4脫水乾 燥,及過滤。渡液在真空中之濃縮,獲得黃色固體。如此 獲得之粗產物自己烷之再結晶化作用,獲得標題化合 物,為米黃色粉末。 143482-1 -73- 201111364 步驟2 : 3-經基-5-[(1Ε)-3-(曱氧基)-1-丙稀小基]苯曱酸 將得自前一步驟之3-溴基-5-羥基苯曱醛(1當量)與 3-曱氧基丙-1-烯-1-基]-4,4,5,5-四曱基-二氧硼伍園(1當量) 合併於DMF(0.05M)中。然後,於此溶液中,添加醋酸鈀(〇ι 當里)、二本鱗(0.2當直)及2M碳酸納水溶液(4當量)。將所 形成之懸浮液在80°C下加熱16小時。以1N hci水溶液使反 應混合物淬滅,並以醚萃取。將合併之有機萃液以水、飽 和NaHC〇3水溶液及鹽水洗滌。以MgS〇4脫水乾燥過淚, 及濾液在真空中之濃縮,獲得粗產物,為褐色焦油。經由 急驟式層析之進一步純化(Si〇2,4:1 (v/v)己烷:Et0Ac— 2:1 (v/v)己烷:EtOAc) ’獲得標題化合物,為黃色油。 步驟3 : 3-(甲氧基)-5-[(1Ε)-3-(甲氧基)-1-丙小稀+基]苯甲盤 將得自前一步驟之3-羥基-5-[(1Ε)-3-(甲氧基)+丙烯小基]苯 甲醛(1當量)與碘曱烷(2_2當量)合併於丙酮(〇 〇7M)中。然 後,於此溶液中,添加碳酸鉀(2當量),並將反應懸浮液於 回流下加熱16小時。使所形成之反應混合物在真空中濃 縮’且使殘留物於水與醚之間作分液處理。分離含水洗液, 並以謎逆萃取。將合併之有機萃液以鹽水進一步洗務,以 MgS〇4脫水乾燥,過濾,及使濾液在真空中濃縮。如此獲得 之粗產物經由急驟式層析之進一步純化(§i〇2,19:i (v/v)己 烷:EtOAc—1:1 (v/v)己烷:a0Ac),獲得標題化合物為黃 色油。 步驟4 : N-({3-(甲氧基)_5_[(1e)-3-(曱氧基)小丙烯巧·基]苯基}曱 基)-環丙胺 143482-1 • 74· 201111364 於知自别一步驟(1當量)之3_(甲氧基)_5 [⑽_3 (甲氧基W 丙-1-烯·1-基]苯甲醛(1當量)在二氯甲烷(〇5M)中之溶液内, 添加%丙基胺(2當量)與硫酸鎂(15當量)。將所形成之懸浮 液在室溫下攪拌12小時。經由過濾移除不溶物。濾液在真 空中之濃縮,獲得粗製亞胺,為黃色油。然後,使其溶於 甲醇(0.3M)中,接著在〇。〇下,分次添加硼氫化鈉(1 5當量), 歷經5分鐘。使反應混合物慢慢溫熱至室溫,歷經丨小時, 然後於至溫下攪拌2小時。以飽和NaHC03水溶液小心地使 反應序滅後’將所形成之混合物以喊萃取。將合併之有機 萃液以水與鹽水洗滌,以MgS〇4脫水乾燥,及過濾。濾液在 真空中之濃縮’獲得標題化合物,為金黃色油。 步驟5 :胺10 於得自前一步驟之N-({3-(甲氧基)-5-[(ie)-3-(甲氧基)-1-丙烯 -1-基]苯基}曱基)環丙胺(1當量)在Et0Ac (〇 〇4M)中之溶液内, 添加鈀(10%w/w,於活化碳上,αι當量)^將容器抽氣,並 φ 以氩回填。然後,將反應懸浮液在氫氣瓶大氣下攪拌L5小 時。以二氯甲烷使反應淬滅,並經過矽藻土床過濾。將不 溶物以EtOAc與曱醇進一步洗滌。濾液在真空中之濃縮,獲 得標題化合物,為無色油。 胺11 N-({3-{[2-(甲氧基)乙基]氧基卜5_[3-(曱氧基)丙基]苯基丨甲基)環 丙胺 胺11係根據胺10中所述之程序製成,但於步驟3中,替代 地使用2-溴乙基曱基趟作為烧基化試劑,碳酸絶作為驗, 143482-1 -75- 201111364 及DMF作為溶劑。 胺12 4-{3,4-二氯·5_[(環丙胺基)甲基]苯基丨丁腈 乂驟1環丙基{[2,3-二氯_5-(2-酮基乙基)苯基]甲基丨胺基甲酸 1,1-二甲基乙酉旨 使得自胺6步驟3之環丙基([2,3_二氣_5(2羥乙基)苯基]甲 基}胺基甲酸U-工甲基乙醋(1當量)與碳酸氫納〇當量)懸 浮於叫㈣遍)令。在(TC下,添加DMP (1當量),並將所 形成之混合物於〇t下攪拌15分鐘,然後在室溫下幻分鐘。 以INNaOH水溶液使反應淬滅,且以醚萃取。接著,將合併 之有機萃液以水與鹽水進—步洗務,以邮〇4脫水乾燥, 過濾’及使濾液在真空中濃縮’而得標題化合物,為不安 定無色油。 步驟2 :環丙基({2,3_二氣·5_[(2E)各氰基冬丙烯小基]苯基}甲 基)胺基曱酸1,1-二甲基乙酯 於無水氣化鋰(1.2當量)之THF(0.1M)懸浮液中,相繼地添 加(氰基曱基)膦酸二乙酯(1.2當量)與1)611 (1當量)。將所形 成之懸 &gt;予液在室溫下攪拌15分鐘,然後以THF (〇 im)溶液逐 滴添加得自前一步驟之環丙基{[2,3_二氣_5_(2_酮基乙基)苯 基]甲基}胺基甲酸U-二曱基乙醋(1當量)。將所形成之粉紅 色懸浮液於室溫下攪拌12小時,接著α1ΝΗα水溶液小心 地使反應淬滅,然後以醚萃取,將合併之有機萃液以水與 鹽水進一步洗滌,以N^SO4脫水乾燥,過濾,及使濾液在 真空中濃縮。如此獲得之粗產物經由急驟式層析之純化 1434S2-1 -76- 201111364 (Si〇2,己烷一&gt; 3:7 (v/v)己烷:EtOAc) ’獲得標題化合物,為 無色油。 步驟3:環丙基{[2,3-二氯-5-(3-氰基丙基)苯基]-曱基丨胺基甲酸 U-二曱基乙酯 於得自前一步驟之環丙基({2,3-二氯-5-[(2E)-3-氰基-2-丙稀 -1-基]苯基}曱基)胺基曱酸1,1-二甲基乙Θ旨(1當量)在EtOAc (0.04M)中之溶液内’添加把(10% w/w,於活化碳上,ο]當 量)。將容器抽氣,並以氫回填。然後’將反應懸浮液在氫 籲 氣瓶大氣下攪拌1.5小時。以二氣曱烷使反應淬滅,且經過 矽藻土床過濾。將不溶物以EtOAc進一步洗滌。濾液在真空 中之濃縮,獲得標題化合物,為無色油。 步驟4:胺12 於得自前一步驟之環丙基{[2,3-二氣-5-(3-氰基丙基)苯基] 曱基}胺基甲酸U-二甲基乙酯(1當量)在CH2Cl2(〇 〇6M)中之 溶液内,添加溴化鋅(11)(10當量)^使所形成之懸浮液音振 φ 15分鐘’然後將其在室溫下攪拌18小時。以IN NaOH水溶液 使反應淬滅,接著以EtOAc萃取。將合併之有機萃液以水與 鹽水進一步洗滌,以NhSO4脫水乾燥,過濾,及使濾液在 真空中濃縮。如此獲得之粗產物經由急驟式層析之純化 (Si02,9:1 (V/V)己烷:Et0Ac— 3:7 (v/v)己烷:Et〇Ac),獲得標 ^化合物’為無色油。 胺13 M3-[(環丙胺基)曱基]_4,5_二氟笨基}丁猜 胺U係根據胺12中所述之程序合成,但替代地使用以類 143482-] •77· 201111364 似方式製自2,3-二氟苯曱醛之環丙基{[2,3_二氟_5_(2經乙基) 苯基]曱基}胺基曱酸U-二甲基乙酯。 胺14 4-{3,4-二氯-5-[(環丙胺基)曱基]苯基}丁酸曱酯 胺14係根據胺12中所述之程序製成,但在Wittig稀化作用 步驟(步驟2)中’以(三苯基-入5 _亞磷烷基)醋酸甲酯置換無 水氣化經、(氰基曱基)膦酸二乙酯及DBU。 胺15 N-({3-[3-(曱氧基)丙基]-1-茶基}甲基)環丙胺 步驟1 : 3-[(1Ε)-3-(曱氧基)-1-丙烯小基]小茶羧酸曱醋 將3-溴基-1-苯羧酸曱酯(1當量)與4 4 5 5_四甲基_2耵玛各 (曱氧基)-1-丙烯-1-基]-1’3,2-二氧硼伍園(15當量)合併於 DMF: n-PrOH之5:1 (v/v)混合物(0.2M)中。然後,於此溶液中, 添加反式-雙(三苯膦)演化鈀(IIX0.05當量),並將容器重複抽 氣,且以氮逆充填。最後,添加2NNa2C〇3水溶液(2當量), 並將所形成之兩相懸浮液在9(TC下加熱8小時。使目前黑色 懸浮液冷卻至室溫,以水稀釋,並以1:1(v/v)己烷:醚萃取。 接著’將合併之有機萃液以1N Na〇H水溶液、m Ηα水溶 液、水及鹽水進一步洗滌。然後’使其以~〇4脫水乾燥, 過濾,及使濾液在真空中濃縮,而得標題化合物,為紅色 油0 步驟2 : 3-[3-(曱氧基)丙基]-i_蕃缓酸曱酉旨 使得自前一步驟之3-[(1Ε)-3-(曱氧基)4_丙烯小基H莕羧酸 曱酯(1當量)與10% w/w鈀/炭(αΐ當量)懸浮於Me〇H (〇 〇8M) 143482-1 -78- 201111364 =°然後,將容器抽氣,並以h2蘇氣。在經充填吃大氣之 虱瓶下,將反應懸浮液於室溫下攪拌2小時。接著,以CH2Cl2 使反應淬滅,經過矽藻土床過濾,及使濾液在真空中濃縮。 如此獲得之粗產物經由急驟式層析之純化(Si〇2,己烷—Η (v/ν)己烷:EtOAc),獲得標題化合物,為無色油。 步驟3: 3-[3-(甲氧基)丙基]+萘曱酸 使得自前一步驟之3-[M曱氧基)丙基]小蕃鲮酸甲酯(1當 _ I)溶於Me0H :卿之2:1 (v/v)混合物(0.08M)中。然後,於此 溶液中,添加LiOH (2.0M水溶液,3當量),並將所形成之混 濁洛液在至/JEL下激烈授拌24小時。接著,於真空中移除揮 發性物質,且以1N Ηα水溶液將殘留物之pH值小心地調整 至〜2 ’然後將其以EtOAc萃取。將合併之有機萃液以水與鹽 水進一步洗滌,以Na2S04脫水乾燥,及過濾。濾液在真空 中&lt; /辰、tffi ’獲得標題化合物,為白色固體。 步驟4 : N-環丙基-3-[3-(曱氧基)丙基]-1-莕羧醯胺 • 在0°C下’於得自前一步驟之3_[3_(曱氧基)丙基H_莕曱酸 (1當量)之CH2C12溶液(0.1M)中,添加氣化草醯(1_2當量),接 著為數滴DMF。將所形成之溶液在室溫下攪拌2小時,然後 於真空中移除揮發性物質。使所形成之殘留物溶於二氣曱 淀(0.1M)中,冷卻至〇〇c,並相繼地逐滴添加Hunig氏鹼(1.2 當量)與環丙基胺(U當量)。將所形成之懸浮液在室溫下攪 拌18小時。以IN HC1水溶液使反應淬滅,且以醚萃取。將 合併之有機萃液以IN NaOH水溶液、水及鹽水進一步洗滌, 以Na2S〇4脫水乾燥,及過濾。濾液在真空中之濃縮,獲得 143482-1 79· 201111364 標題化合物,為白色固體。 步驟5 :胺15 在回流下,於得自前一步驟之N_環丙基_3 [3 (曱氧基)丙 基]-1-茶羧醯胺(1當量)之THF溶液(〇·ΐΜ)中,添加硼烷-硫化 曱烷複合物(6.6當量)。將短路徑蒸餾裝置連接至反應容器, 並慢慢地蒸餾出大部份揮發性物質,歷經15小時期間。使 目前黃色溶液再冷卻至〇°C,且以1N HC1水溶液小心地使反 應淬滅。將所形成之混合物於回流下加熱丨小時,以確保胺 -删烷複合物之完全分解。在以1N NaOH水溶液小心中和之鲁 後’分離水層’並以EtO Ac逆萃取。將合併之有機萃液以鹽 水洗滌,以NadO4脫水乾燥,及過濾。使濾液在真空中濃 縮’並使如此獲得之粗產物經由急驟式層析進一步純化 (Si02 ’ 9:1 (v/v)己烧:EtOAc— 3:7 (v/v)己烧:EtOAc),以顯示 標題化合物,為無色油。 胺16 (2-{3,4-二氯-5-[(環丙胺基)甲基]苯基}乙基)胺基曱酸曱酉旨 步驟1 :環丙基[(2,3-二氣-5-曱醯基苯基)曱基]胺基甲酸ι,μ二 甲基乙酯 於得自胺6步驟2之環丙基[(2,3-二氣-5-乙烯基苯基)曱基] 胺基甲酸U-二曱基乙酯(1當量)之二氣甲烷(0.03M)溶液中, 在-78°C下以剛產生之臭氧起泡,直到發現持久藍色為止。 然後,於其中以一快速部份添加三苯膦(1.2當量),並使所 形成之混合物慢慢溫熱至室溫,歷經3小時。在真空中移除 揮發性物質,且將其餘殘留物以2:1 (v/v)己烷:Et20研製。 143482-1 •80· 201111364 經由過ϋ移除不溶物’及使濾液在真空中濃縮。如此獲得 之粗產物經由急驟式層析之純化(Si02,己烷—1:1 (v/v)己 院:EtOAc) ’獲得標題化合物,為無色油。 步驟2 ·被丙基{[2,3~二氣-5-(經甲基)苯基]甲基}胺基甲酸1,1-二甲基乙酯 在0C下,於得自前一步驟之環丙基[(2,3二氣_5甲醯基苯 基)曱基]fe基甲酸二甲基乙酯之甲醇(016M)溶液中,添 加硼氫化鈉(U當量)。將所形成之溶液於〇c&gt;c下攪拌2小時, 然後在真空中移除揮發性物質。接著,使所形成之殘留物 於醚與IN HC1水溶液之間作分液處理。分離水層,並以醚 逆萃取。將合併之有機萃液以水與鹽水進一步洗滌,以 Na2S04脫水乾燥,過濾,及使濾液在真空中濃縮。如此獲 得之粗產物經由急驟式層析之純化(Si〇2,己烷—3:7 (v/v)己 烷:EtOAc),獲得標題化合物,為無色油。 步驟3 :曱烷磺酸{3,4_二氯_5_[(環丙基二甲基乙基)氧基] 羰基}胺基)甲基]苯基}甲酯 在〇°C下,於得自前一步驟之環丙基{[2,3二氣_ 苯基]曱基}胺基曱酸U-二甲基乙酉旨(1當量)在二氣甲烧(〇1M) 中之溶液内,相繼地添加Hunig氏鹼(3當量)與氣化曱烷磺醯 (U當量)。將所形成之溶液於(TC下攪拌30分鐘,然後在室 溫下15分鐘。接著,將反應混合物以醚稀釋並以爪 水溶液小心地使反應淬滅。分離水層,且以醚逆萃取。將 合併之有機萃液以水與鹽水進一步洗滌,以Na2S〇4脫水乾 燥,過濾,及使濾液在真空中濃縮,而得粗製標題化合物, 143482-1 •81- 201111364 為無色油。 步驟4 :環丙基{[2,3-二氣-5-(|L基曱基)苯基]曱基}胺基甲酸 U-二曱基乙酯 於得自前一步驟之曱烷磺酸{3,4-二氣-5-[(環丙基{[(u-二 曱基乙基)氧基]幾基}胺基)曱基]苯基丨曱酯(1當量)在DMS〇 (0.48M)中之浴液内,添加亂化钟(ι·3當量)與填化納(〇 1當 量)。將所形成之溶液於室溫下攪拌3小時,然後將其稀釋 以醚,並以IN NaOH水溶液使反應淬滅。分離水層,且以醚 逆萃取。將合併之有機萃液以水與鹽水進一步洗蘇,以 NaJO4脫水乾燥’過濾,及使濾液在真空中濃縮。如此獲 得之粗產物經由急驟式層析之純化(Si〇2,19:1 (v/v)己烧: EtOAc— 3:7 (Wv)己烷:EtOAc) ’獲得標題化合物,為無色油。 步驟5 : {[5-(2-胺基乙基)-2,3-二氣笨基]曱基}環丙基胺基曱酸 U-二曱基乙酯 在〇°C下,於得自前一步驟之環丙基{[2,3_二氣_5 (氰基甲 基)苯基]曱基}胺基曱酸1,1_二曱基乙酯(1當量)與氣化鈷(灯) 六水合物(2當量)在曱醇(0.07M)中之溶液内,分次添加硼氫 化鈉(10當量)。將所形成之混合物於下攪拌1〇分鐘然 後在室溫下2小時。以INNaOH水溶液使目前褐色懸浮液淬 滅,接著以EtO Ac萃取。將合併之有機萃液以水與鹽水進一 步洗滌,以Naz S〇4脫水乾燥,並經過矽藻土床過濾。濾液 在真空中之濃細’獲得粗製標題化合物,為淡褐色非晶質 固體。 步驟6:環丙基{[2,3-二氣-5-(2-{[(曱氧基)幾基]胺基丨乙基)苯基] 143482-1 •82- 201111364 曱基}胺基曱酸1,1-二曱基乙酯 在〇°C下,於得自前一步驟之{[5-(2-胺基乙基)-2,3-二氣苯 基]甲基}環丙基胺基曱酸1,1-二甲基乙酯(1當量)在二氯曱 烧(0.07M)中之溶液内,相繼地添加Hunig氏鹼(1.2當量)與氣 甲酸甲酯。然後,使所形成之溶液慢慢地溫熱至室溫,歷 經3小時。接著,將粗製反應混合物以醚稀釋,並以1N Na〇H 水溶液、IN HC1水溶液、水及鹽水相繼洗滌。然後,使醚 _ 萃液以Na〗S04脫水乾燥,過濾’及使濾、液在真空中濃縮。 如此獲得之粗產物經由急驟式層析之純化(Si〇2,19:1 (v/v) 己烧:EtOAc— EtOAc),獲得標題化合物,為淡黃色油。 步驟7 :胺16 於得自前一步驟之環丙基{[2,3-二氣-5-(2-{[(曱氧基)数基] 胺基}乙基)笨基]曱基}胺基曱酸1,1_二曱基乙酯(1當量)在 CH2Cl2(〇.〇6M)中之溶液内,添加HC1 (4.0M,在二氧陸園中, 30當量)。將所形成之溶液於室溫下攪摔3小時。然後,以 _ IN NaOH水溶液使反應淬滅,且以鱗萃取。接著,將人併之 有機萃液以水與鹽水進一步洗滌,以Ν%3〇4脫水乾燥,過 濾,及使濾液在真空中濃縮。如此獲得之粗產物經由急驟 式層析之純化(Si〇2,24:1 (v/v) ¢:¾% : MeOH),獲得標題化 合物’為無色油。 胺17 N-(8-4:琳基甲基)環丙胺 於8-喹啉羧甲醛(1當量)之二氣曱烷(〇13M)溶液中,添加 硫酸鎂(1當量)與環丙基胺(2當量)。將所形成之懸浮液在 143482-1 -83- 201111364 室溫下搜摔丨6小時。經由過據移 卜冷物,並以二氮甲炫 沖洗’然後使合併之濾液在真空中、、曲 甲,辰蝻。使如此獲得之粗 製亞胺溶於曱醇(0.13M)中,接著八4、 刀-欠添加爛鱼化钢q 5杳 量)。將反應混合物在室溫下攪拌 虱化納田 溶液使反應淬滅。接著,以1N N」、時,然後謂HC1水 調整至〜1G ’然後將其以醚萃取 ^液將溶液之pH值 鹽水進-步洗滌’以Na2S04脫水浐:併之有機萃液以水與 真空中濃縮’而得粗製標題化合物:過濾’及使濾液在 胺18 ’為黃色油。(1 eq.) and the resulting suspension was stirred at room temperature for 18 h. Next, the insolubles were removed via filtration through a diatomaceous earth pad and the effluent was concentrated in vacuo. The crude imine thus obtained was then redissolved in a 2.1 (v/v) mixture (0.17 M) of THF : MeOH 143482-1 - 65 · 201111364. Here, sodium borohydride (10 equivalents) was added in portions to the solution, and the resulting mixture was stirred at room temperature for 48 hours. The reaction was quenched with aq. The combined organic extracts were then washed with water and brine, dried over NasSO4, filtered, and concentrated. The crude product thus obtained was purified by flash chromatography eluting elut elut elut Step 3: N-({2,3-digas-5-[(1E)-3_(methoxy H•propene·Η]phenyl}methyl)cyclopropylamine will be obtained from the previous step-[( 5-Mosyl·2,3_di-phenyl)methyl]cyclopropylamine (1 eq.) and 4,4,5,5-tetramethyl-2-[[1](曱 Η Η) ] Oxygen side garden α.5 equivalent) was combined in DMF: n_Pr〇H in a 5:1 (v/v) mixture (0.17M). Then, in this solution, trans bis (triphenyl sulfonate) was added. Palladium amount), and the vessel was repeatedly evacuated and backfilled with nitrogen. Finally, 2NNa2C〇3 water (2 equivalents) was added, and the (IV) two-phase suspension was heated at 9 (TC for 8 hours). The black suspension is cooled to room temperature and diluted with water and taken in the test. Then, the combined organic extracts are further swept in a Na〇H aqueous solution, water and brine. It is dehydrated and dried with Na2S04; it is considered; the solution is concentrated in a vacuum to obtain a viscous red oil. The crude product thus obtained is purified by flash chromatography (Si〇2, 炫炫-3:7 (v /v) Hexane: EtOAc) to give the title compound as a yellow oil. Step 4: Amine 5 (丨2,3-, 1 -muscle·J-LUt)-3-(methoxy)-1-propanyl]benyl}mercapto)-cyclopropylamine (1 告吾>1Λ^ U田置) with 10% w/w palladium on charcoal (0.1 eq. 143482-1 -66 - 201111364 floated in EtOAc (0.03M). Then 'pump the container and let the gas h2. In the gas cylinder filled with H2 atmosphere The reaction suspension was stirred at room temperature for 2 hours, then 'quenched with CI^Cl2' through a bed of diatomaceous earth, and the filtrate was concentrated in vacuo. The crude product thus obtained was subjected to a flash. Purification by chromatography (Si 2 2 hexanes - 1:1 (v/v) hexanes:EtOAc) [2-(decyloxy)ethyl]phenyl}methyl)cyclopropylamine* Step 1: [(5-Mothyl-2,3-dichlorophenyl)methyl]cyclopropylaminocarboxylic acid u_ Dimethylethyl ester will be obtained from N-[(5-glycosyl-2,3-dichlorophenyl)methyl]cyclopropylamine (1 'in) of amine 5 step 2 and di-third to di-dicarbonate The ester q J equivalent) was combined in CH 2 Cl 2 (〇 '17M). Then, to this solution, Hunig's test (1.2 equivalents) was added, and the resulting yellow solution was stirred at room temperature for 3 hours. Next, the reaction mixture was diluted with ether and washed successively with water and brine. Then, the organic layer was dried over Na 2 S 〇 4, filtered, and the filtrate was concentrated in vacuo to give a color oil. The product was purified by flash chromatography eluting elut elut elut elut v, step 2. %, propyl [ο divinylvinylphenyl) fluorenyl] guanidinium ruthenate, 丨 曱 曱 乙 旨 旨 旨 旨 旨 旨 旨 旨 旨 旨 旨 ( ( ( ( ( ( ( ( ( ( ( ( ( Dichlorophenyl)methyl]cyclopropylcarbamic acid U-didecylethyl ester (1 equivalent) and 2-vinyl-4,4,5,5-tetradecyl 1,3,2-oxygen Boronum (1 equivalent) is combined in: n_pr〇H of 2:1 (v/v) mixed 143482-1 -67- 201111364 (0.1M). Then, in this solution, acetic acid Ib (π) (〇 5 equivalents) and triphenylphosphine (〇 15 equivalents) were added, and then the vessel was repeatedly evacuated and counter-filled with nitrogen. Finally, 2 Ν aqueous NafO 3 (2 equivalents) was added, and the resulting two-phase suspension was heated at 90 ° C for 18 hours. The current black suspension was allowed to cool to room temperature, diluted with water and extracted with 1:1 (v/v) hexanes: ether. The combined organic extracts were then further washed with aqueous IN NaOH, water and brine. Then, it was dehydrated and dried with Na2S〇4, and the filtrate was concentrated in vacuo to give a pale yellow oil. The crude product thus obtained was purified by flash chromatography (EtOAc: EtOAc (EtOAc) Step 3: Cyclopropyl {[2,3-dichloro-5-(2-hydroxyethyl)phenyl]methylindolyl decanoic acid u_ fluorenyl B. The cyclopropyl group obtained from the previous step [(2,3_divinylvinylphenyl)indenyl] 1,1-dimethylethyl carbamic acid (1 equivalent), [Ir(c〇D)cl]2 (〇〇25 equivalent) and DPPB (〇.〇5 equivalent) was combined in THF (〇nM). Then, in this solution, 4,4,5,5-tetradecyl-l,3,2-dioxaborin (1.3 eq.) is added, and the formed, 'work color> gluten solution is Stir at room temperature for 12 hours. Finally, sodium perborate (0.1 M aqueous solution, 1 equivalent) was added, and the current black two-phase solution was vigorously stirred at room temperature for further 12 hours. The aqueous layer was separated and back extracted with ether. The combined organic extracts were then further washed with aqueous 1 N NaOH, water and brine. Then, it was dried over NasSO4, filtered, and the filtrate was concentrated in vacuo to give a pale yellow oil. The crude product thus obtained was purified by flash chromatography (Si </RTI> <RTIgt; </RTI> <RTIgt; </RTI> <RTIgt; </RTI> <RTIgt; </RTI> <RTIgt; </RTI> <RTIgt; Colorless oil. 143482-1 •68- 201111364 Step 4: Cyclopropanol (72 3 gcm ^ (helium·5_[2-(methoxy)ethyl]phenyl)methyl)carbamic acid 1,1-dimethyl The ethyl ester was dissolved in THF (〇3M) tj7 with % propyl {[2,3-dichloro! (2-hydroxyethyl)phenyl]methyl}aminocarbamic acid u-dimethyl ethane. Then, in this solution, sodium hydride ((9)% w/w dispersion in oil, i equivalent) was added, and the resulting stock solution was stirred for 5 minutes under / phoenix. Finally, moths were added. (1〇当罝)' and the current light yellow solution was stirred in the dark at room temperature for 10 φ hours. Then, the volatile matter was removed in vacuo, and the residue formed was tested in 1NHC1 aqueous solution. The liquid layer was separated and the aqueous layer was separated and subjected to reverse extraction with ether. Then, the combined organic extracts were washed with an aqueous solution of water, water and brine, followed by dehydration with Na2S 4 and filtration. And the filtrate is concentrated in vacuo to give the title compound (oil-contaminated) as a pale yellow oil. Step 5: Amine 6 to give the cyclopropyl group from the previous step ({2,3_二气_5_[2_( Methoxy Ethyl]ethylidene}methyl)carbamic acid U-didecylethyl ester (1 equivalent) is dissolved in CH2C12 (0.1M). Then, in this solution, HC1 (40m, in dioxane, 30 eq.), and the resulting solution was stirred at room temperature for 2 hours. Then, the reaction was quenched with aqueous 1N NaOH and extracted with ether. Then, the organic extract was washed with water and brine. Drying with Na2S〇4, filtration, and concentrating the filtrate in vacuo. The crude product thus obtained was purified by flash chromatography (SiO2, 9:1 (v/v) hexane: Et 〇Ac- Et 〇Ac ), the title compound was obtained as a colorless oil. Amine 7 143482-1 -69- 201111364 N-(2-indolyl-5-[3-(indolyl)propyl]phenyl}indolyl) propylamine Step 1 : 5-A-N-cyclopropyl-2-methylbenzamide at 0 C in a solution of 5-oxo-2-indenylbenzoic acid (1 eq.) and DMF (12 eq.) In 1M), the gasified grasshopper (I2 equivalent) was added dropwise, and the solution was mixed for 2 hours under 〇t, and then the volatile matter was removed in a vacuum to form a residue. Soluble In a gas methane (10), cooled to o ° C, and successively added cyclopropylamine (15 equivalents) and Hunig's base (2 equivalents) dropwise. The resulting suspension was stirred at room temperature for 18 hours. The reaction was quenched with aqueous HCl and extracted with dichloromethane. The combined organic extracts were dried with &lt;RTI ID=0.0&gt; In the suspension, an equal volume of hexane was added and the title compound was isolated by vacuum filtration. Step 2: N-[(5-Alkyl-2-mercaptophenyl)methyl]cyclopropylamine at 〇 ° C, 5_chloro_N_cyclopropyl-2-methyl obtained from the previous step To a suspension of benzamide (1 eq.) in THF (0.4 M) was added borane (1 〇M in THF, 3 eq.). The resulting suspension was allowed to warm to room temperature over a period of time and then heated under reflux for 1 hour. The current pale yellow solution was re-cooled to 〇 C and the reaction was carefully quenched with aqueous EtOAc. The resulting mixture was heated under reflux for 1 hour to ensure complete decomposition of the amine-sane complex. After careful neutralization with aqueous 1 N NaOH solution, the aqueous layer was separated and purified with EtOAc. The combined organic extracts were washed with brine, dried over MgSO.sub. The filtrate was concentrated in vacuo, and the crude material obtained was purified further purified eluting eluting eluting eluting eluting Colorless oil. 143482-1 ► 70- 201111364 Step 3: [(5-Alkyl-2-methylphenyl)indenyl]cyclopropylamino decanoic acid ι, ΐ-dimethylethyl ester at -78 ° C, To a solution of N_[(5-carbyl-2-methylphenyl)methyl]cyclopropylamine (1 equivalent) in THF (0.3 M) from the previous step, hexamethyldifluoride (0.5 g) was added. M 'in toluene, 1.2 equivalents). After stirring at -78 ° C for 1 hour, a slave was added, and the resulting mixture was slowly warmed to room temperature for 2 hours. The reaction was quenched with saturated aqueous NH.sub.4Cl. The combined organic extracts were washed with brine, dried with EtOAc EtOAc EtOAc. Further purification (Si 2 , hexane - 4:1 (v/v) hexane: EtOAc) was obtained by flash chromatography to afford the title compound as pale yellow oil. Step 4: Cyclopropyl ({2-mercapto-5-[(1Ε)-3-(methoxy)-1-propen-1-yl]phenyl}methyl)carbamic acid 1,1-di Thioglycol ethyl ester will be obtained from [(5-carbyl-2-mercaptophenyl)methyl]cyclopropylamino. decanoic acid 1,1-didecylethyl ester (1 equivalent) and 4 , 4 5,5_tetradecyl 2 [(1e) 3 (曱 oxygen • yl) propylene-1·ylindole, 3,2·dioxaboron (1 eq.) combined with n-BuOH ( 0.48M). Then, in this solution, a ginseng (diphenylarbenium acetonide) dipalladium (yttrium) gas imitation adduct (0.02 equivalent), [2,6,-bis(decyloxy)-2-biphenyl was added. (dicyclohexyl) discane (〇.〇8 equivalent) and powdered potassium phosphate (2 equivalents). The vessel was repeatedly evacuated and counter-filled with nitrogen, and then the resulting suspension was placed at 1 Torr. Heat under 16 for 16 hours. The current black suspension was allowed to cool to room temperature, diluted with Et〇Ac, and transitioned through a Si〇2 batter. Then, the filtrate was concentrated in vacuo, and the crude product thus obtained was directly subjected to purification by flash chromatography (Si 〇 2, hexane - 3:7 (v/v) hexane: Et EtOAc). The title compound was isolated from 143482-1 -71 - 201111364 as a pale yellow oil. Step 5. Indole propyl ({2-methyl·5_[3_(decyloxy)propyl)phenyl}indolyl) decanoic acid 1,1_·indolyl hydrazine Propyl ({2 methyl_5 [(1Ε)_3 (decyloxy H-propenyl)phenyl}indolyl) decanoic acid 1,1-didecylethyl ester (1 equivalent) and 10% w/w palladium/carbon (0.1 eq.) was suspended in Et〇Ac (〇〇8M). Then, the vessel was evacuated and scrubbed with H2. The reaction suspension was placed under a cylinder filled with % atmosphere. After stirring at room temperature for 2 hours, the reaction was quenched with CH.sub.2Cl.sub.sub.sub.sub.sub.sub.sub.sub.sub.sub. - 1:1 (v/v) hexanes: EtOAc (m.) EtOAc: EtOAc: EtOAc Propyl]phenyl}decyl)amino decanoic acid 1,1-didecylethyl ester (1 equivalent) is dissolved in CH2Cl2 (〇1M). Then, in this solution, HC1 (4 〇M, In a dioxane field, 30 equivalents), and the resulting solution was stirred at room temperature for 2 hours. The reaction was quenched with aqueous EtOAc (aq. EtOAc) (EtOAc) (HHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHH Purification by flash chromatography (Si </RTI> <RTI ID=0.0></RTI> </RTI> <RTI ID=0.0> -(Methoxy)ethyl] phenyl}methyl)cyclopropylamine 8 is prepared according to the procedure described for amine 6, but alternatively using step 3 from amine 143482-1 -72-201111364 7 [ (5-Alkyl-2-indenyl)methyl]cyclopropylamino decanoic acid with -didecylethyl ester as the acceptor, n-BuOH as the solvent, ginseng (diphenylarbenium acetonide) Palladium (9) gas imitation adduct as palladium source, [2,6,-bis(methoxy)_2-biphenyl](dicyclohexyl)yl alkane as a ligand, and powdered potassium phosphate as a base, For Suzuki coupling (step 2). Amine 9 N-({2,3-difluoro-5-[3-(methoxy)propyl]phenylindolyl)cyclopropylamine 9 based on amine 5 Made in the procedure described, but alternatively used 2,3_two Benzofurfural is used as a starting material. Amine 10 N-({3-(decyloxy)-5-[3-(methoxy)propyl]phenyl) propylamine Step 1 : 3-bromo group -5-Hydroxybenzaldehyde Addition of n-butylmagnesium hydride in a toluene solution (1.6 M) of n-butyllithium (2.5 M in hexane, 2.1 eq.) at -10 C. 〇M 'in THF, 〇6 when i). The reaction mixture was stirred at -10 ° C for 3 minutes, then 3,5-dibromophenol (1 equivalent) in benzene (0.7 M) was added dropwise over a period of 35 min. After stirring at -10 C for an additional 30 minutes, the reaction mixture was cooled to _4 〇 C then DMF (20 eq.) was added dropwise over 2 s. It was stirred at room temperature for 1 hour. The reaction was carefully quenched with 1 ΝΗ aqueous solution at 〇 ° C and taken with ether. The combined organic extracts were washed with water and brine, dried over MgSO 4 and filtered. The liquid was concentrated in vacuo to give a yellow solid. The recrystallization of the crude product thus obtained was carried out to give the title compound as a beige powder. 143482-1 -73- 201111364 Step 2: 3-Pentyl-5-[(1Ε)-3-(decyloxy)-1-propanyl]benzoic acid will be obtained from the previous step 3-bromo -5-Hydroxybenzaldehyde (1 equivalent) combined with 3-decyloxyprop-1-en-1-yl]-4,4,5,5-tetradecyl-dioxaboron (1 equivalent) In DMF (0.05M). Then, to this solution, palladium acetate (indole), two scales (0.2 as straight), and 2 M aqueous sodium carbonate (4 equivalents) were added. The resulting suspension was heated at 80 ° C for 16 hours. The reaction mixture was quenched with a 1N aqueous solution of EtOAc and extracted with ether. The combined organic extracts were washed with water, aq. NaH.sub.3, and brine. The mixture was dehydrated and dried with MgS(R), and the filtrate was concentrated in vacuo to give a crude product as a brown tar. The title compound was obtained as a yellow oil. m. m. Step 3: 3-(Methoxy)-5-[(1Ε)-3-(methoxy)-1-propanthene]ylbenzene disc will be obtained from the previous step 3-hydroxy-5-[ (1 Ε)-3-(methoxy)+propenyl]benzaldehyde (1 eq.) and iododecane (2-2 eq.) were combined in acetone (〇〇7M). Then, potassium carbonate (2 equivalents) was added to the solution, and the reaction suspension was heated under reflux for 16 hours. The resulting reaction mixture was concentrated in vacuo and the residue was partitioned between water and ether. The aqueous wash was separated and extracted by mystery. The combined organic extracts were further washed with brine, dried over MgSO 4 , filtered, and evaporated. The crude product thus obtained was further purified by flash chromatography ( </ RTI> </ RTI> <RTIgt; </RTI> <RTIgt; </RTI> <RTIgt; </RTI> <RTIgt; Yellow oil. Step 4: N-({3-(Methoxy)_5_[(1e)-3-(decyloxy)propenyl)]phenyl}indolyl)-cyclopropylamine 143482-1 • 74· 201111364 3_(Methoxy)_5 [(10)_3 (methoxy W prop-1-ene-1-yl)benzaldehyde (1 equivalent) in dichloromethane (〇5M) In the solution, % propylamine (2 eq.) and magnesium sulfate (15 eq.) were added. The resulting suspension was stirred at room temperature for 12 hours. Insolubles were removed by filtration. The filtrate was concentrated in vacuo to give crude. The imine is a yellow oil. Then, it is dissolved in methanol (0.3M), and then sodium borohydride (15 eq.) is added in portions over 5 minutes. The reaction mixture is slowly warmed. The mixture was stirred for 2 hours at room temperature and then stirred at room temperature for 2 hours. After carefully quenching the reaction with a saturated aqueous solution of NaHCO3, the mixture was extracted with a mixture. The combined organic extracts were washed with water and brine. Dehydrated with MgS 4 and filtered. The filtrate was concentrated in vacuo to give the title compound as a yellow oil. Step 5: Amine 10 from the previous one N-({3-(Methoxy)-5-[(ie)-3-(methoxy)-1-propen-1-yl]phenyl)indolyl)cyclopropylamine (1 eq.) In the solution of Et0Ac (〇〇4M), palladium (10% w/w, on activated carbon, αι equivalent) was added, the vessel was evacuated, and φ was backfilled with argon. Then, the reaction suspension was placed in a hydrogen cylinder atmosphere. After stirring for 5 hours, the reaction was quenched with EtOAc (EtOAc m.) N-({3-{[2-(Methoxy)ethyl]oxy)5-[3-(indolyl)propyl]phenylhydrazinemethyl)cyclopropylamine 11 is as described in amine 10 The procedure is followed, but in step 3, 2-bromoethylindenyl hydrazine is alternatively used as the alkylating agent, and carbonic acid is used as a solvent, 143482-1 -75- 201111364 and DMF as a solvent. Amine 12 4-{ 3,4-Dichloro·5_[(cyclopropylamino)methyl]phenylindolonitrile 乂1 1 cyclopropyl {[2,3-dichloro-5-(2-ketoethyl)phenyl] 1,1-Dimethylethyl hydrazide for the cyclopropyl group of the amine 6 step 3 ([2,3_digas_5(2-hydroxyethyl) Phenyl] methyl} carbamic acid methyl ethyl ester U- station (1 eq) and sodium bicarbonate square equiv) was suspended in times called iv) Order. At (TC), DMP (1 eq.) was added, and the resulting mixture was stirred at EtOAc for 15 min and then quenched at room temperature. The reaction was quenched with aqueous NaOH and extracted with ether. The combined organic extracts were washed with water and brine, dried with EtOAc EtOAc (EtOAc m. {2,3_Digas·5_[(2E) each cyanobutyryl small group] phenyl}methyl)amino decanoic acid 1,1-dimethylethyl ester in anhydrous lithium carbonate (1.2 equivalents) In a suspension of THF (0.1 M), diethyl (cyanoguanidino)phosphonate (1.2 equivalents) and 1) 611 (1 equivalent) were successively added. The formed suspension was stirred at room temperature for 15 minutes, and then the cyclopropyl group [[2,3_digas_5_(2-ketone) obtained from the previous step was added dropwise with a THF (〇im) solution. U-diphenylacetic acid (1 equivalent) of ethyl ethyl)phenyl]methyl}aminocarbamate. The resulting pink suspension was stirred at room temperature for 12 hours, then the α1ΝΗα aqueous solution was carefully quenched and then extracted with ether. The combined organic extracts were further washed with water and brine and dried over N?SO? Filter, and concentrate the filtrate in vacuo. The crude product thus obtained was purified by flash chromatography, 1434S2-1 -76 - 201111364 (Si2, hexanes &gt; 3:7 (v/v)hexane: EtOAc) to give the title compound as colorless oil . Step 3: cyclopropyl {[2,3-dichloro-5-(3-cyanopropyl)phenyl]-indenyl carbamic acid U-didecylethyl ester in Cyclohexane from the previous step 1,2,3-Dichloro-5-[(2E)-3-cyano-2-propan-1-yl]phenyl}indolyl) decanoic acid 1,1-dimethylethyl hydrazine A solution of (1 eq.) in EtOAc (0.04 M) was added (10% w/w over EtOAc). The container is evacuated and backfilled with hydrogen. Then, the reaction suspension was stirred under a hydrogen atmosphere for 1.5 hours. The reaction was quenched with dioxane and filtered through a pad of Celite. The insoluble material was further washed with EtOAc. The filtrate was concentrated in vacuo to give the title compound. Step 4: Amine 12 is obtained from the previous step of cyclopropyl {[2,3-dioxa-5-(3-cyanopropyl)phenyl]decyl}carbamic acid U-dimethylethyl ester ( 1 equivalent) In a solution of CH2Cl2 (〇〇6M), zinc bromide (11) (10 equivalents) was added, and the resulting suspension was sonicated for φ 15 minutes' and then it was stirred at room temperature for 18 hours. The reaction was quenched with 1N aqueous EtOAc then EtOAc. The combined organic extracts were further washed with water and brine, dried over NaHSOs, filtered, and evaporated. The crude product thus obtained was purified by flash chromatography (SiO 2 , 9:1 (V/V) hexane: Et0Ac-3:7 (v/v) hexane: Et EtOAc) Colorless oil. Amine 13 M3-[(cyclopropylamino)indolyl]_4,5-difluoro-p-phenyl}-d-butylamine U is synthesized according to the procedure described in amine 12, but is used instead of class 143482-] •77· 201111364 a cyclopropyl {[2,3-difluoro-5-(2-ethyl)phenyl]decyl}amino phthalic acid U-dimethylethyl ester from 2,3-difluorobenzaldehyde . Amine 14 4-{3,4-Dichloro-5-[(cyclopropylamino)indolyl]phenyl}butanoic acid decylamine 14 was prepared according to the procedure described for amine 12, but in Wittig thinning In the step (step 2), the anhydrous gasification of diethyl (cyanoguanidino)phosphonate and DBU are replaced by (triphenyl-into-5-phosphinoalkyl)methyl acetate. Amine 15 N-({3-[3-(indolyl)propyl]-1-teayl}methyl)cyclopropylamine Step 1: 3-[(1Ε)-3-(decyloxy)-1- Propylene small base] small tea carboxylic acid vinegar vinegar 3-bromo-1-benzenecarboxylic acid oxime ester (1 equivalent) and 4 4 5 5 -tetramethyl 2 耵 各 各 (曱 ))-1-propene 1-yl]-1'3,2-dioxaboron (15 equivalents) was combined in a 5:1 (v/v) mixture (0.2 M) of DMF: n-PrOH. Then, in this solution, trans-bis(triphenylphosphine) evolved palladium (IIX 0.05 equivalent) was added, and the vessel was repeatedly evacuated and counter-filled with nitrogen. Finally, a 2NNa2C〇3 aqueous solution (2 eq.) was added and the resulting two-phase suspension was heated at 9 (TC for 8 hours. The current black suspension was cooled to room temperature, diluted with water and taken at 1:1 ( v/v) Hexane: Ether extraction. Then 'the combined organic extracts were further washed with 1N Na〇H aqueous solution, m Ηα aqueous solution, water and brine. Then 'dehydrated with ~〇4, filtered, and made The filtrate is concentrated in vacuo to give the title compound as a red oil. Step 2: 3-[3-(decyloxy)propyl]-i- _ _ _ _ _ _ _ _ _ _ _ )-3-(decyloxy)4-propenylhydrazone H荇carboxylate (1 equivalent) and 10% w/w palladium/carbon (αΐ equivalent) suspended in Me〇H (〇〇8M) 143482-1 -78- 201111364 = ° Then, the vessel was evacuated and gas was purged with h2. The reaction suspension was stirred at room temperature for 2 hours under a bottle filled with an atmosphere. Then, the reaction was quenched with CH2Cl2. The filtrate was filtered through a pad of celite, and the filtrate was concentrated in vacuo. The crude product thus obtained was purified by flash chromatography (Si.sub.2, hexanes (v/v) hexane: EtOAc). The title compound is a colorless oil. Step 3: 3-[3-(Methoxy)propyl]+naphthoic acid is obtained from the previous step of 3-[M. 1 When _I) is dissolved in Me0H: 2:1 (v/v) mixture (0.08 M). Then, LiOH (2.0 M aqueous solution, 3 equivalents) was added to the solution, and the resulting turbid suspension was vigorously stirred at /JEL for 24 hours. Next, the volatile material was removed in vacuo, and the pH of the residue was carefully adjusted to &lt;~&apos;&apos;&apos; The combined organic extracts were further washed with water and brine, dried over Na 2 SO 4 and filtered. The title compound was obtained as a white solid (yield). Step 4: N-cyclopropyl-3-[3-(indolyl)propyl]-1-indolecarboxamide • at 0 ° C 'from the previous step 3_[3_(decyloxy) In a CH2C12 solution (0.1 M) of propyl H-decanoic acid (1 equivalent), gasified grass mash (1 - 2 equivalents) was added followed by a few drops of DMF. The resulting solution was stirred at room temperature for 2 hours and then the volatiles were removed in vacuo. The resulting residue was dissolved in dioxon (0.1 M), cooled to 〇〇c, and Hunig base (1.2 eq.) and cyclopropylamine (U equivalent) were added dropwise. The resulting suspension was stirred at room temperature for 18 hours. The reaction was quenched with aqueous <RTI ID=0.0>IN </RTI> </RTI> <RTIgt; The combined organic extracts were further washed with aq. aq. NaOH, water and brine, dried over Na? The filtrate was concentrated in vacuo to give title titled <RTIgt; Step 5: Amine 15 in a THF solution of N-cyclopropyl-3-[3 (decyloxy)propyl]-1-calylamide (1 equivalent) from the previous step under reflux. In addition, a borane-sulfurized decane complex (6.6 equivalents) was added. A short path distillation unit was attached to the reaction vessel and most of the volatiles were slowly distilled over a period of 15 hours. The current yellow solution was again cooled to 〇 ° C and the reaction was carefully quenched with 1N aqueous HCl. The resulting mixture was heated under reflux for a few hours to ensure complete decomposition of the amine-paraffin complex. After careful neutralization with a 1 N aqueous NaOH solution, the water layer was separated and extracted with EtO Ac. The combined organic extracts were washed with brine, dried over Nad.sub.4, and filtered. The filtrate was concentrated in vacuo <RTI ID=0.0></RTI> and the crude material thus obtained was further purified by flash chromatography (SiO 2 &lt;RTI ID=0.0&gt;&gt; To display the title compound as a colorless oil. Amine 16 (2-{3,4-Dichloro-5-[(cyclopropylamino)methyl]phenyl}ethyl)amino decanoic acid hydrazine Step 1: Ring propyl [(2, 3-) Gas-5-nonylphenyl)indenyl]amino acid ι,μ dimethylethyl ester in cyclopropyl [2,3-dioxa-5-vinylphenyl] from step 6 of amine 6 A solution of U-dimercaptoethyl urethane (1 eq.) in dioxane methane (0.03 M) was bubbled with freshly generated ozone at -78 °C until a persistent blue color was observed. Then, triphenylphosphine (1.2 equivalents) was added thereto in a quick portion, and the resulting mixture was slowly warmed to room temperature over 3 hours. Volatile materials were removed in vacuo and the remaining residue was triturated with 2: 1 (v/v) hexanes: Et20. 143482-1 •80· 201111364 The insolubles were removed via hydrazine and the filtrate was concentrated in vacuo. The crude product thus obtained was purified by flash chromatography eluting elut elut elut Step 2 · propyl {[2,3~di-5-(methyl)phenyl]methyl}aminocarbamic acid 1,1-dimethylethyl ester at 0 C, obtained from the previous step Sodium borohydride (U equivalent) was added to a solution of cyclopropyl [(2,3 dioxo-5 methionylphenyl) fluorenyl] methic acid dimethyl acetate in methanol (016M). The resulting solution was stirred under 〇c&gt;c for 2 hours and then the volatiles were removed in vacuo. Next, the resulting residue was subjected to liquid separation between ether and aqueous solution of IN HCl. The aqueous layer was separated and back extracted with ether. The combined organic extracts were further washed with water and brine, dried over Na 2 EtOAc, filtered, and evaporated. The crude product thus obtained was purified by EtOAc EtOAc (EtOAc) Step 3: decanesulfonic acid {3,4-dichloro-5-[(cyclopropyldimethylethyl)oxy]carbonyl}amino)methyl]phenyl}methyl ester at 〇 ° C, From the previous step, cyclopropyl {[2,3 dioxo-phenyl]indolyl} guanidinoic acid U-dimethyl oxime (1 equivalent) in a solution of dimethyl gas (〇1M) Hunig's base (3 equivalents) and gasified decanesulfonium (U equivalent) were successively added. The resulting solution was stirred at (TC for 30 minutes and then at room temperature for 15 minutes. Then, the reaction mixture was diluted with ether and the mixture was carefully quenched with aqueous EtOAc. The aqueous layer was separated and extracted with ether. The combined organic extracts were washed with EtOAc EtOAc (EtOAc m. Cyclopropyl {[2,3-dioxa-5-(|L-indenyl)phenyl]decyl}carbamic acid U-didecylethyl ester in the decanesulfonic acid {3, obtained from the previous step 4-Dimethyl-5-[(cyclopropyl{[(u-didecylethyl)oxy]methyl}}amino)indolyl]phenyl decyl ester (1 equivalent) in DMS 〇 (0.48M In the bath, add a chaotic clock (1·3 equivalent) and a packed sodium (〇1 equivalent). The resulting solution was stirred at room temperature for 3 hours, then diluted with ether and taken in IN. The reaction was quenched with aqueous NaOH solution, and the aqueous layer was separated and extracted with ether. The combined organic extracts were further washed with water and brine, dried with NaJO4, filtered, and filtered. The crude product thus obtained was purified by flash chromatography (EtOAc: EtOAc: EtOAc (EtOAc) Oil. Step 5: {[5-(2-Aminoethyl)-2,3-dioxaphenyl] fluorenyl}cyclopropylamino decanoic acid U-didecylethyl ester at 〇 ° C, Cyclopropyl {[2,3_diox_5(cyanomethyl)phenyl]decyl}amino decanoic acid 1,1-didecylethyl ester (1 equivalent) and gas obtained from the previous step Cobalt (light) hexahydrate (2 equivalents) in a solution of decyl alcohol (0.07 M), sodium borohydride (10 eq.) was added portionwise. The resulting mixture was stirred for 1 hr. The next 2 hours. The current brown suspension was quenched with aqueous NaOH solution and then extracted with EtOAc. The combined organic extracts were washed with water and brine, dried over Naz. The crude title compound was obtained as a pale brown amorphous solid. Step 6: cyclopropyl {[2,3-diox-5-(2-{[(decyloxy))). Aminomethyl)phenyl] 143482-1 •82- 201111 364 曱 } 胺 1 胺 胺 胺 胺 胺 胺 胺 胺 [ [ [ [ [ [ [ [ [ [ [ [ [ [ [ [ [ [ [ [ [ [ [ {[5-(2-aminoethyl)-2,3-diphenyl To a solution of 1,1-dimethylethylcyclopropylamino decanoate (1 eq.) in dichlorohydrazine (0.07 M), Hunig's base (1.2 eq.) and gas were added sequentially. Methyl formate. Then, the resulting solution was slowly warmed to room temperature for 3 hours. Then, the crude reaction mixture was diluted with ether and successively taken in 1N NaHH aqueous solution, aqueous solution of IN HCl, water and brine. washing. Then, the ether extract was dehydrated and dried with Na S04, filtered, and the filtrate was concentrated in vacuo. The crude product thus obtained was purified by flash chromatography eluting elut elut elut elut elut Step 7: Amine 16 is obtained from the previous step of cyclopropyl {[2,3-dioxa-5-(2-{[(indolyl))]amino}ethyl)phenyl] fluorenyl} To a solution of 1,1 -didecylamine amide (1 eq.) in CH.sub.2Cl.sub.2 (.sup..sup.6M) was added HCl (4.0M in EtOAc, 30 eq.). The resulting solution was stirred at room temperature for 3 hours. Then, the reaction was quenched with _IN aqueous NaOH solution and extracted with a scale. Next, the human organic extract was further washed with water and brine, dried over MgSO.sub.4, filtered, and concentrated. The crude product thus obtained was purified by flash chromatography (EtOAc: EtOAc: EtOAc (EtOAc) Amine 17 N-(8-4: arylmethyl)cyclopropylamine in a solution of 8-quinolinecarboxaldehyde (1 eq.) in dioxane (〇 13M), added magnesium sulfate (1 eq.) and cyclopropyl Amine (2 equivalents). The resulting suspension was thrown at room temperature for 14 hours at 143482-1 -83-201111364. After passing through the cold, and flushing with nitroxamidine, then the combined filtrate was placed in a vacuum, koji, 蝻. The crude imine thus obtained was dissolved in decyl alcohol (0.13 M), followed by VIII, knife-under-added rotten fish steel q 5 )). The reaction mixture was stirred at room temperature and the solution was quenched to quench the reaction. Then, with 1N N", then, then the HC1 water is adjusted to ~1G ' and then it is extracted with ether to remove the pH of the solution into the salt water step by step - dehydrated with Na2S04: and the organic extract is water and Concentrate in vacuo to give the crude title compound: <RTI ID=0.0>

N-(8-異喳啉基曱基)環丙胺 胺18係根據胺17中所述之種序朝 喹啉羧甲醛作為起始物質。 ;成,但替代地使用8-異 胺19 N-(5-異奎17林基甲基)環丙胺 胺19係根據胺17中所述之 喹啉羧曱醛作為起始物質。 胺20 程序製成 但替代地使用5-異N-(8-isoindolyl fluorenyl)cyclopropylamine 18 is based on the order described in amine 17 towards quinolinecarboxaldehyde as the starting material. Alternatively, but 8-isoamine 19 N-(5-isoquinoline 17-linylmethyl)cyclopropylamine 19 is used as the starting material according to the quinoline carboxaldehyde as described in the amine 17. Amine 20 is made, but instead uses 5-iso

N-(5-喳啉基甲基)環丙胺 胺20係根據胺17中所 啉羧甲醛作為起始物質 胺21 述之 程序製成 但替代地使用5-喹 N-(l-異崎:#基甲基)環丙胺 胺21係根據胺17中所述之寿。q 喹啉羧曱醛作為起始物質。 氣成’但替代地使用1-異 143482-1 -84. 201111364 胺22 N-({2-[3-(曱氧基)丙基]-4-4啉基}甲基)環丙胺 胺22係根據已公告之專利申請案WO 2007/009250 A1中所 述之程序製成。 胺23 N-({6-[3-(甲氧基)丙基]-8-4淋基}曱基)環丙胺 步驟1 : 6-({[(1,1-二曱基乙基)(二甲基)石夕烷基]氧基}甲基)_8_喹 啉羧甲醛 籲 在_78°C下,於8-溴基-6-({[(l,l-二曱基乙基)(二曱基)石夕烷基] 氧基}甲基)峻啉(1當量)之THF (0.06M)溶液中,逐滴添加正-丁基鋰(2.5M ’在己烷中’ 2.1當量),歷經1〇分鐘期間。將 所形成之黃色溶液在-78°C下攪拌15分鐘,然後逐滴添加 DMF (2當量)’歷經1〇分鐘期間。將目前紅色溶液於_78〇c下 再攪拌2小時,接著,藉由添加飽和nh4 C1水溶液使反應混 合物淬滅。分離水層’並以醚逆萃取。然後,將合併之有 φ 機萃液以鹽水洗滌,以Na2S04脫水乾燥,過濾,及使濾液 在真空中濃縮。如此獲得之粗產物經由急驟式層析之純化 (Si〇2,己烷-&gt; 3:7 (v/v)己烷:EtOAc),獲得標題化合物,為 黃色油,其係在靜置時固化。 步驟2 : Ν-{[6-({[(1,1-二甲基乙基)(二曱基)矽烷基]氧基}甲 基)各喹啉基]曱基}環丙胺 於得自前一步驟之6-({[(1,1_二曱基乙基)(二曱基)矽烷基] 氧基}曱基)-8-喹啉羧甲醛(1當量)之二氣甲烷(〇12M)溶液 中’添加硫酸鎂(1當量)與環丙基胺(2當量)^將所形成之 143482-1 -85- 201111364 懸浮液在室溫下攪拌16小時。經由過濾移除不溶物,並以 二氣甲烷沖洗’然後使合併之濾液在真空中濃縮。使如此 獲得之粗製亞胺溶於曱醇(0·12Μ)中,然後分次添加硼氫化 鈉(1.5當量)。將反應混合物在室溫下攪拌2小時。接著,於 真空中移除揮發性物質,並使所形成之殘留物於醚與爪N-(5-carbolinylmethyl)cyclopropylamine 20 is prepared according to the procedure described for the carboxaldehyde in the amine 17 as the starting material, amine 21, but alternatively 5-quino-N-(l-isosaki: #基基)Cyclopropylamine 21 is based on the life described in amine 17. q Quinoline carboxaldehyde as a starting material. Gas-forming but using 1-iso 143482-1 -84 instead. 201111364 Amine 22 N-({2-[3-(decyloxy)propyl]-4-4 phenyl)methyl)cyclopropylamine 22 It is made according to the procedure described in the published patent application WO 2007/009250 A1. Amine 23 N-({6-[3-(Methoxy)propyl]-8-4 lysyl} decyl) cyclopropylamine Step 1: 6-({[(1,1-didecylethyl)) (Dimethyl) oxalate]oxy}methyl)_8_quinolinecarboxyformaldehyde at 8-78 ° C, at 8-bromo-6-({[(l,l-didecyl) n-Butyllithium (2.5 M 'in hexanes) 2.1 equivalents), over a period of 1 minute. The resulting yellow solution was stirred at -78 °C for 15 minutes and then DMF (2 eq.) was added dropwise over a period of 1 s. The current red solution was stirred at _78 ° C for an additional 2 hours, then the reaction mixture was quenched by the addition of saturated aqueous nh 4 C1. The aqueous layer was separated&apos; and back extracted with ether. Then, the combined φ machine extracts were washed with brine, dried over Na 2 SO 4 , filtered, and the filtrate was concentrated in vacuo. The crude product thus obtained was purified by flash chromatography (EtOAc EtOAc (EtOAc) Cured. Step 2: Ν-{[6-({[(1,1-dimethylethyl)(didecyl)decyl]oxy}methyl)methylquinolinyl]hydrazino}cyclopropylamine from the former a step of 6-({[(1,1-didecylethyl)(didecyl)decyl]oxy}indolyl)-8-quinolinecarboxaldehyde (1 equivalent) of di-methane (〇 12M) Adding magnesium sulfate (1 eq.) and cyclopropylamine (2 eq.) in solution. The resulting 143482-1 -85 - 201111364 suspension was stirred at room temperature for 16 hours. The insolubles were removed via filtration and rinsed with di-methane m~ then the combined filtrate was concentrated in vacuo. The crude imine thus obtained was dissolved in decyl alcohol (0.12 Torr), and then sodium borohydride (1.5 eq.) was added portionwise. The reaction mixture was stirred at room temperature for 2 hours. Next, remove the volatiles in a vacuum and allow the residue to form in ether and claws.

NaOH水溶液之間作分液處理。分離水層,且以醚逆萃取。 將合併之有機萃液以水與鹽水進一步洗滌,以Na2S〇4脫水 乾燥’過遽,及使滤液在真空中濃縮,而得粗製標題化合 物’為黃色油。 步驟3 :環丙基_[(U•二曱基乙基)(二甲基)石夕烧基]氧基} 曱基)-8-喹啉基]曱基}胺基甲酸u_二甲基乙酯 於得自前一步驟之Ν-{[6-({[(1,1-二曱基乙基)(二甲基)矽烷 基]氧基}甲基)-8-啥啉基]甲基丨環丙胺(1當量)在二氣甲烷 (0.12M)中之洛液内,相繼地添加册吨氏鹼(丨2當量)與二碳 酸雙(1,1-二甲基乙基)醋(11當量)。將所形成之溶液在室溫 下攪拌8小時《然後,於真空中移除揮發性物質。如此獲得 之粗產物經由急驟式層析之純化(Si〇2,己烷—3:7 (v/v)己 院.EtOAc),獲得標題化合物,為無色油。 步驟4 :環丙基{[6_(羥甲基)各,查啉基]甲基}胺基甲酸u•二甲 基乙西旨 於得自前一步驟之環丙基二曱基乙基)(二甲基) 夕烷基]氧基}甲基)_8^套啉基]甲基丨胺基甲酸U二曱基乙酯 (1 §量)在THF (0.12M)中之溶液内,添加TBAF (1 0M,在己烷 1.6當置)。將所形成之溶液在室溫下攪拌2小時,然後 143482-1 201111364 於真空中移除揮發性物質。使所形成之殘留物於醚與水之 間作分液處理。分離水層,並以醚逆萃取。將合併之有機 萃液以水與鹽水進一步洗滌,以Na2S04脫水乾燥,過濾, 及使滤液在真空中濃縮。如此獲得之粗產物經由急驟式層 析之純化(Si〇2,9:1 (v/v)己烧:EtOAc— 3:7 (v/v)己烧:EtOAc), 獲得標題化合物,為無色油。 步驟5 :環丙基[(6_曱醯基各喳啉基)甲基]胺基甲酸u二曱基 乙酯 在0C下,於得自前一步驟之環丙基{[6_(羥甲基)_8_喳啉基] 曱基}胺基甲酸1,1-二曱基乙酯(1當量)與碳酸氫鈉J當量) 在二氣曱烷(0.1M)中之懸浮液内,添加DMp (u當量)。將所 形成之混合物於室溫下攪拌2小時,然後以飽和NaHS〇3水溶 液使反應淬滅,接著以與〇萃取。將合併之有機萃液以inA liquid separation treatment was carried out between the aqueous NaOH solutions. The aqueous layer was separated and back extracted with ether. The combined organic extracts were washed with EtOAc (EtOAc m. Step 3: cyclopropyl-[(U•didecylethyl)(dimethyl) oxalate]oxy} fluorenyl)-8-quinolinyl]fluorenyl}aminocarboxylic acid u-dimethyl The ethyl ester is obtained from the previous step -{[6-({[(1,1-didecylethyl)(dimethyl)decyl]oxy}methyl)-8-carbolinyl] Methyl anthracycline (1 eq.) in a solution of di-methane (0.12 M), successively adding a solution of strontium (丨2 equivalent) and bis(1,1-dimethylethyl) dicarbonate Vinegar (11 equivalents). The resulting solution was stirred at room temperature for 8 hours. Then, the volatiles were removed in vacuo. The crude product thus obtained was purified by flash chromatography eluting elut elut elut elut Step 4: Cyclopropyl {[6-(hydroxymethyl)- each, oxalinyl]methyl}aminocarbamic acid u• dimethylethoxime for the cyclopropyldidecylethyl group obtained from the previous step) Add TBAF to a solution of dimethylidene ethyl methacrylate (1 §) in THF (0.12 M) (10 M, placed in hexane 1.6). The resulting solution was stirred at room temperature for 2 hours, then 143482-1 201111364 was removed in vacuo to remove volatiles. The resulting residue is subjected to liquid separation between ether and water. The aqueous layer was separated and back extracted with ether. The combined organic extracts were further washed with water and brine, dried over Na 2 EtOAc, filtered, and evaporated. The crude product thus obtained was purified by flash chromatography (EtOAc: EtOAc (EtOAc:EtOAc) oil. Step 5: Cyclopropyl [(6-fluorenyl porphyrinyl)methyl]carbamic acid u-decylethyl ester at 0 C in cyclopropyl{[6_(hydroxymethyl) from the previous step ) _8_ porphyrinyl] fluorenyl} 1,1-didecyl ethyl carbazate (1 equivalent) and sodium hydrogencarbonate J equivalent) In a suspension of dioxane (0.1 M), DMp was added. (u equivalent). The resulting mixture was stirred at room temperature for 2 hours, then quenched with saturated aqueous NaH.sub.3, and then extracted with EtOAc. Combine the organic extracts in

NaOH水溶液、水及鹽水進一步洗滌,以Na2S〇4脫水乾燥, 及過濾。濾液在真空中之濃縮,獲得粗製標題化合物,為 白色固體。 步驟6 : 3-{8-[(環丙基{[(U_二甲基乙基)氧基]羰基}胺基)甲 基]-6-喹琳基}-2-丙烯酸甲酯 在〇°c下,於得自前一步驟之環丙基[(6甲醯基_8喳啉基) 曱棊]fe基甲酸1,1_二甲基乙酯(1當量)在二氣曱烷⑴〇6M)中 之溶液内添加(二苯基亞正膦基)醋酸曱酯(11當量)。然後, 使所形成之溶液慢慢地溫熱至室溫,歷經4小時。接著,於 真空中移除揮發性物質。如此獲得之粗產物經由急驟式層 析之純化(Si〇2,9:1 (v/v)己燒:Et0Ac_ 3:7 (v/v)己烧:Et〇Ac), 143482-1 •87· 201111364 獲得標題化合物,為白色固體β 步驟7 : 3-{8-[(環丙基{[(1 l 一甲| 土 mi’i —甲基乙基)氧基]幾基丨胺基)曱 基]-6-P奎琳基}丙酸甲西旨 於得自前一步驟之3侧環丙基{[(U-二甲基乙基)氧基燦 基}胺基)甲基]-6-4啉基}_2_丙烯酸甲酷(1當量)在Et〇Ac (0.1M)中之溶液内’添加纪_(w/w),於碳上,〇ι當量卜 將所形成之懸浮液抽氣,並以氫重複逆充填。最後,將反 應懸洋液在經氫充填之氣瓶大氣下攪拌3小時。藉由添加二 氯甲烷使反應淬滅,並經過矽藻土床過濾。然後,使濾液 在真空中濃縮。如此獲得之粗產物經由急驟式層析之純化 (Si〇2 ’ 9.1 (v/v)己烷:Et〇Ac_^Et〇Ac) ’獲得標題化合物為 黃色油。 步驟8 :環丙基{[6-(3-羥丙基)_8_喹啉基]甲基}胺基甲酸la二 甲基乙酯 於得自前一步驟之3·{8_[(環丙基([⑴^二曱基乙基)氧基]羰 基}胺基)曱基]-6-4啉基}丙酸曱酯q當量)在THF (〇 〇8Μ)中 之溶液内,添加删氫化鋰(5當量)。將所形成之混合物於室 溫下授拌14小時’然後將其以醚稀釋,並以1N Na〇H水溶液 使反應淬滅。分離水層,且以醚逆萃取。將合併之有機萃 液以水與鹽水進一步洗滌,以Na2s〇4脫水乾燥,及過濾。 渡液在真空中之濃縮,獲得粗製標題化合物,為無色油。 步驟9 :環丙基({6-[3-(曱氧基)丙基]-8-4啉基}曱基}胺基甲酸 1,1-二曱基乙酉旨 於得自前一步驟之環丙基{[6_(3_羥丙基)-8-喹啉基]甲基} 143482-1 -88- 201111364 胺基甲酸ι,ι-二甲基乙酯U當量)在THF (0 3M)中之溶液内’ 添加氫化納(在石蠟油中之60% (w/w)分散液,L2當量)^將 所形成之懸浮液於室溫下攪拌15分鐘,然後添加碘曱烷(14 當量)。將目前黃色溶液在室溫下攪拌12小時,接著藉由添 加IN NaOH水溶液使反應淬滅。分離水層,並以趟逆萃取。 將合併之有機萃液以水與鹽水進一步洗務,以Na2 脫水 乾燥,過慮’及使:;慮液在真空中漠縮。如此獲得之粗產物 經由急驟式層析之純化(Si〇2,9:1 (v/v)己烷:EtOAc— EtOAc), 胃獲得標題化合物,為無色油。 步驟10 :胺23 於得自前一步驟之環丙基({6-[3-(甲氧基)丙基]喳啉基} 甲基}胺基甲酸1,1-二曱基乙酯(1當量)在CH2Cl2(〇 〇6M)中之 溶液内,添加HC1 (4.0M,在二氧陸園中,3〇當量)。將所形 成之洛液於至溫下搜拌6小時。然後,以in NaOH水溶液使 反應淬滅,並以EtOAc萃取。接著,將合併之有機萃液以水 φ 與鹽水進一步洗滌,以NaaSO4脫水乾燥,及過濾。濾液在 真空中之濃縮,獲得標題化合物,為黃色油。 胺24 N-({3-氣基-5-[3-(曱氧基)丙基]苯基丨曱基)環丙胺 步驟1 : N-[(3-漠基-5-氣苯基)曱基]環丙胺 於3-溴基-5-氣苯曱醛(1當量)與環丙基胺(u當量)之4:1 (v/v) MeOH : THF溶液(0.06M)中’分次添加氰基硼氫化鈉(丄5 當量)’接著為純醋酸(3當量)。將所形成之混合物在室溫 下攪拌20小時。然後,於真空中移除揮發性物質。使所形 143482-1 -89- 201111364 成之殘留物溶於醚與飽和NH4 Cl水溶液中。分離水層,並工、 醚逆萃取。接著,將合併之有機萃液以鹽水洗滌,以 脫水乾燥,及過濾。濾液在真空中之濃縮,獲得粗製標題 化合物,為黃色油。 步驟2 : N-({3-氣基-5-[(1E)-3-(甲氧基)4_丙烯小基]苯基}甲基) 環丙胺 於得自前一步驟之N-[(3-漠基-5-氣苯基)曱基]環丙胺(1當 量)與4,4,5,5-四曱基-2-[(1Ε)-3-(曱氧基)+丙烯小基h,3 2二氧 硼伍園(2當量)之4:1 (v/v) DMF :正-丙醇溶液(〇 15M)中,添加 反式-二漠基雙(三苯膦)纪(11)(0.05當量),接著為碳酸鈉(2M 水溶液,3當量)。將反應容器抽氣,並以氮滌氣五次,然 後在100°C下加熱2小時。將已冷卻之反應混合物倒入飽和 NH4C1水溶液中,接著以Et0Ac萃取。將合併之有機萃液以 水與鹽水進步洗條,以MgS〇4脫水乾燥,過渡,及使淚液 在真空中濃縮。如此獲得之粗產物經由急驟式層析之純化 (Si02 ’ 3 . 7 (v/v)己烷:EtOAc— EtOAc) ’ 獲得標題化合物, 為油狀物。 步驟3 :胺24 於得自前一步驟之N-({3-氣基-5-[(1Ε)-3-(曱氧基)+丙烯-1-基]本基}曱基)環丙胺(1當量)在EtOAc (0.2M)中之溶液内,添 加鈀(10% (w/w) ’於碳上,〇.4當量)。將反應容器抽氣,並 以氫蘇氣兩次,然後於室溫下攪拌14小時。接著,使反應 懸浮液經過矽膠墊片過濾,並將不溶物以Et〇Ac沖洗。濾液 在真空中之濃縮’獲得標題化合物,為淡綠色油。 143482-1 -90- 201111364 胺25 Ν-{[1-(3-曱氧基丙基哚_3-基]曱基}環丙胺 步驟1 : 1-(3-甲氧基丙基)_ih-啕嗓_3_叛曱搭 在0 C下’於吲哚-3-羧曱醛(1當量)之dmf (0.1M)溶液中, 添加氫化鈉(在油中之60% (w/w)分散液,丨丨當量),接著為 1-溴基-3-曱氧基丙烷(ι·5當量p將反應混合物在5〇&lt;&gt;c下攪拌 4小時。然後,將混合物以醚稀釋,以水與鹽水洗滌,以 MgS〇4脫水乾燥,過濾,及使壚液在真空中濃縮。如此獲得 之粗產物經由急驟式層析之純化(Si〇2,1:1 (v/v)己烷:a〇Ac —EtO Ac),獲得標題化合物,為無色油。 步驟2 :胺25 在0 C下,於1-(3-甲氧基丙基卜朱-3-缓甲路(1當量)之 3:1 (Wv) : MeOH溶液(0.1M)中,添加環丙基胺(2當量)' 醋酸(2.5當量),接著為三〇醯氧基硼氫化鈉(15當量)。使 反應物慢慢溫熱至室溫,並在室溫下攪拌3小時。然後,以 • 飽和NaHC〇3水溶液使反應淬滅,以二氣甲烷萃取,以MgS〇4 脫水乾燥,過濾,及使濾液在真空中濃縮。如此獲得之粗 產物經由急驟式層析之純化(Si〇2,96:4 (v/v) CH2Cl2:在·〇Η 中之2.0M NH3) ’獲得標題化合物,為無色油。 胺26 3-{3,4-二氣-5-[(環丙胺基)曱基]苯基丨丙腈 步驟1 : (5-溴基-2,3-二氣笨基)曱醇 在〇°C下,於得自胺S步驟漠基_2,3_二氣笨甲醛(1當 量)之5:1(Wv)Me0H: THF溶液(0.38M)中,分次添加硼氮化納 143482-1 -91 - 201111364 (U當量),歷經45分鐘。將反應溶液在〇t:下攪拌2小時, 然後於真空中移除揮發性物質。接著,使所形成之殘留物 於顿與鹏此】水溶液之間作分液處理。分離水層’並以醚 逆萃取。將合併之有機萃液以1N Na〇H水溶液、水及鹽水進 -步洗務,以Na2S04脫水乾燥,過遽,及使渡液在真空中 濃縮。如此獲得之粗產⑯經由急驟式層析之純化⑽,9:1 (v/v)己烧:Et0Ac〜3:7 (v/v)己烧:Et〇Ac),獲得標題化合物, 為白色固體。 步驟2 : {[(5-溴基_2,3_二氣苯基)甲基]氧基}(u二甲基乙基)二 甲基矽烷 於得自前一步驟之(5·溴基_2,3_二氣苯基)曱醇(1當量)之 DMF (0.34M)溶液中’添加氣基(11二曱基乙基)二甲基矽烷 (U當量)與咪唑(1,5當量)。將所形成之黃色溶液在室溫下 攪拌16小時。然後,將反應混合物以醚稀釋,並以10% HC1 水溶液 '水及鹽水相繼洗滌。使醚萃液以Na2S〇4脫水乾燥, 過渡’及使慮液在真空中濃、缩,而得粗製標題化合物,為 無色油。 步驟3 : {[(2,3-二氯_5_乙烯基苯基)曱基]氧基}(11二曱基乙基) 二甲基矽烷 將得自前一步驟之{[(5_溴基_2,3_二氣苯基)曱基]氧基}(u_ 一甲基乙基)二曱基矽烷(1當量)與2乙烯基_445,5四甲基 -1,3,2-一氧硼伍園(1當量)合併於DMF : n_pr〇H之2:1 (v/v)混合 物(0.11M)中。然後,於此溶液中,添加醋酸鈀⑼(〇 〇5當量) 與三苯膦(0.15當量),接著將容器重複抽氣,並以氮逆充填。 143482-1 -92· 201111364 最後,添加INNa^O3水溶液(2當量),且將所形成之兩相懸 浮液在90°C下加熱8小時。使目前黑色懸浮液冷卻至室溫, 以水稀釋,並以1:1 (v/v)己烷:醚萃取。然後,將合併之有 機萃液以IN NaOH水溶液 '水及鹽水進一步洗滌。接著,使 其以Na2S〇4脫水乾燥,過濾,及使濾液在真空中濃縮而 得粗製標題化合物,為黑色油。 步驟4: 2-[3,4-二氣-5-({[(l,l-二甲基乙基)(二甲基)矽烷基]氧基} 甲基)苯基]乙醇 將得自前一步驟之{[(2,3·二氣_5_乙烯基苯基)曱基]氧 基ku-二甲基乙基)二曱基矽烷(1當量)' [Ir(COD)a]2(0025當 量)及DPPB (0.05當量)合併於THF (0·11Μ)中。然後,於此溶 液中’添加4,4,5,5-四曱基-ΐ,3,2-二氧硼伍園(1.3當量),並將所 形成之紅色溶液在室溫下攪拌16小時。最後,添加過硼酸 鈉(〇‘1Μ水溶液’ 1當量且將目前黑色兩相溶液於室溫下 再激烈搜拌8小時。分離水層,並以醚逆萃取。接著,將合 併之有機萃液以IN NaOH水溶液、水及鹽水進一步洗滌。然 後’使其以Na2S04脫水乾燥,過濾,及使濾液在真空中濃 '缩’而得黑色油。如此獲得之粗產物經由急驟式層析之純 化(Si02 ’ 9:1 (v/v)己烷:EtOAc— 1:1 (v/v) EtOAc :己烷),獲得 標題化合物,為淡黃色油。 步驟5 :曱院磺酸2_[3,4_二氯_5_({[(u_二曱基乙基)(二曱基)矽 烧基]氧基}甲基)苯基]乙酯 在o°c下’於得自前_步驟之2_[3 4_二氣_5_(丨[(11_二甲基乙 基)(二曱基)矽烷基]氧基丨曱基)苯基]乙醇(1當量)之二氣曱 143482-1 -93· 201111364 烧(〇.11Μ)溶液中,添加Humg氏驗(15當量)與氣化甲烧績酿 (1]當量)。將所形成之懸浮液在(TC下授㈣分H㈣ 溫下15分鐘。然後’將反應物以醚稀釋,且以1N HC1水溶 液使反應淬滅。分離水層,並以醚逆萃取。將合併之有機 萃液以IN Na0H水溶液、水及鹽水進—步洗條,以恥抑 脫水乾燥’過濾,及使濾液在真空中濃縮,而得標題化合 物,為褐色油。 步驟6. 3-[3’4-二氣_5_({[(u_二甲基乙基)(二曱基)石夕烷基]氧基} 曱基)苯基]丙腈 於得自前一步驟之甲烷磺酸2_[3,4_二氣_5_({[(11二曱基乙 基)(一曱基)石夕烧基]氧基}曱基)苯基]乙自旨(1當量)之DMSO (0.4M)溶液中,添加氰化鉀(13當量)。將所形成之溶液在8〇 C下攪拌4小時。然後,將反應物以醚稀釋,並以水使反應 淬滅。分離水層,且以醚逆萃取。將合併之有機萃液以水 與鹽水進一步洗滌,以N^SO4脫水乾燥,過濾,及使濾液 在真空中濃縮’而得標題化合物,為粉紅色油。 步驟7 : 3-[3,4-二氣-5-(經甲基)苯基]丙腈 於得自前一步驟之3-[3,4-二氣-5-({[(l,l-二曱基乙基)(二甲 基)石夕烷基]氧基}曱基)苯基]丙腈(1當量)之THF (0·1Μ)溶液 中,添加TBAF (1.0Μ THF溶液,1.2當量·)。將所形成之溶液 在室溫下攪拌3小時。然後,將反應物以醚稀釋,並以水使 反應淬滅。分離水層,且以醚逆萃取。將合併之有機萃液 以水與鹽水進一步洗滌,以Na2S04脫水乾燥,過濾,及使 濾液在真空中濃縮。如此獲得之粗產物經由急驟式層析之 143482·】 -94- 201111364 純化(Si〇2 ’ 9:1 (v/v)己烷:EtOAc-^ 3:7 (v/v)己烷:EtOAc),獲 得標題化合物,為無色油。 步驟8 : 3-(3,4-二氯_5-甲醯基苯基)丙腈 在0°C下’於得自前一步驟之3-[3,4-二氣-5-(羥甲基)苯基] 丙腈(1當量)與碳酸氫鈉(1.1當量)在二氣曱烷(0.1M)中之懸 浮液内’添加DMP (1.1當量)^將所形成之混合物於室溫下 授拌2小時,然後以飽和NaHS03水溶液使反應淬滅,接著以The NaOH aqueous solution, water and brine were further washed, dried over Na 2 SO 4 , and filtered. The filtrate was concentrated in vacuo to give crystallite crystallite Step 6: 3-{8-[(cyclopropyl{[(U-dimethylethyl)oxy)carbonyl}amino)methyl]-6-quinolinyl}-2-propenoic acid methyl ester in hydrazine 1,1-dimethylethyl ester (1 equivalent) in dioxane (1) obtained from the previous step in cyclopropyl [(6-methylindenyl-8 oxalinyl) hydrazinyl] (Diphenylphosphoranylidene) decyl acetate (11 equivalents) was added to the solution in 〇6M). The resulting solution was then slowly warmed to room temperature over 4 hours. Next, the volatiles are removed in a vacuum. The crude product thus obtained is purified by flash chromatography (Si〇2, 9:1 (v/v) hexane: Et0Ac_ 3:7 (v/v) hexane: Et 〇Ac), 143482-1 •87 · 201111364 The title compound is obtained as a white solid. Step 7: 3-{8-[(cyclopropyl{[(1 l 甲甲 | 土mi'i-methylethyl)oxy] benzylamino) Mercapto]-6-P-quinein}methyl-propionate is the 3-sided cyclopropyl{[(U-dimethylethyl)oxyl)amino)methyl]-6 from the previous step. -4 啉 基 _2 _2 _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ Pump down and repeat the filling with hydrogen. Finally, the reaction suspension was stirred for 3 hours under a hydrogen-filled gas cylinder atmosphere. The reaction was quenched by the addition of methylene chloride and filtered through a pad of Celite. Then, the filtrate was concentrated in a vacuum. The crude product thus obtained was purified by flash chromatography (yield: </ RTI> </ RTI> <RTIgt; </RTI> <RTIgt; </RTI> <RTIgt; Step 8: cyclopropyl {[6-(3-hydroxypropyl)_8-quinolinyl]methyl}carbamic acid la dimethyl ethyl ester from the previous step 3·{8_[(cyclopropyl) ([(1)^Dimercaptoethyl)oxy]carbonyl}amino)indenyl]-6-4 phenyl}}-propionic acid propionate q equivalent) in a solution of THF (〇〇8Μ), added hydrogenation Lithium (5 equivalents). The resulting mixture was stirred at room temperature for 14 hours' then diluted with ether and quenched with 1N aqueous NaH. The aqueous layer was separated and back extracted with ether. The combined organic extracts were further washed with water and brine, dried over Na.sub.2, and filtered. The broth was concentrated in vacuo to give the crude title compound. Step 9: Cyclopropyl ({6-[3-(decyloxy)propyl]-8-4 phenyl}} yl} carbamic acid 1,1-dimercaptoacetate for the ring from the previous step Propyl {[6_(3-hydroxypropyl)-8-quinolinyl]methyl} 143482-1 -88- 201111364 Amino acid ι,ι-dimethylethyl ester U equivalent) in THF (0 3M) Adding hydrogenation (60% (w/w) dispersion in paraffin oil, L2 equivalent) in the solution. The resulting suspension was stirred at room temperature for 15 minutes and then added with decane (14 equivalents) ). The current yellow solution was stirred at room temperature for 12 hours then quenched by aqueous EtOAc. The aqueous layer was separated and extracted by hiccup. The combined organic extracts were further washed with water and brine, and dried with Na2 dehydration, and the mixture was allowed to react in a vacuum. The crude product thus obtained was purified by flash chromatography (EtOAc EtOAc (EtOAc) Step 10: Amine 23 is obtained from the previous step of 1,1-didecylethyl ({6-[3-(methoxy)propyl]indolyl)methyl}carbamic acid (1). Equivalent) In a solution of CH2Cl2 (〇〇6M), add HCl (4.0M in 3D equivalents in dioxane). Mix the formed solution for 6 hours at room temperature. Then, in NaOH The aqueous solution was quenched with EtOAc (EtOAc)EtOAc. Amine 24 N-({3-carbyl-5-[3-(indolyl)propyl]phenylindenyl)cyclopropylamine Step 1: N-[(3-Molyl-5-phenyl)曱 ]] cyclopropylamine in 3-bromo-5-gasbenzaldehyde (1 equivalent) and cyclopropylamine (u equivalent) in 4:1 (v/v) MeOH: THF solution (0.06 M) Subsequent addition of sodium cyanoborohydride (丄5 eq.) was followed by pure acetic acid (3 eq.). The resulting mixture was stirred at room temperature for 20 hr. then the volatile material was removed in vacuo. -1 -89- 201111364 The residue is dissolved The aqueous layer was separated with EtOAc (EtOAc)EtOAc. , as a yellow oil. Step 2: N-({3-carbyl-5-[(1E)-3-(methoxy)4-propenyl]phenyl}methyl)cyclopropylamine from the previous step N-[(3-Molyl-5-phenylphenyl)indolyl]cyclopropylamine (1 equivalent) and 4,4,5,5-tetradecyl-2-[(1Ε)-3-(oxime Base) + propylene small group h, 3 2 dioxonium (2 equivalents) of 4:1 (v/v) DMF: n-propanol solution (〇15M), add trans-di-di-diyl double ( Triphenylphosphine (11) (0.05 equivalents) followed by sodium carbonate (2M in water, 3 eq.). The reaction vessel was evacuated and purged with nitrogen five times and then heated at 100 ° C for 2 hours. The cooled reaction mixture was poured into a saturated aqueous solution of NH.sub.4Cl.sub.sub.sub.sub.sub.sub.sub.sub.sub.sub.sub.sub. Crude product Purification (Si02 '3.7 (v/v) hexanes: EtOAc-EtOAc) EtOAc. 5-[(1Ε)-3-(decyloxy)+propen-1-yl]benyl}mercapto)cyclopropylamine (1 eq.) in EtOAc (0.2M). w/w) 'On carbon, 〇. 4 equivalents). The reaction vessel was evacuated and hydrogenated twice with hydrogen, then stirred at room temperature for 14 hours. Next, the reaction suspension was filtered through a silicone pad and the insoluble material was rinsed with Et〇Ac. The filtrate was concentrated in vacuo to give the title compound as a pale green oil. 143482-1 -90- 201111364 Amine 25 Ν-{[1-(3-Methoxypropyl hydrazin-3-yl)indolyl}cyclopropylamine Step 1: 1-(3-methoxypropyl)_ih-啕嗓_3_ Rebel is placed in a dmf (0.1M) solution of indole-3-carboxyfurfural (1 equivalent) at 0 C, adding sodium hydride (60% (w/w) in oil) The dispersion, 丨丨 equivalent), followed by 1-bromo-3-indolylpropane (m·5 eq. p. The reaction mixture was stirred at 5 〇 &lt;&gt;c for 4 hours. Then, the mixture was diluted with ether Washed with water and brine, dehydrated with MgS〇4, filtered, and concentrated in vacuo. The crude product thus obtained was purified by flash chromatography (Si〇2, 1:1 (v/v) Hexane: a 〇Ac-EtO Ac), the title compound was obtained as a colorless oil. Step 2: Amine 25 at 0 C in 1-(3-methoxypropyl-Bu-Zhu-3-Jiejia Road (1) Equivalent) 3:1 (Wv): MeOH solution (0.1 M) was added with cyclopropylamine (2 eq.) &apos; acetic acid (2.5 eq.), followed by sodium trioxy borohydride (15 eq.). The reaction was slowly warmed to room temperature and stirred at room temperature for 3 hours. Then, saturated aqueous solution of NaHC? It should be quenched, extracted with di-methane, dehydrated with MgSO 4 , filtered, and concentrated in vacuo. The crude product thus obtained was purified by flash chromatography (Si 〇 2, 96:4 (v/) v) CH2Cl2: 2.0M NH3 in · 〇Η 'The title compound is obtained as a colorless oil. Amine 26 3-{3,4-dis-5-[(cyclopropylamino)indolyl]phenyl propyl Nitrile Step 1: (5-Bromo-2,3-dioxaphenyl) decyl alcohol at 〇 ° C, obtained from the amine S step 基 _2 2, 3 _ 2 gas aldehyde (1 equivalent) 5 :1(Wv)Me0H: In a THF solution (0.38 M), sodium borohydride 143482-1 -91 - 201111364 (U equivalent) was added in portions over 45 minutes. The reaction solution was stirred at 〇t: for 2 hours. The volatiles are then removed in a vacuum. The resulting residue is then subjected to a liquid separation between the aqueous solution and the aqueous solution. The aqueous layer is separated and stripped with ether. The combined organic extract is 1N. The aqueous solution of Na〇H, water and brine are further washed with dehydrated Na2SO4, dried, and concentrated in vacuo. The crude product thus obtained is purified by flash chromatography (10), 9:1 ( v/v) burned: Et0Ac 3:7 (v/v) hexanes: EtOAc (EtOAc: EtOAc) Adding (u dimethylethyl) dimethyl decane to a solution of (5·bromo-2-,3-diphenyl) sterol (1 eq.) in DMF (0.34 M) from the previous step Base (11-decylethyl) dimethyl decane (U equivalent) with imidazole (1,5 equivalents). The resulting yellow solution was stirred at room temperature for 16 hours. Then, the reaction mixture was diluted with ether and washed successively with a 10% aqueous HCl solution of water and brine. The ether extract was dehydrated to dryness with Na.sub.2.sub.4, and the title compound was obtained as a colorless oil. Step 3: {[(2,3-Dichloro-5-vinylphenyl)indolyl]oxy}(11-didecylethyl)dimethyloxane will be obtained from the previous step {[(5_bromo) Base 2,3_di-phenylphenyl)indolyl]oxy}(u-monomethylethyl)didecyldecane (1 equivalent) with 2 vinyl _445,5 tetramethyl-1,3,2 - Monooxonil (1 equivalent) was combined in a 2:1 (v/v) mixture of DMF: n_pr〇H (0.11 M). Then, to this solution, palladium acetate (9) (5 eq.) and triphenylphosphine (0.15 equivalent) were added, and then the vessel was repeatedly evacuated and counter-filled with nitrogen. 143482-1 -92· 201111364 Finally, an aqueous solution of INNa^O3 (2 equivalents) was added, and the resulting two-phase suspension was heated at 90 ° C for 8 hours. The current black suspension was allowed to cool to room temperature, diluted with water and extracted with 1:1 (v/v) hexanes: ether. The combined organic extracts were then further washed with aqueous IN NaOH 'water and brine. Then, the title compound was obtained as a black oil. Step 4: 2-[3,4-Dioxa-5-({[l,l-dimethylethyl)(dimethyl)decyl]oxy}methyl)phenyl]ethanol will be obtained from the former {[(2,3·二气_5_vinylphenyl)indenyl]oxyku-dimethylethyl)didecyldecane (1 equivalent) '[Ir(COD)a]2 (0025 eq.) and DPPB (0.05 eq.) were combined in THF (0·11 Μ). Then, 4,4,5,5-tetradecyl-indole, 3,2-dioxaboron (1.3 eq.) was added to the solution, and the resulting red solution was stirred at room temperature for 16 hours. . Finally, sodium perborate (〇'1Μ aqueous solution' 1 equivalent was added and the current black two-phase solution was vigorously searched for 8 hours at room temperature. The aqueous layer was separated and stripped with ether. Then, the combined organic extracts were combined. It was further washed with aq. NaOH, water and brine, then dried over Na2SO4, filtered, and concentrated to give a black oil in vacuo. The crude product thus obtained was purified by flash chromatography. SiO 2 '9:1 (v/v) hexanes: EtOAc (EtOAc): _Dichloro_5_({[(u_didecylethyl)(diindenyl) fluorenyl]oxy}methyl)phenyl]ethyl ester at o °c 'from the previous step _ 2_ [3 4_二气_5_(丨[(11-dimethylethyl)(didecyl)decyl]oxyindenyl)phenyl]ethanol (1 equivalent) of dioxane 143482-1 - 93· 201111364 Add a Humg test (15 equivalents) and a gasified formazan (1) equivalent in a solution of the burnt (〇.11Μ) solution. The suspension formed is given at (TC) sub-H (four) temperature 15 Minutes. Then 'put the reaction to Dilute and quench the reaction with 1N aqueous HCl solution. The aqueous layer was separated and extracted with ether. The combined organic extracts were washed with IN Na0H aqueous solution, water and brine, and dried under reduced pressure. And the filtrate is concentrated in vacuo to give the title compound as a brown oil. Step 6. 3-[3'4-di-gas_5_({[(u-dimethylethyl))) Alkyl]oxy} decyl)phenyl]propionitrile in the previous step of methanesulfonic acid 2_[3,4_digas_5_({[(11-didecylethyl))) Addition of potassium cyanide (13 equivalents) to a solution of DMSO (0.4 M) in DMSO (0.4 eq.). The resulting solution was stirred at 8 ° C. Then, the reaction was diluted with ether and the reaction was quenched with water. The aqueous layer was separated and extracted with ether. The combined organic extracts were washed with water and brine, dried over N?SO? And the filtrate is concentrated in vacuo to give the title compound as a pink oil. Step 7: 3-[3,4-dis-5-(methyl)phenyl]propanenitrile from the previous step 3-[3,4-digas-5-({[(l, Add TBAF (1.0 Μ THF solution) to a solution of l-dimercaptoethyl)(dimethyl)oxalyl]oxy}mercapto)phenyl]propanenitrile (1 eq.) in THF (0·1 Μ) 1.2 equivalents.) The resulting solution was stirred at room temperature for 3 hours. Then, the reaction was diluted with ether and quenched with water. The aqueous layer was separated and extracted with ether. The extract was further washed with water and brine, dried over Na2SO4, filtered, and then evaporated. The crude product thus obtained was purified by flash chromatography 143482·] -94- 201111364 (Si 〇 2 ' 9:1 (v/v) hexane: EtOAc-^ 3:7 (v/v) hexane: EtOAc The title compound was obtained as a colorless oil. Step 8: 3-(3,4-Dichloro-5-methylphenyl)propionitrile at 0 ° C in 3-[3,4-digas-5-(hydroxyl) obtained from the previous step Add a DMP (1.1 eq.) to a suspension of phenyl]propionitrile (1 eq.) and sodium bicarbonate (1.1 eq.) in dioxane (0.1 M). The mixture was stirred for 2 hours, then the reaction was quenched with saturated aqueous NaHS03, then

Et2〇萃取。將合併之有機萃液以IN NaOH水溶液、水及鹽水 進一步洗務’以NhSO4脫水乾燥,及過濾。濾液在真空中 之濃縮,獲得粗製標題化合物,為白色固體。 步驟9 :胺26Et2〇 extraction. The combined organic extracts were further washed with aqueous 1N NaOH, water and brine. The filtrate was concentrated in vacuo to give crystallite crystallite Step 9: Amine 26

於得自前一步驟之3_(3,4_二氣_5_曱醯基苯基)丙腈(1當量) 之二氣甲烷(0.11M)溶液中,添加硫酸鎂(1當量)與環丙基胺 (1.2當里)。將所形成之懸浮液在室溫下攪拌16小時。經由 過濾:除不溶物,並以二氣甲烧沖洗,然後使合併之遽液 :真肀/辰縮。使如此獲得之粗製亞胺溶於甲醇(011M)中, 接著分次添加硼氫化鈉(3當量)。將反應混合物在室溫下攪 拌16小時。然後,於真空中移除揮發性物質,且使所形成 之殘留物於㈣1N Na〇H水溶液之間作分液處理。分離水 層’並以㈣萃取。將合併之有機萃液以水與鹽水進一步 洗條’以㈣抑脫水乾燥,過濾',及使渡液在真空中濃縮。 如此獲得之粗產物經由急驟式層析之純化⑽2,9:丄㈣己 烧:Et0AC—Et0AC) ’獲得標題化合物,為益色油。 胺27 143482-1 -95- 201111364 N-(2-{3,4-二氣-5-[(環丙胺基)曱基]苯基}乙基)丙醯胺 步驟1 : ({[5-(2-疊氮基乙基)_2,3_二氣苯基]曱基}氧基)(u_二曱 基乙基)二甲基矽烷 在室溫下’於得自胺26步驟5之曱烷磺酸2_[3,4_二氣_5_ ({[(l’l-二甲基乙基)(二曱基)矽烷基]氧基}曱基)苯基]乙酯(1 當罝)之DMF (0.4M)溶液中,添加疊氮化鈉(5當量)。將所形 成之溶液在室溫下攪拌丨2小時,然後於8〇°c下3小時。接著, 將反應混合物以醚稀釋,並以水洗滌。分離水層,且以醚 逆萃取。將合併之有機萃液以水與鹽水進一步洗滌,以 Naz SO4脫水乾燥,過濾,及使濾液在真空中濃縮,而得粗 製標題化合物’為粉紅色油。 步驟2: 2-[3,4-二氣-5_({[(u_:甲基乙基)(二甲基)石夕烧基]氧基) 甲基)苯基]乙胺 於得自前一步驟之({ [5-(2_疊氮基乙基)_2,3二氣苯基]甲基} 氧基)(1’1 一甲基乙基)二曱基矽烷〇當量)與三苯膦(1 2當 ,添加水(3當量)。將所形成之溶液Add magnesium sulfate (1 equivalent) and cyclopropane to a solution of 3_(3,4_diqi_5-nonylphenyl)propanenitrile (1 eq.) in dioxane (0.11 M) from the previous step. Amine (1.2 inside). The resulting suspension was stirred at room temperature for 16 hours. By filtration: In addition to insoluble matter, and rinsed with two gas, then the combined mash: true 辰 / 缩. The crude imine thus obtained was dissolved in methanol (011 M), followed by sodium borohydride (3 eq.). The reaction mixture was stirred at room temperature for 16 hours. Then, the volatile matter was removed in a vacuum, and the resulting residue was subjected to liquid separation between (iv) 1N Na〇H aqueous solution. The aqueous layer was separated and extracted by (iv). The combined organic extracts were further washed with water and brine to dryness, filtered, and concentrated in vacuo. The crude product thus obtained was purified by flash chromatography (10) 2, 9: y (yield: EtOAc: EtOAc (EtOAc) Amine 27 143482-1 -95- 201111364 N-(2-{3,4-dioxa-5-[(cyclopropylamino)indolyl]phenyl}ethyl)propanamide Step 1: ({[5- (2-Azidoethyl)_2,3-dioxaphenyl]indolyl}oxy)(u-didecylethyl)dimethyl decane at room temperature in step 5 of amine 26 2,[3,4_diox_5_({[(l'l-dimethylethyl)(didecyl)decyl]oxy}indolyl)phenyl]ethyl sulfonate (1 Add sodium azide (5 equivalents) to a solution of DMF (0.4 M) in 罝). The resulting solution was stirred at room temperature for 2 hours and then at 8 ° C for 3 hours. Next, the reaction mixture was diluted with ether and washed with water. The aqueous layer was separated and extracted with ether. The combined organic extracts were washed with EtOAc EtOAc EtOAc. Step 2: 2-[3,4-Digas-5-({[(u_:methylethyl)(dimethyl)))]oxy)methyl)phenyl]ethylamine from the previous Step ({ [5-(2_azidoethyl)_2,3 dioxaphenyl]methyl}oxy)(1'1 monomethylethyl)didecyldecane oxime equivalent) with triphenyl Phosphine (1 2 when, add water (3 equivalents). The solution formed

罝)之THF (0.1M)溶液中,添加 在50°C下攪拌18小時。然後,In THF (0.1 M) solution, the mixture was stirred at 50 ° C for 18 hours. then,

氧基}甲基)苯基]-乙基}丙醯胺Oxy}methyl)phenyl]-ethyl}propanamide

、Hunig氏鹼(3當量) 143482-1 •96· 201111364 及丙酸(1.1當量)之DMF (0.2M)溶液中,分次添加六氟磷酸 0-(7-氮苯并三唑-1-基)-N,N,N’,N,-四曱基錁(ι·2當量)。將所形 成之反應溶液在室溫下攪拌48小時。將目前帶紅色溶液以 醚稀釋,並以IN NaOH水溶液、水及鹽水相繼洗滌。然後, 使有機萃液以Na2S〇4脫水乾燥,過濾,及使濾液在真空中 濃縮,而得褐色油。如此獲得之粗產物經由急驟式層析之 純化(Si02 ’ 7:3 (v/v)己院:EtOAc— Et0Ac),獲得標題化合物, 為無色油。 _ 步驟4 ·· N-{2-[3,4-二氯-5-(經甲基)苯基]乙基}丙醯胺 於得自前一步驟之N-{2-[3,4-二氯-5-({[(1,1_二甲基乙基)(二 甲基)石夕燒基]氧基}甲基)苯基]乙基丨丙酿胺q當量)之THF (0.12M)溶液中’添加TBAF (1·〇Μ THF溶液,i乂當量)。將所 形成之溶液在室溫下攪拌2小時。將目前橘色溶液以醚稀 釋,並以IN NaOH水溶液使反應淬滅。分離水層,且以醚逆 萃取。將合併之有機萃液以水與鹽水進一步洗滌,以Na2 s 〇4 _ 脫水乾燥,及過濾。濾液在真空中之濃縮,獲得粗製標題 化合物’為淡黃色油。 步驟5 : N-[2-(3,4-二氣_5_甲醯基苯基)乙基]丙醯胺 在〇°C下,於得自前一步驟之n_{2_[3,4_二氣_5_(羥甲基)苯基] 乙基1丙醯胺(1當量)與碳酸氩鈉(U當量)在二氣曱烷(0.1M) 中之懸浮液内,添MDMP 當量)。將所形成之混合物於 至溫下攪拌2小時,然後以飽和NaHS〇3水溶液使反應淬滅, 接著以Εΐ;2〇萃取。將合併之有機萃液以1N Na〇H水溶液、水 及鹽水進一步洗滌,以N^SO4脫水乾燥,過濾,及使濾液 143482-1 -97- 201111364 析之純化 ’獲得標 在真空中濃縮。如此獲得之粗產物經由急驟式層 (Si〇2 ’ 19.1 (v/v)己院:Et〇Ac— 3:7 (v/v)己烷:Et〇Ac) 題化合物’為白色固體。 步驟6 :胺27 於得自前-步驟之叫(3,4_二氣_5甲醯基苯基)·乙基]丙酿 胺(1當量)之二氣甲烷(〇 11M)溶液中,添加硫酸鎂U當量) 與環丙基胺(1.2當量)。將所形成之懸浮液在室溫下授掉^ 小時。經由過濾移除不溶物’並以二氯曱烷沖〉先,然後使 合併之濾液在真空中濃縮。使如此獲得之粗製亞胺溶於曱 醇(0.11M)中,接著分次添加硼氫化鈉(1 5當量)。將反應混 合物在室溫下攪拌8小時。然後,於真空中移除揮發性物質, 且使所形成之殘留物於Et0Ac與1N Na〇H水溶液之間作分液 處理。分離水層,並以Et〇Ac逆萃取。將合併之有機萃液以 水與鹽水進一步洗滌,以Na2S〇4脫水乾燥,過濾,及使濾 液在真空中濃縮。如此獲得之粗產物經由急驟式層析之純 化(Si〇2 ’ 95:5 CI^Cl2 :在MeOH 中之2.0M NH3),獲得標題化 合物,為無色油。 胺28 N-[3-溴基-5-(3-曱氧基丙基)芊基]環丙胺 步驟1 : 3-溴基-5-(3-曱氧基丙基)苯甲醛 在室溫下,於烯丙基甲基醚(3J當量)之THF溶液(〇 3M) 中,添加硼烧-硫化曱烷複合物(1·〇當量)。將此溶液在室溫 下攪拌30分鐘。然後,於此溶液中,相繼地添加3 5二溴基 苯甲醛(1.0當量)、Pd(dppf)Cl2(0O25當量)及固體曱醇鈉(1 5當 143482-1 -98- 201111364 里)。將所形成之混合物加熱至回流,歷經丨5小時。將已冷 卻之反應混合物以水稀釋,且以醚萃取。使合併之有機萃 液以MgS〇4脫水乾燥,過濾,及使濾液在真空中濃縮。如此 獲得之粗產物經由急驟式層析之純化(Si〇2,5·95, Hunig's base (3 equivalents) 143482-1 • 96· 201111364 and propionic acid (1.1 equivalents) in DMF (0.2M) solution, adding hexafluorophosphate 0-(7-nitrobenzotriazole-1-) Base) - N, N, N', N, - tetradecyl hydrazine (1⁄2 eq.). The resulting reaction solution was stirred at room temperature for 48 hours. The current reddish solution was diluted with ether and washed successively with 1N aqueous NaOH, water and brine. Then, the organic extract was dried over Na2SO4, filtered, and the filtrate was concentrated in vacuo to give brown oil. The crude product thus obtained was purified by flash chromatography (EtOAc: EtOAc (EtOAc) _ Step 4 ·· N-{2-[3,4-Dichloro-5-(methyl)phenyl]ethyl}propanamine in N-{2-[3,4- from the previous step Dichloro-5-({[(1,1-dimethylethyl)(dimethyl)) oxo]oxy}methyl)phenyl]ethyl hydrazinamine q equivalent) of THF ( Add TBAF (1·〇Μ THF solution, i乂 equivalent) in 0.12 M) solution. The resulting solution was stirred at room temperature for 2 hours. The current orange solution was diluted with ether and quenched with aqueous 1N NaOH. The aqueous layer was separated and extracted with ether. The combined organic extracts were further washed with water and brine, dried over Na 2 s 〇 4 _, and filtered. The filtrate was concentrated in vacuo to give crude title compound <RTI ID=0.0> Step 5: N-[2-(3,4-dioxa_5-methylnonylphenyl)ethyl]propanamide at 〇°C, n_{2_[3,4_ from the previous step Dioxo_5_(hydroxymethyl)phenyl]ethyl 1 propylamine (1 eq.) and sodium argon carbonate (U eq.) in a suspension of dioxane (0.1 M), MDMP equivalent). The resulting mixture was stirred at ambient temperature for 2 hours, then quenched with saturated aqueous NaH.sub.3, and then extracted with EtOAc. The combined organic extracts were further washed with aq. 1N NaHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHHH The crude product thus obtained was passed through a flash layer (Si 〇 2 ' 19.1 (v/v) hexane: Et 〇Ac-3:7 (v/v) hexane: Et 〇Ac). Step 6: Amine 27 is added to a solution of di-methane (〇11M) obtained from the pre-step (3,4_dioxa-5-nonylphenyl)ethyl] arylamine (1 equivalent). Magnesium sulfate U equivalent) with cyclopropylamine (1.2 equivalents). The resulting suspension was allowed to stand at room temperature for an hour. The insolubles were removed via filtration and washed with dichloromethane, then the combined filtrate was concentrated in vacuo. The crude imine thus obtained was dissolved in decyl alcohol (0.11 M), followed by sodium borohydride (15 eq.). The reaction mixture was stirred at room temperature for 8 hours. Then, the volatile matter was removed in a vacuum, and the resulting residue was subjected to liquid separation between Et0Ac and 1N Na〇H aqueous solution. The aqueous layer was separated and back-extracted with Et 〇Ac. The combined organic extracts were further washed with water and brine, dried over Na.sub.2.sub.4, filtered, and concentrated in vacuo. The crude product thus obtained was purified by flash chromatography (EtOAc: EtOAc: EtOAc: EtOAc Amine 28 N-[3-Bromo-5-(3-decyloxypropyl)decyl]cyclopropylamine Step 1: 3-Bromo-5-(3-methoxypropyl)benzaldehyde at room temperature Next, a borax-sulfurized decane complex (1·〇 equivalent) was added to a solution of allylic methyl ether (3 J equivalent) in THF (〇3M). This solution was stirred at room temperature for 30 minutes. Then, in this solution, 3 5 dibromobenzaldehyde (1.0 equivalent), Pd (dppf) Cl 2 (0 25 equivalent), and solid sodium decoxide (1 5 when 143482-1 - 98 - 201111364) were successively added. The resulting mixture was heated to reflux and allowed to stand for 5 hours. The cooled reaction mixture was diluted with water and extracted with ether. The combined organic extracts were dried over MgSO.sub.4, filtered and evaporated. The crude product thus obtained is purified by flash chromatography (Si〇2, 5.95)

EtOAc:己烷— 7:3(v/v)Et〇Ac:己烷),獲得標題化合物,為 無色油。 步驟2 :胺28 _ 將得自前—步驟之3-溴基-5-(3-甲氧基丙基)苯甲醛(1當 里)與環丙基胺(2當量)合併於CH2 (¾ (0.19M)中。然後,於其 中添加MgS〇4(l當量),並將所形成之懸浮液在室溫下攪拌 23小時。然後,經由過濾,經過矽藻土墊移除不溶物,及 使濾液在真空中濃縮。接著,使如此獲得之粗製亞胺再溶 於MeOH (0.19M)中。於此溶液中,分次添加硼氫化鈉(1.5當 量),且將所形成之混合物在〇t:下攪拌3〇分鐘,然後於室 溫下16小時。藉由與2N HC1水溶液一起攪拌3〇分鐘而使反 • 應淬滅。接著,以INNaOH水溶液使所形成之混合物鹼化, 並在真空中移除揮發性物質。將殘留物自水以萃取, 以Na2S〇4脫水乾燥,過濾,及使濾液在真空中濃縮,而得 標題化合物,為無色油。 胺29 4-[(環丙胺基)甲基]-N-[2-(甲氧基)乙基]_2_茶胺 步驟1 : 3-{[2-(甲氧基)乙基]胺基}小莕羧酸甲酯 將剛純化之碳酸铯(1.4當量)、醋酸鈀⑼(〇 〇2當量)及外 消旋-BINAP (0.03當量)合併於無水甲苯(〇 25M)中。將容器重 143482-1 •99- 201111364 複抽氣’並以氮逆充填。最後,添加3-溴基小萘羧酸甲酯(1 當量)與2-曱氧基乙胺(1.2當量),且將所形成之混合物於1〇〇 C下加熱20小時。使目前黑色懸浮液冷卻至室溫,以醚稀 釋’並經過矽藻土墊過濾。濾液在真空中之濃縮,獲得褐 色油’可使其經由管柱層析進一步純化⑸〇2,19:1 (v/v)己 烧:EtOAc— 1:1 (v/v)己烷:Et〇Ac) ’而得標題化合物,為黃 色油。 步驟2 : 3-{[2-(曱氧基)乙基]胺基}小茶甲酸 使得自前一步驟之3_{[2_(甲氧基)乙基]胺基丨小莕羧酸甲鲁 自曰(1當量)溶於MeOH: THF之2:1 (v/v)混合物(〇.〇8M)中。然後, 於此溶液中,添加LiOH (1ΌΜ水溶液,3.4當量),並將所形 成之混濁溶液在室溫下激烈攪拌16小時。接著,於真空中 移除揮發性物質,且以1NHC1水溶液將殘留物之pH值小心 地調整至〜2,然後將其以Et〇Ac萃取。將合併之有機萃液以 水與鹽水進一步洗滌,以NasSO4脫水乾燥,及過濾。濾液 在真中之濃,獲得標題化合物,為黃色固體。 步驟3 : N-環丙基·3·{[2_(甲氧基)乙基]胺基H茶羧醯胺 · 於得自前一步驟之3-丨[2-(曱氧基)乙基]胺基丨莕曱酸(1當 量)、Hunig氏鹼(3當量)及環丙基胺(1 5當量)之dmf (〇 im) 溶液中,分次添加六氟磷酸〇_(7_氮苯并三唑小基)n,n,n,,N,_ 四甲基錁(1.2當量)。將所形成之反應溶液在室溫下攪拌48 小時。將目前帶紅色溶液以Et0Ac稀釋,並以1N Na〇H水溶 液、水及鹽水相繼洗滌。然後,使有機萃液wNa2s〇4脫水 乾燥,過濾,及使濾液在真空中濃縮,而得褐色油。如此 143482-1 •100· 201111364 獲得之粗產物經由急驟式層析之純化(Si〇2,4:1 (v/v)己烷: EtOAc— EtOAc) ’獲得標題化合物,為白色固體。 步驟4:胺29 在回流下,於得自前一步驟之N_環丙基_3_{[2_(曱氧基)乙 基]胺基H-蒸羧醯胺(1當量)之THF溶液(0.09M)中,添加硼烷 -硫化曱烷複合物(6.2當量)^然後,將短路徑蒸餾裝置連接 至反應谷器’並慢慢地蒸德出大部份揮發性物質,歷經1 ^ 小時期間。使目前褐色溶液再冷卻至Ot:,且以IN HC1水溶 液小心地使反應泮滅。將所形成之混合物於回流下加熱1 小時,以確保胺-蝴烧複合物之完全分解。在以IN NaOH水 溶液小心中和之後,分離水層,並以Et0Ac逆萃取。將合併 之有機萃液以鹽水洗滌,以NaaSO4脫水乾燥,及過渡。使 濾液在真空中濃縮,並使如此獲得之粗產物經由急驟式層 析進一步純化(Si02,3:2 (v/v)己烷:EtOAc— EtOAc),以顯示 標題化合物,為黃色油,其係於靜置時快速地變深。 • 胺30 3-{8-[(環丙胺基)曱基]-6-4啉基丨丙腈 步驟1 : {[6-(2-氰基乙稀基)-8-峻》林基]甲基}環丙基胺基曱酸 1,1-二曱基乙酯 於剛乾燥之氣化鋰(1.2當量)與(氰基曱基)膦酸二乙顆(1 2 當量)之THF (0.13M)懸浮液中,添加DBU (1.2當量)。將反應 懸浮液在室溫下攪拌30分鐘,接著,最後添加環丙基[(6甲 醯基各喹啉基)曱基]胺基曱酸1,1-二曱基乙酯(1當量,胺23 步驟5)。然後,將所形成之溶液於室溫下攪拌16小時。、 143482-1 201111364 10% HC1水溶液使如此獲得之粗製反應混合物淬滅,且以醚 萃取。將合併之有機萃液以IN NaOH水溶液、水及鹽水進一 步洗滌’以Na2 S04脫水乾燥’過濾,及使濾液在真空中濃 縮。如此獲得之粗產物經由急驟式層析之純化(Si〇2,9:1 (v/v) 己烧:EtOAc— 3:7 (v/v)己烧:EtOAc),獲得標題化合物,為 白色固體。 步驟2 : {[6-(2-氰基乙基)-8-喹啉基]甲基}環丙基胺基曱酸ι,ι_ 二曱基乙酯 於得自前一步驟之{[6-(2-氰基乙烯基)-8-喹啉基]曱基}環 丙基胺基曱酸1,1_二曱基乙酯(1當量)在Et〇Ac (〇 1M)中之溶 液内’添加鈀(10% (w/w),於碳上,0 2當量)。將所形成之 懸浮液抽氣,並以氫重複逆充填。最後,將反應懸浮液在 經氫充填之氣瓶大氣下攪拌4小時。藉由添加二氯曱烧使反 應淬滅,並經過矽藻土床過濾。然後,使濾液在真空中濃 縮。如此獲得之粗產物經由急驟式層析之純化(si〇2,9:1 (v/v) 己烷:EtOAc— 3:7 (v/v)己烷:EtOAc),獲得標題化合物,為 黃色油。 步驟3 :胺30 於得自前一步驟之{[6-(2-氰基乙基)-8-喳啉基]曱基丨環丙 基胺基甲酸U-二甲基乙醋(1當量)之CW容液(〇_中, 添加溴化鋅(11)(10當量)。使所形成之懸浮液音振15分鐘, '在至咖下攪拌小時。藉由添加Et〇Ac與1N Na〇H水溶液 使反應淬滅,然後音振15分鐘。分離水相,並以Et〇Ac逆萃 取°將合併之有機萃液以水與鹽水進—步絲,以¥〇4 143482-1 -102- 201111364 脫水乾燥,及過濾。據液在真空中之濃縮,獲得標題化合 物,為黃色油。 胺31 N-({3-[2-(曱氧基)乙基]-μ茶基丨甲基)環丙胺 步驟1 : 3-乙稀基-1-茶級酸甲醋 將3-漠基-1-錢酸甲能(1當量)與2_乙稀基々Μ—四甲基 -1,3,2-二氧棚伍園(1當量)合併於DMF : n_pr〇H之2:ι 混合 物(〇·1Μ)中。於此溶液中,首先添加Pd(PPh3)2Br2(0.05當量), 接著為ZNNa2CCVJc溶液(2當量)。將兩相懸浮液抽氣,並以 氛逆充填三次然後將其在贼下加熱8小時。使目前黑色 懸浮液冷卻至室溫,以水稀釋,且以1:1 (v/v)己烷:醚萃取。 接著,將合併之有機萃液以1N Na〇H水溶液、1〇% Ηα水溶 液、水及鹽水進一步洗滌。然後’使其以Na2S〇4脫水乾燥, 並經過矽膠墊片過濾。濾液在真空中之濃縮,獲得粗製標 題化合物’為金黃色油。 φ 步驟2 : 3-(2·羥乙基)-1_莕羧酸曱酯 將得自前一步驟之3_乙烯基莕羧酸曱酯(1當量)、 [Ir(COD)Cl]2 (0.025 當量)及 DPPB (〇.〇5 當量)合併於 THF (0.12M) 中。然後,於此溶液中,添加4,4,5,5_四曱基^二孓二氧硼伍圜 (1.2當量)’並將所形成之紅色溶液在室溫下攪拌16小時。 最後,添加過删酸鈉(0.1M水溶液,2當量),且將目前黑色 兩相/谷液於至溫下再激烈授拌丨2小時。分離水層,並以醚 逆萃取。接著’將合併之有機萃液以1N Na〇H水溶液、水及 鹽水進一步洗滌。然後’使其以Na2S04脫水乾燥,過濾, 143482-1 •103- 201111364 及使;慮液在真二中》辰縮,而得淡黃色油。如此獲得之粗產 物經由急驟式層析之純化(Si〇2,9:1 (v/v)己烷:Et〇Ac—1:1EtOAc: hexane - 7:3 (v/v). Step 2: Amine 28 _ 3-bromo-5-(3-methoxypropyl)benzaldehyde (1 mM) from the previous step was combined with cyclopropylamine (2 eq.) in CH2 (3⁄4 ( Then, MgS〇4 (1 equivalent) was added thereto, and the resulting suspension was stirred at room temperature for 23 hours. Then, through filtration, the insoluble matter was removed through a diatomaceous earth pad, and The filtrate was concentrated in vacuo. The crude imine thus obtained was redissolved in MeOH (0.19 M). To this solution, sodium borohydride (1.5 eq.) was added portionwise and the mixture formed was : stirring for 3 minutes, then at room temperature for 16 hours. The reaction was quenched by stirring with 2N HCl aqueous solution for 3 Torr. Next, the resulting mixture was basified with IN NaOH aqueous solution and vacuum The volatiles are removed. The residue is taken from water, EtOAc (EtOAc m. )methyl]-N-[2-(methoxy)ethyl]_2-theanine Step 1: 3-{[2-(Methoxy)ethyl]amino} oxime carboxy Acid methyl ester The freshly purified cesium carbonate (1.4 eq.), palladium acetate (9) (〇〇2 eq.) and racemic-BINAP (0.03 eq.) were combined in anhydrous toluene (〇25M). The container weighed 143482-1. 99- 201111364 Re-extraction' and filling with nitrogen. Finally, methyl 3-bromo-naphthalenecarboxylate (1 equivalent) and 2-methoxyethylamine (1.2 equivalents) are added, and the resulting mixture is Heat at 20 ° C for 20 hours. Allow the current black suspension to cool to room temperature, dilute with ether and filter through a pad of diatomaceous earth. Concentrate the filtrate in vacuo to give a brown oil. Further purification of (5) 〇2, 19:1 (v/v) hexanes: EtOAc - 1:1 (v/v) hexane: EtOAc (EtOAc) Step 2: 3-{[2-(decyloxy)ethyl]amino}calic acid formic acid 3_{[2_(methoxy)ethyl]amine hydrazide carboxylic acid from the previous step The hydrazine (1 equivalent) was dissolved in a 2:1 (v/v) mixture of MeOH: THF (〇. 〇 8M). Then, LiOH (1 Torr aqueous solution, 3.4 equivalent) was added to the solution, and the resulting turbid solution was vigorously stirred at room temperature for 16 hours. Next, the volatile matter was removed in vacuo, and the pH of the residue was carefully adjusted to &lt;~&gt; The combined organic extracts were further washed with water and brine, dried over NasSO4 and filtered. The filtrate was concentrated in EtOAc to give the title compound as a yellow solid. Step 3: N-cyclopropyl·3·{[2_(methoxy)ethyl]amino H tea carboxamide · 3-[2-(decyloxy)ethyl] from the previous step Addition of bismuth hexafluorophosphate (7-nitrobenzene) in a solution of aminic decanoic acid (1 equivalent), Hunig's base (3 equivalents) and cyclopropylamine (15 equivalents) in dmf (〇im) And triazole small group) n, n, n,, N, _ tetramethyl hydrazine (1.2 equivalents). The resulting reaction solution was stirred at room temperature for 48 hours. The current reddish solution was diluted with Et0Ac and washed sequentially with 1N Na〇H aqueous solution, water and brine. Then, the organic extract wNa2s 〇4 was dehydrated, filtered, and the filtrate was concentrated in vacuo to give a brown oil. Thus 143482-1 • 100· 201111364 The title compound was obtained as a white solid. Step 4: A solution of the N-cyclopropyl_3_{[2_(decyloxy)ethyl]amine H-carboylguanamine (1 eq.) in THF from the previous step. In M), a borane-sulfurized decane complex (6.2 equivalents) is added. Then, a short path distillation apparatus is connected to the reaction vessel' and slowly vaporizes most of the volatile matter over a period of 1 ^ hour. . The current brown solution was again cooled to Ot: and the reaction was carefully quenched with aqueous <RTI ID=0.0># </RTI> The resulting mixture was heated under reflux for 1 hour to ensure complete decomposition of the amine-blow-burning complex. After careful neutralization with aqueous IN NaOH, the aqueous layer was separated and extracted with Et0Ac. The combined organic extracts were washed with brine, dried over Na.sub.2SO.sub.4 and dried. The filtrate was concentrated in vacuo and EtOAc (EtOAc m. It quickly deepens when it is still standing. • Amine 30 3-{8-[(cyclopropylamino)indolyl]-6-4 phenyl hydrazinonitrile Step 1: {[6-(2-Cyanoethylene)-8-Jun] Methyl}cyclopropylamino decanoic acid 1,1-didecylethyl ester in freshly dried lithium (1.2 equivalents) and (cyanomethyl)phosphonic acid (1 2 equivalents) of THF ( In a suspension of 0.13 M), DBU (1.2 equivalents) was added. The reaction suspension was stirred at room temperature for 30 minutes, and finally, 1,1-didecylethyl cyclopropyl [(6-methylindolyl quinolyl) fluorenyl] decanoate (1 equivalent, Amine 23 Step 5). Then, the resulting solution was stirred at room temperature for 16 hours. 143482-1 201111364 10% aqueous HC1 solution The crude reaction mixture thus obtained was quenched and extracted with ether. The combined organic extracts were washed with aq. 1N NaOH, water and brine &lt;&apos;&gt; The crude product thus obtained was purified by flash chromatography (EtOAc: EtOAc (EtOAc:EtOAc) solid. Step 2: {[6-(2-Cyanoethyl)-8-quinolinyl]methyl}cyclopropylamino decanoic acid ι,ι_didecylethyl ester in the previous step {[6- (2-Cyanovinyl)-8-quinolinyl]fluorenyl}cyclopropylamino decanoic acid 1,1-didecylethyl ester (1 equivalent) in EtEAc (〇1M) solution 'Add palladium (10% (w/w) on carbon, 0 2 equivalents). The resulting suspension was evacuated and repeatedly filled with hydrogen. Finally, the reaction suspension was stirred under a hydrogen-filled gas cylinder atmosphere for 4 hours. The reaction was quenched by the addition of dichlorohydrazine and filtered through a bed of diatomaceous earth. Then, the filtrate was concentrated in a vacuum. The crude product thus obtained was purified by flash chromatography eluting elut elut elut elut elut elut elut elut elut oil. Step 3: Amine 30 is obtained from the previous step of {[6-(2-cyanoethyl)-8-carbinyl]hydrazinylcyclopropylcarbamic acid U-dimethylacetic acid (1 equivalent) CW liquid (in _, add zinc bromide (11) (10 equivalents). The resulting suspension was sonicated for 15 minutes, 'stirred under the coffee. By adding Et〇Ac and 1N Na〇 The aqueous solution of H is quenched and then sonicated for 15 minutes. The aqueous phase is separated and subjected to reverse extraction with Et〇Ac. The combined organic extracts are fed with water and brine to a volume of 〇4 143482-1 -102- 201111364 Dehydrated and dried, and filtered. The title compound was obtained as a yellow oil from EtOAc (EtOAc: EtOAc) Cyclopropylamine Step 1: 3-Ethyl-1-butylic acid methyl vinegar 3-Methyl-1-carboxylic acid A (1 equivalent) and 2_Ethyl 々Μ-tetramethyl-1,3 , 2-dioxane shed (1 equivalent) is combined in DMF: n_pr〇H 2: ι mixture (〇·1Μ). In this solution, first add Pd(PPh3)2Br2 (0.05 eq.), followed by ZNNa2CCVJc solution (2 equivalents). The two-phase suspension is evacuated and filled three times with an atmosphere. It was then heated under thieves for 8 hours. The current black suspension was cooled to room temperature, diluted with water and extracted with 1:1 (v/v) hexanes: ether. Next, the combined organic extracts were taken at 1N. The aqueous solution of Na〇H, 1% aqueous solution of Ηα, water and brine were further washed. Then, it was dried over Na 2 SO 4 and filtered through a pad of silica gel. The filtrate was concentrated in vacuo to give crude title compound. Oil φ Step 2: 3-(2·Hydroxyethyl)-1_indole carboxylic acid oxime ester The 3' vinyl carboxylic acid oxime ester (1 equivalent), [Ir(COD)Cl] from the previous step 2 (0.025 eq.) and DPPB (〇.〇5 eq.) were combined in THF (0.12 M). Then, 4,4,5,5-tetradecyl^dioxadifluoride was added to the solution. (1.2 eq.)' and the resulting red solution was stirred at room temperature for 16 hours. Finally, sodium sulphate (0.1 M in water, 2 eq.) was added and the current black phase/cold solution was applied to the temperature. The mixture was vigorously stirred for 2 hours. The aqueous layer was separated and back-extracted with ether. Then the combined organic extracts were further washed with 1N NaH aqueous solution, water and brine. After the 'dehydration and drying with Na2S04, filtration, 143482-1 • 103- 201111364 and the solution; the liquid is in the true two", and the pale yellow oil is obtained. The crude product thus obtained is purified by flash chromatography ( Si〇2,9:1 (v/v) Hexane: Et〇Ac—1:1

EtO Ac .己烧),獲得標題化合物,為淡黃色油。 步驟3 : 3_[2-(曱氧基)乙基]-1-茶羧酸甲酯 使得自前一步驟之3-(2-羥乙基)_1_莕羧酸曱酯(1當量)與 碘曱烷(19當量)溶於THF (0·3Μ)中。然後,於此溶液中,添 加氫化鈉(在油中之60% w/w分散液,1當量),並將所形成 之懸浮液在室溫下’於黑暗中攪拌18小時。接著,於真空 中移除揮發性物質’並使所形成之殘留物於醚與1N 水 /谷液之間作分液處理。分離水層,且以醚逆萃取。然後, 將合併之有機萃液以1N NaOH水溶液、水及鹽水進一步洗 滌。接著’使其以NaaSO4脫水乾燥,過濾,及使濾液在真 二中/辰縮’而得黃色油。如此獲得之粗產物經由急驟式層 析之純化(Si〇2 ’ 19:1 (v/v)己烧:EtOAc— 1:1 (v/v) EtOAc:己烷), 獲得標題化合物,為淡黃色油。 . 步驟4 : {3-[2-(甲氧基)乙基]小茶基}曱醇The title compound was obtained as a pale yellow oil. Step 3: Methyl 3-(2-(decyloxy)ethyl]-1-carboxylate, 3-(2-hydroxyethyl)_1-indolecarboxylate (1 equivalent) and iodine from the previous step The decane (19 equivalents) was dissolved in THF (0.33). Then, to this solution, sodium hydride (60% w/w dispersion in oil, 1 equivalent) was added, and the resulting suspension was stirred at room temperature for 18 hours in the dark. Next, the volatile matter was removed in a vacuum and the resulting residue was subjected to liquid separation between ether and 1N water/cold. The aqueous layer was separated and back extracted with ether. The combined organic extracts were then further washed with 1N aqueous NaOH, water and brine. Then, it was dehydrated and dried with NaaSO4, filtered, and the filtrate was subjected to a second oil to give a yellow oil. The crude product thus obtained was purified by flash chromatography (EtOAc: EtOAc: EtOAc (EtOAc) Yellow oil. Step 4: {3-[2-(Methoxy)ethyl]小茶基} sterol

使得自前一步驟之3_[2-(曱氧基)乙基]小茶羧酸曱酯(1當 置)溶於曱苯(0.1M)中。然後,於此溶液中,添加DIBA1_H 〇 5M 甲苯溶液,2.4當量)’並將所形成之溶液在室溫下激烈授 拌4小時。以1Ν Ηα水溶液使如此獲得之反應混合物淬滅, 且以喊萃取。將合併之有機萃液以水與鹽水進一步洗滌, 以% SO4脫水乾燥’及過遽。濾液在真空中之漠縮,獲得 標題化合物,為無色油。 步驟5 : 3·[2-(甲氧基)乙基]-1-莕羧曱醛 143482-1 201111364 在〇°C下,於得自前一步驟之{3_[2·(甲氧基)乙基]小莕基} 曱醇(1當量)與碳酸氫鈉(1.1當量)在二氯曱烷(01M)中之懸 浮液内,添加DMP (1.1當量)。將所形成之混合物於室溫下 攪拌2小時,然後以飽和NaHS〇3水溶液使反應淬滅’接著以 EhO萃取。將合併之有機萃液以1N Na〇H水溶液、水及鹽水 進一步洗滌,以Na2S〇4脫水乾燥,過濾,及使濾液在真空 中濃縮。如此獲得之粗產物經由急驟式層析之純化(Si〇2, 19:1 (v/v)己烷:Et0Ac— 1:1 (v/v)己烧:Et〇Ac),獲得標題化合 物,為無色油。 步驟6:胺31 於知自前一步驟之3-[2-(甲氧基)乙基]莕羧甲醛(1當量) 之一氣甲烷(0.15M)溶液中,添加硫酸鎂(1當量)與環丙基胺 (1.2當置)。將所形成之懸浮液在室溫下攪拌2〇小時。經由 過濾移除不溶物,並以二氯甲烷沖洗’然後使合併之濾液 在真空中濃縮。使如此獲得之粗製亞胺溶於甲醇(〇15M)中, 接著分次添加硼氫化鈉(1.5當量)。將反應混合物在室溫下 攪拌8 j、時。然後,於真空中移除揮發性物質,且使所形成 之殘留物於Et〇Ac與1NNa0H水溶液之間作分液處理。分離 水層,並以EtOAc逆萃取。將合併之有機萃液以水與鹽水進 一步洗滌,以Na2S〇4脫水乾燥,及過濾。濾液在真空中之 /辰縮,獲得標題化合物,為無色油。 胺32 [(環丙胺基)甲基]_2_萘基}乙基)乙醯胺 步驟1 ·· 3-0[(甲磺醯基)氧基]乙基丨小茶羧酸甲酯 143482-1 -105- 201111364 在0°C下,於得自胺31步驟2之3-(2-羥乙基)-1-蕃羧酸曱酯 (1當量)與Hunig氏鹼(1.5當量)之二氣曱烷(0 〇3M)溶液中,添 加氯化曱烷磺醯(1.3當量)^將所形成之溶液於下攪拌3〇 分鐘,然後在室溫下15分鐘。接著’以1〇% Ηα水溶液使反 應混合物淬滅。分離含水洗液,並以醚逆萃取。將合併之 有機萃液以水與鹽水進一步洗滌,以Na2 s〇4脫水乾燥,及 過濾。濾液在真空中之濃縮,獲得粗製標題化合物,為無 色油。 步驟2: 3-(2-疊氮基乙基H-莕羧酸酯 鲁 於得自前一步驟之3-{2-[(甲磺醯基)氧基]乙基}小莕羧酸 甲酯(1當量)之DMFC0.25M)溶液中,添加疊氮化鈉(5當量)。 將所形成之溶液在55。(:下攪拌12小時,然後於80t下另外3 小時。接著,將反應混合物以趟稀釋,並以水洗滌。分離 水層,且以醚逆萃取。將合併之有機萃液以水與鹽水進一 步洗滌,以N^SO4脫水乾燥,過濾,及使濾液在真空中濃 縮,而得粗製標題化合物,為粉紅色油。 步驟3 : 3-(2-胺基乙基)-1-茶羧酸甲醋 % 於得自前一步驟之3-(2-疊氮基乙基H_莕羧酸自旨(1當量) 與三苯膦(1.2當量)之THF(0.1M)溶液中,添加水(3當量j。將 所形成之溶液在50°C下攪拌5小時。然後,於真空中移除揮 發性物質,且如此獲得之粗產物經由急驟式層析之純化 (Si〇2 ’ 96:4 (v/v) (¾¾ :在 MeOH 中之 2·〇Μ NH3),獲得標題 化合物,為無色油。 步驟4,3-[2-(乙醯胺基)乙基]-茶叛酸曱西旨 143482-1 -106- 201111364 於得自前一步驟之3-(2-胺基乙基)-1-蕃緩酸曱醋(1當量)、 Hunig氏鹼(3當量)及醋酸(1.1當量)之DMF (0.2M)溶液中,分 次添加六氟磷酸0-(7-氮苯并三唑_ι_基)_N,N,N,,N,·四曱基錁 (1.1當量)。將所形成之反應溶液在室溫下攪拌48小時。將 目前帶紅色溶液以醚稀釋,並以IN NaOH水溶液、水及鹽水 相繼洗滌。然後,使有機萃液以N^SO4脫水乾燥,過渡, 及使濾液在真空中濃縮’而得淡黃色油。如此獲得之粗產 • 物經由急驟式層析之純化(Si〇2,7:3 (Wv)己烧:Et〇Ac~&gt; EtOAc —95:5 (v/v) CH2C12 :在 MeOH 中之 2.0M NH3),獲得標題化合 物,為無色油。 步驟5 : N-{2-[4-(經曱基)-2-莕基]乙基}乙醯胺 使得自前一步驟之3-[2-(乙醯胺基)乙基莕羧酸曱酯(1當 量)溶於THF(0_18M)中。然後,於此溶液中,添加硼氫化鋰 (12當量),並將所形成之溶液在5〇t:下激烈攪拌5小時。將 如此獲得之反應混合物以醚進一步稀釋,且以1N 水溶 φ 液小心地使反應淬滅。分離水層,並以EtOAc逆萃取。將合 併之有機萃液以IN NaOH水溶液、水及鹽水進一步洗滌,以 NazSO#脫水乾.燥,及過濾。濾液在真空中之濃縮,獲得標 題化合物,為白色固體。 步驟6 : N-[2-(4-曱醯基_2_萘基)乙基]乙醯胺 在〇C下,於得自前一步驟之Ν·{2-[4-(羥曱基)_2_萘基]乙基} 乙醯胺(1虽量)與碳酸氫鈉(1.2當量)在二氯甲烷(0.09Μ)中 之懸浮液内,添加DMPai當量)。將所形成之混合物於室 溫下㈣18小時’㈣以飽和NaHSC&gt;3水溶液使反應泮滅, 143482-1 •107· 201111364 接著以EhO萃取。將合併之有機萃液以10% HC1水溶液、水 及鹽水進一步洗滌’以Na2S04脫水乾燥,過濾,及使濾液 在真空中濃縮。如此獲得之粗產物經由急驟式層析之純化 (Si02,19:1 (v/v)己烷:EtOAc— 1:1 (v/v)己烷:EtOAc),獲得標 題化合物,為無色油。 步驟6 :胺32 於得自前一步驟之N-[2-(4-曱醯基-2-莕基)-乙基]乙醯胺(1 當量)之二氯曱烷(0.12M)溶液中,添加硫酸鎂(丨當量)與環 丙基胺(2當量)。將所形成之懸浮液在室溫下攪拌48小時。 經由過濾移除不溶物,並以二氣甲烷沖洗,然後使合併之 渡液在真空中濃縮。使如此獲得之粗製亞胺溶於曱醇 (0.12M)中,接著分次添加棚氫化鈉(丨5當量)。將反應混合 物在室溫下攪拌3小時。然後,於真空中移除揮發性物質, 且使所形成之殘留物於EtOAc與IN NaOH水溶液之間作分液 處理。分離水層,並以Et0Ac逆萃取。將合併之有機萃液以 水與鹽水進一步洗滌,以N^SO4脫水乾燥,及過濾。濾液 在真空中之濃細’獲得標題化合物,為無色油。 胺33 N-[(2-溴苯基)曱基]環丙胺 於2-溴基芊醇(1當量)之THF溶液(〇 15M)中,添加三乙胺 (1.6當量)。使反應混合物冷卻至〇它,然後逐滴添加氣化曱 烷磺醯(1.3當量)。接著,使所形成之溶液慢慢地溫熱至室 溫。於1.5小時後’將環丙基胺(5當量)添加至目前混濁懸浮 液中。於另外18小時後’將反應混合物以驗稀釋,並以爪 143482-1 -108- 201111364The 3-(2-(decyloxy)ethyl] tea carboxylic acid oxime ester (1) was dissolved in toluene (0.1 M) from the previous step. Then, in this solution, DIBA1_H 〇 5M toluene solution (2.4 eq.) was added and the resulting solution was vigorously stirred at room temperature for 4 hours. The reaction mixture thus obtained was quenched with an aqueous solution of 1 Η Ηα, and extracted by shouting. The combined organic extracts were further washed with water and brine, dried &lt;RTI ID=0.0&gt; The filtrate was in a vacuum to give the title compound as a colorless oil. Step 5: 3·[2-(Methoxy)ethyl]-1-indolecarboxyfurfural 143482-1 201111364 At 〇°C, in the previous step {3_[2·(methoxy)B DMP (1.1 eq.) was added to a suspension of decyl alcohol (1 eq.) with sodium bicarbonate (1.1 eq.) in dichloromethane (1M). The resulting mixture was stirred at room temperature for 2 hours, then quenched with saturated aqueous NaH.sub.3 solution. The combined organic extracts were further washed with aq. EtOAc EtOAc EtOAc. The crude product thus obtained was purified by flash chromatography (Si2, 19:1 (v/v) hexane: EtOAc (EtOAc/EtOAc) It is a colorless oil. Step 6: Amine 31 is added to a solution of 3-[2-(methoxy)ethyl]indolecarboxaldehyde (1 eq.) in one of the previous steps in methane (0.15 M). Propylamine (1.2 when placed). The resulting suspension was stirred at room temperature for 2 hours. The insoluble material was removed by filtration and washed with dichloromethane. then the combined filtrate was concentrated in vacuo. The crude imine thus obtained was dissolved in methanol (〇15M), followed by sodium borohydride (1.5 eq.). The reaction mixture was stirred at room temperature for 8 j. Then, the volatile matter was removed in a vacuum, and the resulting residue was subjected to liquid separation between Et?Ac and 1NN a0H aqueous solution. The aqueous layer was separated and extracted with EtOAc. The combined organic extracts were further washed with water and brine, dried over Na 2 EtOAc, and filtered. The filtrate was reduced in vacuo to give the title compound as a colourless oil. Amine 32 [(cyclopropylamino)methyl]_2-naphthyl}ethyl)acetamidine Step 1 ··3-0[(Methanesulfonyl)oxy]ethylhydrazine tea carboxylic acid methyl ester 143482- 1-105-201111364 2-(2-hydroxyethyl)-1-carboxylic acid carboxylic acid ester (1 equivalent) and Hunig's base (1.5 equivalents) obtained from step 2 of amine 31 at 0 °C To the gas decane (0 〇 3 M) solution, decanesulfonium chloride (1.3 eq.) was added. The resulting solution was stirred under reflux for 3 Torr and then at room temperature for 15 minutes. The reaction mixture was then quenched with a 1% aqueous solution of Ηα. The aqueous wash was separated and back extracted with ether. The combined organic extracts were further washed with water and brine, dried over Na 2 s 4 and filtered. The filtrate was concentrated in vacuo to give the crude title compound. Step 2: 3-(2-azidoethyl H-indolecarboxylate) is obtained from methyl 3-{2-[(methylsulfonyl)oxy]ethyl} hydrazide carboxylate from the previous step (1 equivalent) of DMFC 0.25 M) solution was added sodium azide (5 equivalents). The resulting solution was at 55. (: stirring for 12 hours, then at 80t for an additional 3 hours. Next, the reaction mixture is diluted with hydrazine and washed with water. The aqueous layer is separated and stripped with ether. The combined organic extracts are further water and brine. The mixture was washed with EtOAc (EtOAc m. Vinegar % is added to a solution of 3-(2-azidoethyl H-indolecarboxylic acid) from the previous step (1 eq.) and triphenylphosphine (1.2 eq.) in THF (0.1 M). Equivalent j. The resulting solution was stirred at 50 ° C for 5 hours. Then, the volatile material was removed in vacuo, and the crude product thus obtained was purified by flash chromatography (Si 〇 2 ' 96:4 ( v/v) (3⁄43⁄4: 2·〇Μ NH3 in MeOH), the title compound is obtained as colorless oil. Step 4, 3-[2-(ethylamino)ethyl]-tea 143482-1 -106- 201111364 3-(2-Aminoethyl)-1-baramic acid vinegar (1 eq.), Hunig's base (3 eq.) and acetic acid (1.1 eq.) from the previous step DMF (0.2M In the solution, 0-(7-azabenzotriazole_ι_yl)_N,N,N,,N,·tetradecylphosphonium hexafluorophosphate (1.1 equivalent) was added in portions. The resulting reaction solution was added. Stir at room temperature for 48 hours. Dilute the current reddish solution with ether and wash successively with 1 N aqueous NaOH solution, water and brine. Then, the organic extract is dehydrated and dried with N^SO4, and the filtrate is placed in vacuo. Concentrated to give a pale yellow oil. The crude material thus obtained was purified by flash chromatography (Si 〇 2, 7:3 (Wv) hexane: Et 〇Ac~&gt; EtOAc - 95:5 (v/ v) CH2C12: 2.0M NH3 in MeOH afforded the title compound as colourless oil. Step 5: N-{2-[4-(sulfenyl)-2-mercapto]ethyl}ethylamine 3-[2-(ethylamino)ethyl hydrazide carboxylic acid oxime ester (1 eq.) was dissolved in THF (0-18 M) from the previous step. Then, lithium borohydride (12 eq.) was added to this solution. The resulting solution was stirred vigorously for 5 hours at 5 Torr: The reaction mixture thus obtained was further diluted with ether and the reaction was quenched carefully with 1N aqueous EtOAc. The combined organic extracts were washed with EtOAc EtOAc EtOAc EtOAc. -(4-indolyl-2-yl-naphthyl)ethyl]acetamidine at 〇C, from the previous step {·{2-[4-(hydroxyindenyl)_2-naphthyl]ethyl } Ethylamine (1) is added to a suspension of sodium bicarbonate (1.2 equivalents) in dichloromethane (0.09 Torr) with DMPai equivalent). The resulting mixture was quenched at room temperature (IV) for 18 hours (4) with saturated aqueous NaHSC &gt; 3, 143482-1 • 107·201111364 followed by extraction with EhO. The combined organic extracts were further washed with aq. 10% aqueous HCI, water and brine. The crude product thus obtained was purified by flash chromatography (EtOAc, EtOAc (EtOAc) Step 6: Amine 32 in a solution of N-[2-(4-mercapto-2-indolyl)-ethyl]acetamide (1 eq.) in dichloromethane (0.12M) from the previous step Add magnesium sulfate (丨 equivalent) and cyclopropylamine (2 equivalents). The resulting suspension was stirred at room temperature for 48 hours. The insolubles were removed via filtration and rinsed with di-methane, then the combined mixture was concentrated in vacuo. The crude imine thus obtained was dissolved in decyl alcohol (0.12 M), followed by sodium hydride (5 eq.). The reaction mixture was stirred at room temperature for 3 hours. The volatiles were then removed in vacuo and the residue formed was partitioned between EtOAc and aqueous EtOAc. The aqueous layer was separated and back-extracted with Et0Ac. The combined organic extracts were further washed with water and brine, dried over N?SO?, and filtered. The title compound was obtained as a colorless oil. Amine 33 N-[(2-Bromophenyl)indolyl]cyclopropylamine To a solution of 2-bromodecyl alcohol (1 eq. The reaction mixture was allowed to cool to dryness, and then vaporized decanesulfonium (1.3 eq.) was added dropwise. Next, the formed solution was slowly warmed to room temperature. Cyclopropylamine (5 equivalents) was added to the current turbid suspension after 1.5 hours. After another 18 hours, the reaction mixture was diluted and tested with claws 143482-1 -108- 201111364

NaOH水溶液使反應淬滅。分離有機萃液,以鹽水洗滌’以 Na2 SO#脫水乾燥,過遽’及使遽液在真空中濃縮。如此獲 得之粗產物經由急驟式層析之純化(Si〇2,4:ι (v/v)己烷: EtOAc— 1:4 (Wv)己烷:EtOAc),獲得標題化合物,為淡黃色 油。 胺34 N-{ [1-(2-曱氧基乙基)_1H_啕哚各基]甲基}環丙胺 步驟1 : 1-(2-甲氧基乙基引哚_3_羧甲醛 使令朵-3-羧甲醛(1當量)溶於dmf (0.46M)中。添加氫化鈉 (1.3當量)’並將所形成之溶液在室溫下攪拌20分鐘。然後, 添加碘化鉀(1當量)與μ溴基冬甲氧基乙烷(2當量),且將反 應洛液於室溫下攪拌48小時。接著,以鹽水使反應混合物 淬滅,並以EtOAc萃取。使合併之有機萃液以MgS〇4脫水乾 燥。過濾、’及濾液在真空中之濃縮,獲得黃色油。如此獲 得之粗產物經由急驟式層析之純化(Si02,9··1 (v/v)己烷: EtOAc^ EtOAc),獲得標題化合物,為橘色油。 步驟2 :胺34 使得自前一步驟之H2-曱氧基乙基哚-3-羧曱醛(1 當量)與環丙基胺(2當量)溶於CH2Cl2(〇15M)中。然後,添加 硫馱鎂(1當夏)與甲酸(〇1當量),並將所形成之懸浮液在室 /m下攪拌8小時。經由過濾移除不溶物,及使濾液在真空中 /辰縮。接著,使殘留物溶於MeOH (0.15M)中,且分次添加硼 氫化鈉(1.5當$ )。將所形成之懸浮液在室溫下攪拌16小時。 :真工中移除揮發性物質。然後,使所形成之殘留物溶於 143482· 1 -109- 201111364 醚中,以1NHC1水溶液小心地使反應淬滅’接著以ινν&amp;〇η 水溶液中和。分離含水洗液,並以醚逆萃取。將合併之有 機萃液以水與鹽水進一步洗滌,以NhSO4脫水乾燥,過濾, 及使濾液在真空中濃縮。如此獲得之粗產物經由急驟式層 析之純化(Si〇2,EtOAc- 7:3 (Wv) EtOAc : MeOH),獲得標題化 合物,為橘色油。 胺35 Ν-{[1-(2,2,2-三氟乙基)-lH-吲哚-3-基]曱基}環丙胺 胺35係根據胺34中所述之程序製成,但在步驟,替 代地使用1-碘基-2,2,2-三氟乙烷作為烷基化作用試劑。 胺36 Ν-{[1-(4,4,4-三氣丁基)-1Η-叫丨哚-3-基]曱基丨環丙胺 胺36係根據胺34中所述之程序製成,但在步驟1中,替 代地使用1-碘基-4,4,4-三氟丁烷作為烷基化作用試劑。 胺37 N-[(l-丁基-1H-4嗓-3-基)曱基]環丙胺 胺37係根據胺34中所述之程序製成,但在步驟i中,替 代地使用1-碘基丁烷作為烷基化作用試劑。 胺38 Ν-({1-[3-(乙氧基)丙基HH-吲哚-3-基}甲基)環丙胺 胺38係根據胺34中所述之程序製成,但在步驟1中,替 代地使用1-溴基-3-乙氧基丙烷作為烷基化作用試劑。 胺39 N-({ 1-[3,3,3-二氟-2-(二氟曱基)丙基]_1H吲哚_3基丨甲基)環丙胺 143482-1 -】】0· 201111364 胺39係根據胺34中所述之程序製成,但在步驟1中,替 代地使用1,1,1,3,3,3-六氟-2-(碘基甲基)丙烷作為烷基化作用 試劑。 N-(3-{3-[(環丙胺基)曱基]_m•吲哚丨基}丙基)乙醯胺 步驟1 : [3-(3-甲醯基-1Η-叫哚小基)丙基]胺基甲酸第三汀酯 使?卜木-3-羧甲醛(1當量)溶於DMF (〇 15M)中。添加氫化鈉 φ (1.3當置)’並將所形成之溶液在室溫下攪拌20分鐘❶然後’ 添加碘化四丁基銨(1當量)與3_溴基丙基胺基曱酸第三丁 酯(2當量),且將反應溶液於室溫下攪拌18小時。接著,以 飽和Nt^ci水溶液使反應混合物淬滅,並以Et〇Ac萃取。使 合併之有機萃液以MgS A脫水乾燥。過濾’及濾液在真空中 之濃縮’獲得黃色油。如此獲得之粗產物經由急驟式層析 之純化(Si02 ’ 7:3 (v/v)己院:EtOAc— EtOAc),獲得標題化合 物,為淡粉紅色固體。 • 步驟2: N-[3_(3-甲醢基-m-吲哚-1-基)丙基]乙醯胺 於得自前一步驟之[3_(3_曱醯基·m_吲哚小基)丙基]胺基甲 酸第三-丁酯之經攪拌二氣甲烷(〇〇9M)溶液中,添加(在 二氧陸園令之4N溶液,45當量)。將所形成之溶液在室溫 下攪拌1小時,然後於真空十移除揮發性物質。接著,將二 氣甲院添加至紅色殘留物中,並再一次於真空中移除揮發 性物質,而得紅色膠質。然後’於如此獲得之粗製胺中, 添加二氣甲烧(0._與三乙胺(22當量)。#反應溶液變成 均勻時,添加氯化乙酿(1〇5當量),且將所形成之混合物於 143482-1 201111364 至/瓜下再攪拌2小時。最後,以IN NaOH水溶液使反應淬滅, 並以二氣甲院萃取。使合併之有機萃液以MgSC«水乾燥, 過濾,及濾液在真空中之濃縮,獲得粗製標題化合物,為 黃色固體》 步驟3 :胺40 使知自別步驟之N-[3-(3-曱醯基-1H-吲噪-1-基)丙基]乙酿 胺α當量)與環丙基胺(2當量)溶於CH2Cl2(〇1M)中。然後, 添加硫酸鎂(2當量)與甲酸(〇2當量),並將所形成之懸浮液 在室溫下攪拌20小時。經由過濾移除不溶物,及使濾液在 真空中濃縮。接著,使殘留物溶於MeOH (0.1M)中,並分次 添加硼氫化鈉(1當量)。將所形成之懸浮液在室溫下攪拌历 小時。於真空中移除揮發性物質。然後,使所形成之殘留 物/谷於驗中,以IN HC1水溶液小心地使反應淬滅,接著以 IN NaOH水溶液中和。分離含水洗液’且以醚逆萃取。將合 併之有機萃液以水與鹽水進一步洗滌,以Na2S〇4脫水乾燥, 過;慮及使/慮液在真空中濃縮。如此獲得之粗產物經由急 驟式層析之純化(Si02,1:9 (v/v) MeOH : EtOAc-&gt; 1:1 ΟΛΟ EtOAc :The reaction was quenched with aqueous NaOH. The organic extract was separated, washed with brine, dried over Na 2 SO. The crude product thus obtained was purified by flash chromatography (EtOAc: EtOAc:EtOAc:EtOAc . Amine 34 N-{ [1-(2-decyloxyethyl)_1H_indenyl]methyl}cyclopropylamine Step 1: 1-(2-methoxyethyl hydrazine _3_carboxaldehyde Benzyl-3-carboxaldehyde (1 eq.) was dissolved in dmf (0.46 M). Sodium hydride (1.3 eq.) was added and the resulting solution was stirred at room temperature for 20 min. Then, potassium iodide (1 eq.) was added. The reaction mixture was quenched with brine and extracted with EtOAc over EtOAc (EtOAc). The MgS〇4 was dehydrated and dried. Filtration, 'and the filtrate was concentrated in vacuo to give a yellow oil. The crude product thus obtained was purified by flash chromatography (Si02, 9·1 (v/v) hexane: EtOAc^ EtOAc) to give the title compound as an orange oil. Step 2: Amine 34 </ RTI> </ RTI> </ RTI> </ RTI> </ RTI> </ RTI> </ RTI> <RTIgt; In CH2Cl2 (〇15M). Then, strontium magnesium (1 in summer) and formic acid (〇1 equivalent) were added, and the resulting suspension was stirred at room/m for 8 hours. Insoluble matter was removed by filtration. And the filtrate was allowed to dry in vacuo. The residue was dissolved in MeOH (0.15M) and sodium borohydride (1.5%) was added portionwise. The resulting suspension was stirred at room temperature for 16 hours. : Remove volatiles from the work. Then, dissolve the residue in 143482·1 -109- 201111364 ether, carefully quench the reaction with 1NHC1 aqueous solution, and then neutralize with ινν &amp; The aqueous washings were separated and extracted with ether. The combined organic extracts were further washed with water and brine, dried over NaHSO4, filtered, and the filtrate was concentrated in vacuo. The crude product thus obtained was subjected to flash chromatography Purification (Si 2 , EtOAc - 7:3 (EtOAc):EtOAc) lH-Indol-3-yl]fluorenyl}cyclopropylamine 35 is prepared according to the procedure described in amine 34, but in the step, 1-iodo-2,2,2-trifluoroethane is used instead. As an alkylation reagent. Amine 36 Ν-{[1-(4,4,4-trimethylbutyl)-1Η-called 丨哚-3-yl]nonyl fluorenyl propylamine 36 is based on amine 34 Said program However, in step 1, 1-iodo-4,4,4-trifluorobutane is alternatively used as the alkylating agent. Amine 37 N-[(l-butyl-1H-4嗓-3) -Based] fluorenyl] Cyclopropylamine 37 is prepared according to the procedure described for amine 34, but in step i, 1-iodobutane is alternatively used as the alkylating agent. Amine 38 Ν-({ 1-[3-(Ethoxy)propylHH-indol-3-yl}methyl)cyclopropylamine 38 is prepared according to the procedure described for amine 34, but in step 1, alternatively 1 is used. -Bromo-3-ethoxypropane as an alkylating agent. Amine 39 N-({ 1-[3,3,3-difluoro-2-(difluoroindolyl)propyl]_1H吲哚_3yl fluorenylmethyl)cyclopropylamine 143482-1 -]]0· 201111364 Amine 39 is prepared according to the procedure described for amine 34, but in step 1, 1,1,1,3,3,3-hexafluoro-2-(iodomethyl)propane is optionally used as the alkyl group. Chemical reagent. N-(3-{3-[(cyclopropylamino)indolyl]-m•indolyl}propyl)acetamide Step 1: [3-(3-methylindolyl-1Η-哚哚小基) The propyl] carbamic acid tert-butyl ester was dissolved in DMF (〇15M). Add sodium hydride φ (1.3 when set) and stir the resulting solution at room temperature for 20 minutes, then add 'tetrabutylammonium iodide (1 equivalent) and 3 -bromopropylamino decanoic acid Butyl ester (2 equivalents), and the reaction solution was stirred at room temperature for 18 hours. Next, the reaction mixture was quenched with a saturated aqueous solution of EtOAc and extracted with EtOAc. The combined organic extracts were dehydrated and dried with MgS A. Filtration and concentration of the filtrate in vacuo afforded a yellow oil. The crude product thus obtained was purified by flash chromatography (EtOAc EtOAc (EtOAc) • Step 2: N-[3_(3-methylindolyl-m-indol-1-yl)propyl]acetamide is obtained from the previous step [3_(3_曱醯基·m_吲哚小小The propyl]amino]carbamic acid tert-butyl ester was added to a stirred two-gas methane (〇〇9M) solution (4N solution in dioxin, 45 equivalents). The resulting solution was stirred at room temperature for 1 hour and then the volatiles were removed under vacuum. Next, the second gas chamber was added to the red residue, and the volatile matter was again removed in a vacuum to obtain a red gum. Then, in the crude amine thus obtained, a second gas is added (0._ with triethylamine (22 equivalents). # When the reaction solution becomes homogeneous, chlorinated ethylene (1〇5 equivalent) is added, and The resulting mixture was stirred for an additional 2 hours at 143482-1 201111364 to / melon. Finally, the reaction was quenched with 1N aqueous NaOH solution and extracted with MeOH. The combined organic extracts were dried with &lt;RTIgt; And the filtrate is concentrated in vacuo to give the crude title compound as a yellow solid. Step 3: Amine 40 </ RTI> </ RTI> N-[3-(3-indolyl-1H- 吲 -1- -1- yl) The arylamine (equivalent) and cyclopropylamine (2 equivalents) were dissolved in CH2Cl2 (〇1M). Then, magnesium sulfate (2 equivalents) and formic acid (〇2 equivalent) were added, and the resulting suspension was stirred at room temperature for 20 hours. The insolubles were removed via filtration and the filtrate was concentrated in vacuo. The residue was dissolved in MeOH (0.1M) and sodium borohydride (1 eq.). The resulting suspension was stirred at room temperature for a period of time. Remove volatiles in a vacuum. Then, the formed residue/valley was subjected to an examination, and the reaction was carefully quenched with an aqueous solution of IN HCl, followed by neutralization with an aqueous solution of IN NaOH. The aqueous wash solution was separated and back extracted with ether. The combined organic extracts were further washed with water and brine, dried over Na 2 S 〇 4, and allowed to concentrate in vacuo. The crude product thus obtained was purified by flash chromatography (SiO2, 1:9 (v/v) MeOH: EtOAc-&gt; 1:1 EtOAc:

MeOH) ’獲得標題化合物,為白色固體。 胺41 N-(3-{3-[(環丙胺基)曱基]_出_吲哚丨基丨丙基)丙醯胺 胺41係根據胺40中所述之程序製成,但在步驟2中,替 代地使用氯化丙醯作為烷基化作用試劑。 胺42 N-(2-{3-[(環丙胺基)曱基]_1H-吲哚4_基}乙基)乙醯胺 143482-1 201111364 胺42係根據胺40中所述之裎戽 4心杜序製成,但在步驟1中,替 代地使用2-溴基乙基胺基甲醅坌— T ®文第二-丁酯作為烷基化作用試 劑。 胺43 叫{3_[(環丙胺基)甲基HH♦朵+基}乙基)丙酿胺 胺42係根據胺4G中所述之程序製成,但在步驟η,替 代地使用2-漠基乙基胺基曱酸第三_丁醋作為烧基化作用試The title compound was obtained as a white solid. Amine 41 N-(3-{3-[(cyclopropylamino)indolyl]-exidine-mercaptopropyl)propanamide 41 is prepared according to the procedure described in amine 40, but in the step In 2, propionyl chloride is used instead as an alkylating agent. Amine 42 N-(2-{3-[(cyclopropylamino)indolyl]_1H-吲哚4_yl}ethyl)ethylamine 143482-1 201111364 Amine 42 is based on the oxime 4 described in the amine 40 The core is prepared, but in step 1, 2-bromoethylaminocarbamidine-T® second-butyl ester is alternatively used as the alkylation reagent. The amine 43 is called {3_[(cyclopropylamino)methylHH♦dol +yl}ethyl)propanolamine 42 is prepared according to the procedure described in the amine 4G, but in step η, instead of 2-di Triethyl butyl citrate as the alkylation test

知及在步驟2中’使用氣化丙酿作為院基化作用試劑。 胺44 Ν-{[1-(2·丙烯小基)-ΐΗ_吲哚_3_基]甲基}環丙胺 步驟1 : 1-稀丙基-1Η-叫卜果-3-緩甲駿 使叫丨^各叛甲酸α當量)溶於DMF (ο··)中。添加氫化納 (2.5當直)’並將所形成之溶液在室溫下攪拌%分鐘。然後, 添加3-溴丙烯(1當量),且將反應溶液於室溫下攪拌2〇小時。 接著以鹽水使反應混合物淬滅,並以Et〇Ac萃取。使合併之 • 有機萃液以MSS〇4脫水乾燥。過濾,及濾液在真空中之濃縮, 獲得育色油。如此獲得之粗產物經由急驟式層析之純化 (Si02,4:1 (v/v)己烷:EtOAc— 3..7 (v/v)己烷·· Et0Ac),獲得標 題化合物,為淡黃色油。 步驟2:胺44 使得自前一步驟之1_烯丙基-1H-吲嗓_3_羧甲醛(丨當量)與 環丙基胺(2當量)溶於MeOH (0.05M)中。然後,添加氰基侧 氫化鈉(2當量)與醋酸(4當量),並將所形成之懸浮液在室 溫下攪拌18小時。接著,於真空中移除揮發性物質。辦 143482^1 -113- 201111364 使所形成之殘留物溶於謎中,以IN NaOH水溶液小心地使反 應淬滅。分離含水洗液,且以醚逆萃取。將合併之有機萃 液以水與鹽水進一步洗滌,以Na2S04脫水乾燥,過濾,及 使濾液在真空中濃縮。如此獲得之粗產物經由急驟式層析 之純化(Si02,EtOAc— 4:1 (v/v) EtOAc : MeOH),獲得標題化合 物’為黃色油。 胺45 Ν-{[1-(苯基甲基)-1H-吲哚-3-基]曱基}環丙胺 胺45係根據胺44中所述之程序製成’但在步驟1中,替 代地使用溴化芊作為烷基化作用試劑。 胺46 队{[1-(2-峨啶基曱基HH_吲哚各基]曱基}環丙胺 胺46係根據胺44中所述之程序製成,但在步驟i中,替 代地使用碘化四丁基銨(1當量)與氯化2_甲基吡啶鹽酸鹽 (1.5當量)作為烷基化作用混合物。 胺47 N-{[1-(3-吡啶基甲基ΗΗ·吲哚_3_基]甲基}環丙胺 胺47係根據胺44中所述之程序製成,但在步驟κ,替 代地使用碘化四丁基銨(1當量)鱼 里J -、氣化3-甲基峨咬鹽酸鹽 (1.5當量)作為烷基化作用混合物。 孤 胺48 N-UH4金定I甲基HH♦呆_3_基]甲基}環丙胺 胺48係根據胺辦所述之程序^, 代地使用演™咬氣漠酸鹽(1當量)作為:基二: 143482-1 -114. 201111364 試劑。 胺49 Ν-({1-[(4-氟苯基)曱基]-1Η-吲哚-3-基}曱基)環丙月安 胺49係根據胺44中所述之程序製成,但在步驟,替 代地使用1-(溴基甲基)-4-氟基苯(1.5當量)作為燒基化作用試 劑。 胺50 Ν-({1-[(4-氯苯基)甲基]-lH-吲哚-3-基}曱基)環丙月安 胺50係根據胺44中所述之程序製成,但在步驟i中,替 代地使用1-(溴基曱基)-4-氣苯(1.5當量)作為烷基化作用試 劑。 胺51 Ν-({1-[(3-氟苯基)甲基]-1H-啕哚-3-基}曱基)環丙月安 胺51係根據胺44中所述之程序製成,但在步称1中,替 代地使用1-(溴基曱基)-3-氟基苯(1·5當量)作為烷基化作用試 劑。 胺52 Ν-({1-[(3-氣苯基)曱基]_1Η-啕哚-3-基}曱基)環丙胺 胺52係根據胺44中所述之程序製成’但在步称1中,替 代地使用1-(溴基曱基)_3_氣苯(1.5當量)作為烷基化作用試 劑。 胺53 3-({3-[(環丙胺基)曱基哚小基}甲基)笨曱腈胺53係根 據胺44中所述之程序製成,但在步驟1中,替代地使用1-消 143482-1 • 115· 201111364 基甲基)-3-氰基苯(ι·5當量)作為烷基化作用試劑。 胺54 Ν-({ Η(3-甲基苯基)甲基]_1Η_啕哚各基丨甲基)環丙胺 胺54係根據胺44中所述之程序製成,但在步驟ι中替 代地使用Η漠基甲基)-3_甲苯(L5當量)作為燒基化作用試 劑。 胺55 N-({5-氟基-1-[3-(曱氧基)丙基;|-1H_啕哚_3基}曱基)環丙胺 胺SS係根據胺44中所述之程序製成,但在步驟,替籲 代地使用埃化四丁基録(1當量)_臭基_3曱氧基丙烧(21 當量)作為烷基化作用混合物,及5_氟基_m吲哚_3羧甲醛(ι 當量)作為起始p?丨嗓。 N-{ [6-漠基-1-(苯基甲基)·1Η_吲哚;基]曱基}環丙胺 步驟1 : 6-演基-1Η-Μ丨11朵-3-缓甲酸·It is known that in step 2, gasification is used as a hospitalization reagent. Amine 44 Ν-{[1-(2· propylene small group)-ΐΗ_吲哚_3_yl]methyl}cyclopropylamine Step 1: 1-Dilyl-1Η-called 卜果-3-慢甲Let 丨^ each of the formic acid α equivalent) dissolved in DMF (ο··). Sodium hydride (2.5 as straight) was added and the resulting solution was stirred at room temperature for a minute. Then, 3-bromopropene (1 equivalent) was added, and the reaction solution was stirred at room temperature for 2 hours. The reaction mixture was then quenched with brine and extracted with EtOAc. The combined organic extracts were dehydrated and dried with MSS®4. Filtration and concentration of the filtrate in vacuo afforded a coloured oil. The crude product thus obtained was purified by flash chromatography (EtOAc, EtOAc: EtOAc (EtOAc) Yellow oil. Step 2: Amine 44 was dissolved in MeOH (0.05 M) from the previous step of 1- allyl-1H-indole-3-carbaldehyde (e.e. equivalent) and cyclopropylamine (2 eq.). Then, sodium cyanoside (2 equivalents) and acetic acid (4 equivalents) were added, and the resulting suspension was stirred at room temperature for 18 hours. Next, the volatiles are removed in a vacuum. Office 143482^1 -113- 201111364 The residue formed was dissolved in the mystery and the reaction was carefully quenched with aqueous 1N NaOH. The aqueous wash was separated and back extracted with ether. The combined organic extracts were further washed with water and brine, dried over Na 2 EtOAc, filtered and evaporated. The crude product thus obtained was purified by flash chromatography eluting elut elut elut elut elut Amine 45 Ν-{[1-(phenylmethyl)-1H-indol-3-yl]indolyl}cyclopropylamine 45 is made according to the procedure described in amine 44, but in step 1, instead Barium bromide is used as an alkylation reagent. Amine 46 Team {[1-(2-Acridinesulfinyl)HH_indolyl]hydrazino}cyclopropylamine 46 was prepared according to the procedure described for amine 44, but in step i, alternatively used Tetrabutylammonium iodide (1 equivalent) and 2-methylpyridine hydrochloride (1.5 equivalents) were used as the alkylation mixture. Amine 47 N-{[1-(3-pyridylmethylΗΗ·吲)哚_3_yl]methyl}cyclopropylamine 47 is prepared according to the procedure described in amine 44, but in step κ, instead using tetrabutylammonium iodide (1 equivalent), J-, gasification 3-methyl hydrazine hydrochloride (1.5 eq.) as a mixture of alkylation. Cycloamine 48 N-UH4 jinding I methyl HH ♦ _3_ yl] methyl} cyclopropylamine 48 based on amine The procedure described above is used as a substitute for the bite gas salt (1 equivalent) as: base 2: 143482-1 -114. 201111364 reagent. amine 49 Ν-({1-[(4-fluorophenyl)) Indolyl]-1Η-indolyl-3-yl}hydrazino)cyclopropaminan 49 is prepared according to the procedure described in amine 44, but in the step, instead of 1-(bromomethyl)- 4-fluorobenzene (1.5 equivalents) as an alkylating agent. Amine 50 Ν-({1-[(4-chlorophenyl)methyl]-lH-indol-3-yl}曱Cyclopropaminan 50 is prepared according to the procedure described for amine 44, but in step i, 1-(bromomercapto)-4- benzene (1.5 equivalents) is alternatively used as the alkylation. Reagents: Amine 51 Ν-({1-[(3-fluorophenyl)methyl]-1H-indol-3-yl} yl)cyclopropaminan 51 is prepared according to the procedure described for amine 44 However, in the step 1, 1-(bromodecyl)-3-fluorobenzene (1.5 equivalents) was used instead as the alkylation reagent. Amine 52 Ν-({1-[(3) -Phenylphenyl)indenyl]_1Η-indol-3-yl}indenyl)cyclopropylamine 52 is prepared according to the procedure described in amine 44, but in step 1, alternatively 1-(bromo)曱3) Benzene (1.5 eq.) as an alkylation reagent. Amine 53 3-({3-[(cyclopropylamino)indolyl hydrazide} methyl) cumin nitrileamine 53 based on amine Prepared by the procedure described in 44, but in step 1, instead of 1-? 143482-1 • 115· 201111364 methyl)-3-cyanobenzene (1·5 equivalent) as the alkylation reagent Amine 54 Ν-({ Η(3-methylphenyl)methyl]_1 Η 啕哚 啕哚 丨 丨 methyl) Cyclopropylamine 54 is based on the procedure described in amine 44 , But using Η desert-ylmethyl alternative in the step ι) -3_ toluene (L5 eq) of the base functions as a burning reagent. Amine 55 N-({5-fluoro-1-[3-(indolyl)propyl;|-1H_啕哚_3yl}decyl)cyclopropylamine SS based on the procedure described for amine 44 Manufactured, but in the step, using tetrabutylene (1 equivalent) _ odoryl _3 methoxy propylene (21 equivalents) as the alkylation mixture, and 5-fluoro group _m吲哚_3 Carboxaldehyde (ι equivalent) was used as the starting p?丨嗓. N-{[6-Molyl-1-(phenylmethyl)·1Η_吲哚; yl] fluorenyl} cyclopropylamine Step 1: 6-Alkyl-1Η-Μ丨11-3-hydroxycarboxylic acid·

在〇°C下’於6-溴基-1Η-♦朵(1當量)之DMF (〇顿)溶液中, 添加氣化磷醯(1.2當量)。使所形成之溶液溫熱至室溫,並 在室溫下攪拌16小時。使所形成之溶液再冷卻至〇&lt;t,然後 小心地添加Na〇H(2M水溶液,2.8當量)。於室溫下再攪拌2 小時後,將粗製反應混合物以水稀釋,且以Et〇Ac萃取。使 合併之有機萃液以MgS〇4脫水乾燥。過濾,及濾液在真空中 之濃縮,獲得黃色油。如此獲得之粗產物經由急驟式層析 之純化(Si〇2,己烷—Et0Ac),獲得標題化合物,為褐色固Gasified phosphonium (1.2 equivalents) was added to a solution of 6-bromo-1 Η-♦ (1 equivalent) in DMF at 〇 °C. The resulting solution was allowed to warm to room temperature and stirred at room temperature for 16 hours. The resulting solution was re-cooled to 〇 &lt;t, then Na 〇H (2M aqueous solution, 2.8 eq.) was carefully added. After stirring for an additional 2 hours at room temperature, the crude reaction mixture was diluted with water and extracted with EtOAc. The combined organic extracts were dried over anhydrous MgS 4 . Filtration and concentration of the filtrate in vacuo afforded a yellow oil. The crude product thus obtained was purified by flash chromatography (EtOAc, EtOAc-EtOAc)

143482-1 •116- 201111364 步驟2 : 1-芊基-6-溴基_ih,哚-3-羧曱醛 使得自前一步驟之6_溴基丨哚各羧甲醛(1當量)溶於 DMF (0.19Μ)中。添加氫化鈉(1 5當量),並將所形成之溶液 在室溫下檀拌20分鐘。然後,添加溴化苄(1當量),且將反 應溶液於室溫下攪拌24小時。接著,以水使反應混合物淬 滅’並以EtOAc萃取。使合併之有機萃液以MgS〇4脫水乾燥。 過濾,及濾液在真空中之濃縮,獲得黃色油。如此獲得之 籲 粗產物經由急驟式層析之純化(Si〇2,4:1 (Wv)己烷:EtOAc·^ 3:7 (v/v)己院:EtOAc),獲得標題化合物,為黃色固體。 步驟3 :胺56 使得自前一步驟之1_苄基_6_溴基_1H_^哚各羧甲醛(1當 量)與環丙基胺(2當量)溶於Me〇H (〇 〇5M)中,然後,添加氰 基硼氫化鈉(2當量)與醋酸(4當量),並將所形成之懸浮液 在室溫下攪拌16小時。接著,於真空中移除揮發性物質。 然後,使所形成之殘留物溶於醚中,以1NNa〇H水溶液小心 φ 地使反應淬滅。分離含水洗液,且以醚逆萃取。將合併之 有機卒液以水與鹽水進一步洗滌,以Na2S〇4脫水乾燥,過 濾,及使濾液在真空中濃縮。如此獲得之粗產物經由急驟 式層析之純化(Si02,Et〇Ac~&gt; 2:3 (v/v) EtOAc : MeOH),獲得標 題化合物,為黃色油。 胺S7 n_UH(3-氟苯基)甲基]-6-(甲氧基)_1H•吲哚各基]甲基}環丙胺 胺57係根據胺44中所述之程序製成,但在步驟2中,替 代地使用1-(溴基曱基)-3-氟基苯(1.5當量)作為烷基化作用試 143482-1 201111364 劑,及在步驟1中,使用6_甲氧基_1H_吲哚_3綾甲醛(1當量) 作為起始丨嗓。 胺58 N-{[4-曱基小(苯基甲基)_1H_吲哚_3_基]曱基}環丙胺 胺58係根據胺56中所述之程序製成’但在步驟i中替 代地使用4-甲基-1料嗓(1當量)作為起始吲哚,及在步驟2 中,使用溴化卞(1當量)作為烷基化作用試劑。 胺59 3_[(環丙胺基:)甲基]-1-(苯基甲基卜朵4甲腈 籲 胺59係根據胺56中所述之程序製成,但在步驟ι中替 代地使用刪卜朵-4-甲腈(1當量)作為起始啊,及在步驟2 中,使用溴化芊(1當量)作為烷基化作用試劑。 胺60 N-U4-氟基-H苯基甲基)-1H_吲哚冬基]曱基}環丙胺 胺60係根據胺56中所述之鞋庠制士' 矛王序製成,但在步驟1中,替 代地使用4·氣基善《(1當量)作為起始㈣,及在步驟2 中,使用演化爷(1.5當量)作為炫基化作用試劑。 · 胺61 N.敗基-Η(3·氟苯基)甲基HH_啊_3基}甲基)環丙胺 胺6:L係根據胺56中所述之程序製成,但在步^中替 代地使用4-氟基-1H-»?丨哚(1當量)作主 I)作為起始十朵,及在步郭2 中’使用1-(溴基曱基)-3-氟基笨(15去旦 田里)作為烷基化作用試 劑。 胺62 143482-1 •118- 201111364 N-({4-氟基-i_[3_(曱氧基)丙基]_1H_吲哚各基}甲基淹丙胺 胺62係根據胺56中所述之程序製成,但在步驟,替 代地使用4-氟基-1Ηβ丨哚(1當量)作為起始吲哚。再者,^臭 基-3-甲氧基丙烧(2當量)與埃化四丁基敍(1當量)係在步帮 2中作為烷基化作用混合物使用。 胺63 ΜΗ-氯基-H3-(甲氧基)丙基ΗΗ·4哚彳基丨甲基)環丙胺 胺63係根據胺56巾所述之料製成,但在 代地使用4-氯基_1Η♦朵(1當量)作為起始令朵。再者,㈣ 基-3-甲氧基丙院(2當量)與蛾化四丁基_當量)係在步驟 2中作為烷基化作用混合物使用。 胺64 Ν-([4-氯基小(苯基甲基)_1Η_啊_3基]甲基腌丙胺 胺64係根據胺56中所述之程序製成,但在步則中,替 代地使用4-氣基,♦朵(1當量)作為起始♦朵,及在步驟2 中’使用漠化辛(1.5當量)作為貌基化作用 胺65 叫漠基小(苯基甲基)_1Η♦朵烟甲基}環丙胺 /Μ係根據胺%中所述之程序製成’但在步則中,替 代地使用4-溴基-1Η-卩引卩朵(1春旦从 |木(1田里)作為起始β哚,及在步驟2 中,使用溴化芊(1.5當量)作Α 里)作為烷基化作用試劑。 胺66 Ν-[(4-漠基-H(3_a笨基)甲基 胺⑽根二;基甲基你丙胺 序4成,但在步驟,替 201111364 始哨哚,及在步驟2 )作為燒基化作用試 代地使用4-溴基-1H蚓哚(1當量)作為起 中,使用ί-(溴基甲基)-3-敦基苯(15當量 劑0 胺67 Ν-({4-漠基小[3-(甲氧基)丙基]_1Η_吲哚 衣J暴}甲基)環丙胺 胺67係根據胺56中所述之程序製成,但在步驟η,替 代地使用4-漠基養♦朵(1當量)作為起始㈣。再者,卜漠 基-3-甲氧基丙烧(2當量)與蛾化四丁基則當量)係在步驟 2中作為烷基化作用混合物使用。 胺68 Ν-[(4-氟基-1Η-吲哚-3-基)甲基)環丙胺 胺68係根據胺56中所述之程序製成,但在步驟i中替 代地使用4-氟基-1H♦呆(1當量)作為起始♦朵。再者,步驟 2為非必要。 1-{H(環丙胺基)甲基]-5-[3-(甲氧基)丙基]苯基丨乙酮 胺69係根據已公告之專利申請案2⑽7/⑽925〇 中所 述之程序製成。 胺70 5-[(環丙胺基)甲基]-1,3-雙[3-(甲氧基)丙基]_2,4(1H,3H)_嘧啶二酮 步驟1 : 1,3-雙(3-甲氧基丙基)-2,4-二酮基-l,2,3,4-四氫嘧啶竣 甲醛 在〇°C下,於5-甲醯基尿嘧啶(1當量)之DMF (0.35M)溶液中 ,相繼地添加1-溴基-3-甲氧基丙烷(2.2當量)與DBU (2.2當 143482-1 -120- 201111364 量)。將所形成之溶液在室溫下攪拌72小時。然後,於真空 中移除揮發性物質。使如此獲得之粗產物混合物經由管柱 層析直接地接受純化(Sl〇2, Et0Ac),而得標題化合物,為 黃色油。 步驟2 :胺70 於得自前一步驟之1,3-雙(3-曱氧基丙基)_2,4•二酮基_u,3,4_ 四氫嘲啶-5-羧甲醛α當量)之二氣甲烷(01M)溶液中,添加 # 硫酸鎮(1當量)與環丙基胺(2當量)。將所形成之懸浮液在 室溫下攪拌16小時《經由過濾移除不溶物,並以二氣曱烷 沖洗,然後使合併之濾液在真空中濃縮β使如此獲得之粗 製亞胺溶於甲醇(0·1Μ)中,接著分次添加蝴氫化納(15當量) 。將反應混合物在室溫下攪拌16小時,然後以飽和NaHC〇3 水溶液使反應淬滅,接著以EtOAc萃取。將合併之有機萃液 以水與鹽水進一步洗滌,以NasSO4脫水乾燥,過濾,及使 遽液在真空中濃縮。如此獲得之粗產物經由管柱層析之純 參 化(si02,CH2C1 广 85:15 (v/v) CH2C12 :在 MeOH 中之 2M NH3), 獲得標題化合物,為白色固體。 胺71 N-[5-(3-甲氧基丙基)-2,3-二曱基苄基]環丙胺 步驟1 : 5-溴基-2,3-二甲基苯甲酸 於2,3-二甲基苯甲酸(1當量)之經攪拌醋酸溶液⑴2M)中, 相繼地添加硝酸(12當量)、水(25當量)及溴(U當量)。最後, 逐滴添加硝酸銀(1M水溶液’ 1.3當量),歷經30分鐘期間。 於至溫下再授拌一小時後,將粗製反應混合物以水稀釋, 143482-] • 121 - 201111364 並以EtOAc萃取。然後,將合併之有機萃液以鹽水洗滌,以143482-1 •116- 201111364 Step 2: 1-Mercapto-6-bromo _ih, hydrazine-3-carboxyfurfural so that the 6-bromo hydrazine carboxaldehyde (1 eq.) from the previous step is dissolved in DMF (0.19Μ). Sodium hydride (15 eq.) was added and the resulting solution was sanded at room temperature for 20 min. Then, benzyl bromide (1 equivalent) was added, and the reaction solution was stirred at room temperature for 24 hours. The reaction mixture was then quenched with water and extracted with EtOAc. The combined organic extracts were dried over MgSO4. Filtration and concentration of the filtrate in vacuo afforded a yellow oil. The crude product thus obtained was purified by flash chromatography (EtOAc: EtOAc: EtOAc (EtOAc) solid. Step 3: Amine 56 is obtained by dissolving 1 -benzyl-6-bromo-1H_^ each carboxaldehyde (1 equivalent) and cyclopropylamine (2 equivalents) in the previous step in Me〇H (〇〇5M). Then, sodium cyanoborohydride (2 eq.) and acetic acid (4 eq.) were added, and the resulting suspension was stirred at room temperature for 16 hr. Next, the volatiles are removed in a vacuum. Then, the resulting residue was dissolved in ether, and the reaction was quenched with a 1 N NaH aqueous solution. The aqueous wash was separated and back extracted with ether. The combined organic strokes were further washed with water and brine, dried over Na2SO4, filtered, and concentrated. The crude product thus obtained was purified by flash chromatography (EtOAc, EtOAc (EtOAc) Amine S7 n_UH(3-fluorophenyl)methyl]-6-(methoxy)_1H•indenyl]methyl}cyclopropylamine 57 is prepared according to the procedure described in amine 44, but in the step In 2, 1-(bromoindenyl)-3-fluorobenzene (1.5 equivalents) is used instead as the alkylation test 143482-1 201111364, and in step 1, 6_methoxy_1H is used. _吲哚_3绫formaldehyde (1 equivalent) as the starting point. Amine 58 N-{[4-indolyl small (phenylmethyl)_1H_吲哚_3_yl]indolyl}cyclopropylamine 58 is made according to the procedure described in amine 56, but in step i Alternatively, 4-methyl-1 hydrazine (1 equivalent) was used as the starting hydrazine, and in step 2, cesium bromide (1 equivalent) was used as the alkylating agent. The amine 59 3_[(cyclopropylamino:)methyl]-1-(phenylmethyl bromide 4 carbonitrile amine 59 is prepared according to the procedure described in the amine 56, but is used alternatively in the step ι Budo-4-carbonitrile (1 equivalent) is used as a starting point, and in step 2, cesium bromide (1 equivalent) is used as an alkylating agent. Amine 60 N-U4-fluoro-H-phenyl ))-1H_吲哚冬基]曱基}Cyclopropylamine 60 is made according to the shoe last's spearman's order described in amine 56, but in step 1, instead using 4·gas base "(1 equivalent) as the starting (four), and in step 2, using the evolutionary master (1.5 equivalents) as the saponification reagent. · Amine 61 N. aryl-indole (3. fluorophenyl) methyl HH_ ah _ 3 yl} methyl) cyclopropylamine 6: L is prepared according to the procedure described in amine 56, but in step ^ Instead of using 4-fluoro-1H-»?丨哚 (1 equivalent) as the main I) as the starting ten, and in Step 2, 'using 1-(bromomethyl)-3-fluoro Stupid (15 to Dantian) as an alkylation reagent. Amine 62 143482-1 •118- 201111364 N-({4-Fluoro-i_[3_(decyloxy)propyl]_1H_吲哚}}methyl propylamine 62 is based on the amine 56 The procedure was made, but in the step, 4-fluoroyl-1Ηβ丨哚 (1 equivalent) was used instead as the starting oxime. Furthermore, odoryl-3-methoxypropane (2 equivalents) and Aihua Tetrabutyl (1 equivalent) is used as an alkylation mixture in Step 2. Amine 63 ΜΗ-Chloro-H3-(methoxy)propyl ΗΗ·4哚彳 丨 methyl) Cyclopropylamine The amine 63 was prepared according to the material described for the amine 56 towel, but 4-chloro-based oxime (1 equivalent) was used as the starting powder. Further, (iv)yl-3-methoxypropene (2 equivalents) and moth tetrabutyl-equivalent are used as the alkylation mixture in the step 2. Amine 64 Ν-([4-Chloro-small (phenylmethyl) Η 啊 _ _ 3 yl] methyl propylamine amide 64 is made according to the procedure described in amine 56, but in the step, alternatively Use a 4-gas base, ♦ (1 equivalent) as the starting ♦, and in step 2 'Use desertification xin (1.5 equivalents) as the pheno-acting amine 65 called Moji-small (phenylmethyl)_1Η ♦ Tobacco methyl} cyclopropylamine / guanidine is made according to the procedure described in % of amine 'but in the step, instead of 4-bromo-1Η-卩 卩 ( (1 Chundan from | wood ( 1 (Tianli) as the starting β哚, and in step 2, using cesium bromide (1.5 equivalents) as the alkylation reagent. Amine 66 Ν-[(4-Moji-H (3_a stupid) Methylamine (10) root two; methyl group propylamine 4, but in the step, for the 201111364 start whistle, and in step 2) as the alkylation test using 4-bromo-1H 蚓哚(1 equivalent) As a starting point, use ί-(bromomethyl)-3-dylbenzene (15 equivalents of 0 amine 67 Ν-({4-Mosyl small [3-(methoxy))propyl]) _ 吲哚 J J violent } methyl) cyclopropylamine 67 is made according to the procedure described in amine 56, but in step η Alternatively, 4-diyl amide (1 equivalent) is used as the starting (4). Further, 卜-methoxy-3-methoxypropane (2 equivalents) and moth tetrabutyl equivalent) are used in step 2 as The alkylation mixture is used. Amine 68 Ν-[(4-Fluoro-1Η-indol-3-yl)methyl)cyclopropylamine 68 is prepared according to the procedure described in amine 56, but in step i Instead of using 4-fluoro-1H ♦ (1 equivalent) as the starting ♦. Furthermore, step 2 is not necessary. 1-{H(Cyclopropylamino)methyl]-5-[3-(methoxy)propyl]phenyl acetophenone amine 69 is according to the procedure described in the published patent application 2 (10) 7/(10) 925 已production. Amine 70 5-[(cyclopropylamino)methyl]-1,3-bis[3-(methoxy)propyl]_2,4(1H,3H)-pyrimidinedione Step 1: 1,3-double (3-methoxypropyl)-2,4-dione-l,2,3,4-tetrahydropyrimidinium formaldehyde at 〇 ° C in 5-methylmercaptouracil (1 equivalent) In the DMF (0.35 M) solution, 1-bromo-3-methoxypropane (2.2 equivalents) and DBU (2.2 when 143482-1 -120-201111364 amount) were successively added. The resulting solution was stirred at room temperature for 72 hours. The volatiles are then removed in a vacuum. The crude product mixture thus obtained was directly purified by column chromatography to give the title compound (yield: EtOAc). Step 2: Amine 70 is obtained from the previous step of 1,3-bis(3-decyloxypropyl)_2,4•dioneyl_u,3,4_tetrahydrozeridin-5-carboxaldehyde α equivalent) In the di-methane (01M) solution, # sulfuric acid (1 equivalent) and cyclopropylamine (2 equivalents) were added. The resulting suspension was stirred at room temperature for 16 hours. The insoluble material was removed by filtration and washed with dioxane, and then the combined filtrate was concentrated in vacuo to give the crude imine thus obtained dissolved in methanol. In the case of 0·1Μ), the butterfly hydrogenation (15 equivalents) was added in portions. The reaction mixture was stirred at room temperature for 16 h then EtOAc EtOAc m. The combined organic extracts were further washed with water and brine, dried over NasSO4, filtered, and concentrated. The crude product thus obtained was purified by column chromatography eluting elut elut elut elut elut elut elut elut Amine 71 N-[5-(3-methoxypropyl)-2,3-dimercaptobenzyl]cyclopropylamine Step 1: 5-Bromo-2,3-dimethylbenzoic acid at 2,3 Nitric acid (12 equivalents), water (25 equivalents) and bromine (U equivalent) were successively added to a stirred acetic acid solution (1) 2M) of dimethylbenzoic acid (1 eq.). Finally, silver nitrate (1 M aqueous solution '1.3 equivalents) was added dropwise over a period of 30 minutes. After stirring for an additional hour at room temperature, the crude reaction mixture was diluted with water, 143482-] • 121 - 201111364 and extracted with EtOAc. The combined organic extracts are then washed with brine to

Na2S04脫水乾燥,過濾,及使遽液在真空中濃縮。如此獲 得之粗產物在己烷中之研製,獲得標題化合物,為黃色固 體。 步驟2 : 5-溴-N-環丙基-2,3-二曱基苯甲醯胺 於得自前一步驟之5-溴基-2,3-二曱基苯曱酸(1當量)之經 擾掉DMF(0.2M)溶液中’添加HATU(U當量)、環丙基胺(12 當量)及Hunig氏驗(3當^。冑所形成之反應混合物在室溫 下獲拌18小時。然後’以飽和氣化銨水溶液使反應泮滅, 並以EtOAc萃取。將合併之有機萃液以水與鹽水進一步洗 滌,以Ν^〇4脫水乾燥,過渡,及使遽液在真空中濃縮。 如此獲得之粗產物經由急驟式層析之純化(Si〇2,7:3 (ν/ν)己 烷:Et〇AC~&gt;Et〇AC),獲得標題化合物,為白色固體。 步驟3: N-環丙基_5_[⑽各甲氧基+丙稀小基]2,3二甲基苯甲 醯胺 將得自前一步驟之5-溴_Ν_環丙基_2,3二f基苯甲醯胺(ι 當量)與4,4,5,5-四甲基![(1e)_3_(甲氧基)」丙烯小基η,3,2·二 氧硼伍園(1.5當量)合併於DMF ·· n_pr〇H之5:1 (ν/ν)混合物 (0.1Μ)中。然後,於此溶液中,添加反式雙(三苯膦)漠化鈀 (11)(0.05田里)’並將谷器重複抽氣,且以氮逆充填。最後, 添加2Μ Na2C03水溶液(3當量),並將所形成之兩相懸浮液 在觸。C下加熱18小時。使目前黑色懸浮液冷卻至室溫以 水稀釋,且以⑽萃取。接著,將合併之有機萃液以水與鹽 水洗滌,以NaaSO4脫水乾燥,過濾,及使濾液在真空中濃 143482-1 •122· 201111364 縮。粗產物經由急驟式層析之純化(Si〇2,9:i(v/v)己貌:Ε· —EtO Ac),獲得標題化合物,為白色固體。 步驟4 : &amp;環丙基—Μ-甲氧基丙基)-2,3-二甲基苯甲醯胺 使得自前—步驟之N環丙基_5·[(1Ε)·3_曱氧基小丙稀小基]_ 2’3 一甲基苯甲酿胺(1當幻與鹏*纪/炭(〇 〇5當量)懸浮 於EtOAc ((Χ2Μ)中。然後,將容器抽氣,並以%條氣。在經 充填&amp;大氣之氣瓶下,將反應懸浮液於室溫下攪拌6小時。 接著,使反應懸浮液經過矽藻土床過濾,並使濾液在真空 中濃縮,而得標題化合物,為白色固體。 步驟5 :胺71 於得自前一步驟之N_環丙基_5_(3_曱氧基丙基)_2,3_二曱基 苯曱醯胺(1當量)在THF (0.1M)中之回流溶液内,裝有短路徑 蒸餾裝置逐滴添加硼烷-硫化二曱烷複合物(6當量)。使溶液 濃縮至0.3M,歷經30分鐘,並添加HC1 (2N水溶液’ 6 5當量)。 將混合物於80°C下攪拌1小時,冷卻至室溫,以2N Na〇H水 φ 溶液賦與鹼性,並以EtOAc萃取。然後,將合併之有機萃液 以鹽水洗滌,以NazSO4脫水乾燥,過濾,及使濾液在真空 中濃縮。粗產物經由急驟式層析之純化(Si〇2 ’ 9:1 (v/v)己烷: EtOAc— EtOAc),獲得標題化合物,為淡黃色油。 胺72 N-[2-氣基-5-(2-曱氧基乙氧基)芊基]環丙胺 步驟1 : 1-氣基-4-(2-甲氧基乙氧基)·2-甲苯 於4-氯基-3-甲基盼(1當量)在DMF (0.7Μ)中之經授拌溶液 内,添加&amp; CO3 (1.2當量)。將混合物於50°C下攪拌5分鐘, 143482-1 • 123 201111364 然後添加1-溴基-2-甲氧基乙烧(1.5當量)。在7〇°C下2小時後, 使反應混合物冷卻至室溫,接著以水與醚稀釋。分離有機 相’並以2N NaOH水溶液、水及鹽水相繼洗滌。使有機萃液 以Naa S〇4脫水乾燥,過滤,及使渡液在真空中漠縮,而得 標題化合物,為帶黃色油。 步驟2 : 2-(溴基曱基)-μ氣基_4-(2-曱氧基乙氧基)苯 使付自别一步驟之1-氯基-4-(2-曱氧基乙氧基)_2_曱苯(1當 畺)、NBS (1.1當量)及過氧化二苯甲醯(〇 〇5當量)在 (0.2M)中之混合物回流2小時。然後,於真空中移除揮發性 物質,並使所开&gt; 成之殘留物懸浮於己烧中。經由過濾移除 不溶物,且以己烷進一步洗滌。使濾液在真空中濃縮,而 得標題化合物,為無色油。 步驟3 : 2-氣基-5-(2-曱氧基乙氧基)苯曱醛 將得自前一步驟之2-(溴基甲基H•氣基_4_(2_甲氧基乙氧 基)苯(1當量)與NM0 (3當量)在9〇t下,於二氧陸圜(〇3M) 中授拌6小時。‘然後’以飽和碳酸氫鈉水溶液使反應混合物 淬滅,且以醚萃取。將合併之有機萃液以水與鹽水進一步 洗滌,以NaiSO4脫水乾燥,過濾,及使濾液在真空中濃縮。 如此獲得之粗產物經由急驟式層析之純化(Si〇2,9:ι (v/v)己 烷:EtOAc—EtOAc),獲得標題化合物。 步驟4 :胺72 曰將得自前一步驟之2·氯基甲氧基乙氧基)苯甲醛(1當 量)與環丙基胺(2當量)合併於CH2C12(〇2M)中。然後,於其 中添加MgS04 (1.5當量),並將所形成之懸浮液在室溫下攪拌 143482-1 •124- 201111364 18小時。接著,經由過濾,經過矽藻土墊移除不溶物,及 使濾液在真空中濃縮。然後,使如此獲得之粗製亞胺再溶 於THF : Me〇H之2:1 (v/v)混合物(0.2M)中。於此溶液中,分次 添加蝴氫化鈉(5當量),且將所形成之混合物在室溫下搜摔 18小時。以飽和碳酸氫鈉水溶液使反應淬滅,並以醋酸乙 酯萃取。接著,將合併之有機萃液以鹽水洗滌,以 脫水乾燥,過濾,及使濾液在真空中濃縮。粗產物經由急 驟式層析之純化(Si〇2,9:1 (v/v)己烷·· Et0Ac— Et〇Ac),獲得 標題化合物,為帶黃色油。 胺73 N-(2-萘基甲基)環丙胺 胺73係根據胺π中所述之程序製成,但替代地使用孓萘 甲醛作為起始物質。 胺74 N-({3-[U氟曱基)硫基]笨基}曱基)環丙胺 胺74係根據胺17中所述之程序製成,但替代地使用^七三 II曱基)硫基]苯曱經作為起始物質。 胺75 N-{[5-[3-(曱氧基)丙基]_2_(甲硫基)苯基]甲基}環丙胺 步驟1 : 5-溴基-2-(甲硫基)苯甲酸曱酯 於碳酸铯(3當量)與5_溴基_2_酼基苯曱酸(1當量)之DMp (0.2M)懸浮液中’添加破曱烧(5當量)。然後,將所形成之 懸洋液在室溫下攪拌1小時。移除揮發性物質,接著添加 EtOAc與飽和水溶液。分離有機相,以Na2S〇4脫水乾 1434B2-1 -125- 201111364 燥,過濾,及使濾液在真空中濃縮成淡黃色油。使其再一 次溶於DMF (0.2M)中,並相繼地添加氫化鈉(3當量)與峨甲 烷(5當量)。接著,將反應容器密封,且加熱至7〇〇c,歷經 16小時。於冷卻至室溫後,將Et〇Ac與飽和Nh4C1水溶液添 加至粗製反應混合物中。分離有機相,以MgS〇4脫水乾燥, 過濾,及使濾液在真空中濃縮成褐色油。如此獲得之粗產 物經由急驟式層析之純化(Si〇2,己烷—3:2 (v/v)己烷: EtOAc) ’獲得標題化合物,為淡黃色固體。 步驟2 : 5-[3-(曱氧基)丙基]_2-(甲硫基)苯曱酸甲酯 於9-BBN (2當量)之THF (〇.29M)溶液中,逐滴添加烯丙基 甲基ϋ (2.1當量)’並將所形成之溶液在室溫下攪拌,直到 不再發現氣體釋出為止。然後,將反應混合物加熱至50c»c, 歷經1小時。接著,於此溶液中,添加得自前一步驟之5-溴基_2_(曱硫基)苯甲酸甲酯(1當量)、磷酸鉀(2.5當量)及[1,1,-雙(二苯基膦基)-二環戊二烯鐵]二鈀(π)二氣甲烷複合物(〇工 當量)之DMF (0.34M)溶液。將所形成之紅色懸浮液在8〇°c下 加熱16小時。於冷卻至室溫後,將反應物以醚與水稀釋。 分離有機層’並以水與鹽水進一步洗滌,以MgS〇4脫水乾燥, 過滤’且使渡液在真空中濃縮。如此獲得之粗產物經由急 驟式層析之純化(Si〇2 ’ 9:1 (v/v)己烷:EtOAc— 7:3 (v/v)己烷: EtO Ac) ’獲得標題化合物,為無色油。 步驟3 : 5-[3-(曱氧基)丙基]_2_(曱硫基)字醇 使得自前一步驟之5_[3_(曱氧基)丙基]·2_(甲硫基)苯曱酸甲 醋(1當量)溶於THF (0.1Μ)中,然後添加氫化鋰鋁(1當量)。 143482-1 -126- 201111364 將如此獲得之反應混合物在室溫下攪拌16小時。接著,以 IN HC1水溶液使反應淬滅,且以醚萃取。將合併之有機萃 液以水與鹽水進一步洗滌,以NkSO4脫水乾燥,及過濾。 濾液在真空中之濃縮,獲得粗製標題化合物,為白色固體。 步驟4 : 5-[3-(曱氧基)丙基]-2-(甲硫基)苯曱酿 於得自前一步驟之5-[3-(甲氧基)丙基]_2•(曱硫基)罕醇(1當 量)之二氣曱烷溶液中,添加碳酸氫鈉(5當量)與DMp(11當 量)。將所形成之反應懸浮液在室溫下攪拌1.5小時。以飽 和NaHS〇3水溶液使反應淬滅,然後以二氯曱烷萃取。將合 併之有機萃液以INNaOH水溶液、水及鹽水進一步洗滌,以Na2S04 was dehydrated, filtered, and the mash was concentrated in vacuo. The crude product thus obtained was triturated in hexane to give the title compound as a yellow solid. Step 2: 5-Bromo-N-cyclopropyl-2,3-dimercaptobenzamide in 5-bromo-2,3-dimercaptobenzoic acid (1 equivalent) from the previous step The reaction mixture formed by adding HATU (U equivalent), cyclopropylamine (12 equivalents) and Hunig's test (3 when 胄.) was stirred in a DMF (0.2 M) solution for 18 hours at room temperature. The reaction was then quenched with saturated aqueous ammonium sulphate and extracted with EtOAc. The combined organic extracts were further washed with water and brine, dried and evaporated, and evaporated and evaporated. The crude product thus obtained was purified by flash chromatography (EtOAc: EtOAc: EtOAc: EtOAc: EtOAc N-cyclopropyl_5_[(10) methoxy+propyl small base] 2,3 dimethyl benzamide will be obtained from the previous step of 5-bromo-indole_cyclopropyl-2,3 dif Benzobenzamide (1 eq) with 4,4,5,5-tetramethyl![(1e)_3_(methoxy)propenyl η,3,2·dioxaboron (1.5 equivalents) ) is combined in a 5:1 (v/v) mixture (0.1 Μ) of DMF ·· n_pr〇H. Then, in this solution, add Trans bis(triphenylphosphine) desertified palladium (11) (0.05 ton) and the gas was repeatedly pumped and reverse packed with nitrogen. Finally, 2 Μ aqueous Na2C03 (3 equivalents) was added and formed The two-phase suspension was heated at 18 ° C. The current black suspension was cooled to room temperature and diluted with water and extracted with (10). The combined organic extracts were washed with water and brine and dried over NaaSO. Filtration, and the filtrate was concentrated in a vacuum 143482-1 •122· 201111364. The crude product was purified by flash chromatography (Si〇2,9:i(v/v): Ε·-EtO Ac), The title compound is obtained as a white solid. Step 4: &amp; cyclopropyl- hydrazino-methoxypropyl)-2,3-dimethylbenzamide as the N-cyclopropyl _5. (1Ε)·3_曱oxy propylene small base]_ 2'3 monomethylbenzamide (1 when illusion and Pengji / charcoal (〇〇 5 equivalent) suspended in EtOAc ((Χ2Μ) Then, the vessel was evacuated and purged with a strip of gas. The reaction suspension was stirred at room temperature for 6 hours under a filled &amp; atmospheric cylinder. Next, the reaction suspension was passed through a bed of diatomaceous earth. Filtration and concentrating the filtrate in vacuo to give the title compound as a white solid. Step 5:amine 71 </RTI> </RTI> <RTIgt; The borane-dioxane-sulphide complex (6 equivalents) was added dropwise in a short-path distillation apparatus in a refluxing solution of dimercaptobenzamine (1 equivalent) in THF (0.1 M). The solution was concentrated to 0.3 M over 30 minutes and HCl (2N aqueous solution &lt The mixture was stirred at 80 &lt;0&gt;C for 1 h, cooled to rt and EtOAc (EtOAc)EtOAc. Then, the combined organic extracts were washed with brine, dried over NazSO4, filtered, and evaporated. The crude product was purified by flash chromatography eluting elut elut elut elut Amine 72 N-[2-Alkyl-5-(2-decyloxyethoxy)indolyl]cyclopropylamine Step 1: 1-Alkyl-4-(2-methoxyethoxy)·2- Toluene was added to &lt;CO3 (1.2 eq.) in a stirred solution of 4-chloro-3-methyl-(1 eq.) in DMF (0.7 EtOAc). The mixture was stirred at 50 ° C for 5 minutes, 143482-1 • 123 201111364 and then 1-bromo-2-methoxyethene (1.5 equivalents) was added. After 2 hours at 7 ° C, the reaction mixture was cooled to room temperature then diluted with water and ether. The organic phase was separated and washed successively with 2N aqueous NaOH, water and brine. The organic extract was dried over Na.sub.2.sub.4, filtered, and then evaporated to dryness to give the title compound as a yellow oil. Step 2: 2-(Bromoindenyl)-μ-carbyl-4-(2-decyloxyethoxy)benzene is added to 1-chloro-4-(2-methoxy-4-) from another step A mixture of oxy) 2 - fluorene (1 hydrazine), NBS (1.1 eq.) and diphenylguanidinium peroxide (5 eq.) in (0.2 M) was refluxed for 2 hours. Then, the volatile matter was removed in a vacuum, and the residue which was opened was suspended in the burned. The insoluble material was removed via filtration and further washed with hexane. The filtrate was concentrated in vacuo to give the title compound. Step 3: 2-Alkyl-5-(2-decyloxyethoxy)benzofural will be obtained from the previous step 2-(bromomethyl H• gas-based _4_(2-methoxyethoxy) Benzene (1 eq.) and NM0 (3 eq.) were mixed in dioxane (〇3M) for 6 hours at 9 〇t. 'Then' then quenched with a saturated aqueous solution of sodium bicarbonate, and The combined organic extracts were further washed with water and brine, dried over NaiSO4, filtered, and the filtrate was concentrated in vacuo. The crude product thus obtained was purified by flash chromatography (Si〇2,9 : ι (v/v) hexanes: EtOAc (EtOAc) ieldielielielielielielielielielielielielielielielielielielielielielielielielielielielielielielieliel Propylamine (2 equivalents) was combined in CH2C12 (〇2M). Then, MgS04 (1.5 equivalents) was added thereto, and the resulting suspension was stirred at room temperature for 143482-1 • 124 - 201111364 for 18 hours. Next, the insoluble matter was removed through a diatomaceous earth pad through filtration, and the filtrate was concentrated in vacuo. Then, the crude imine thus obtained was redissolved in a 2:1 (v/v) mixture (0.2 M) of THF : Me〇H. To this solution, sodium hydrogen halide (5 eq.) was added in portions, and the resulting mixture was poured at room temperature for 18 hours. The reaction was quenched with saturated aqueous sodium bicarbonate and extracted with ethyl acetate. Next, the combined organic extracts were washed with brine, dried over Celite, filtered, and concentrated. The crude product was purified by flash chromatography eluting elut elut elut elut The amine 73 N-(2-naphthylmethyl)cyclopropylamine amine 73 was prepared according to the procedure described for the amine π, but instead using phthalamic acid as the starting material. Amine 74 N-({3-[U-fluoroindenyl)thio]]yl}indenyl)cyclopropylamine 74 is prepared according to the procedure described for amine 17, but alternatively using succinyl) Thio]benzoquinone is used as a starting material. Amine 75 N-{[5-[3-(indolyl)propyl]_2-(methylthio)phenyl]methyl}cyclopropylamine Step 1: 5-bromo-2-(methylthio)benzoic acid The oxime ester was added to the DMp (0.2 M) suspension of cesium carbonate (3 eq.) and 5-bromo-2-indolebenzoic acid (1 eq.) in EtOAc (5 eq.). Then, the formed suspension was stirred at room temperature for 1 hour. The volatiles were removed, followed by EtOAc and saturated aqueous. The organic phase was separated, dried over Na 2 EtOAc EtOAc (EtOAc) It was again dissolved in DMF (0.2 M), and sodium hydride (3 eq.) and methane (5 eq.) were successively added. Next, the reaction vessel was sealed and heated to 7 ° C for 16 hours. After cooling to room temperature, Et 〇Ac and a saturated aqueous solution of Nh 4 C 1 were added to the crude reaction mixture. The organic phase was separated, dried with EtOAc (EtOAc)EtOAc. The crude product thus obtained was purified by flash chromatography eluting elut elut elut elut Step 2: Methyl 5-[3-(decyloxy)propyl]_2-(methylthio)benzoate is added dropwise to a solution of 9-BBN (2 equivalents) in THF (〇.29M) Propylmethylhydrazine (2.1 equivalents)' and the resulting solution was stirred at room temperature until no more gas evolution was observed. The reaction mixture was then heated to 50c»c for 1 hour. Next, in this solution, methyl 5-bromo-2-(indolyl)benzoate (1 equivalent), potassium phosphate (2.5 equivalent) and [1,1,-bis(diphenyl) were added from the previous step. A solution of phosphinyl)-dicyclopentadienyl iron] dipalladium (π) digas methane complex (labile equivalent) in DMF (0.34 M). The resulting red suspension was heated at 8 ° C for 16 hours. After cooling to room temperature, the reaction was diluted with ether and water. The organic layer was separated and washed further with water and brine, dried with &lt;RTI ID=0.0&gt;&gt; The crude product thus obtained was purified by flash chromatography (Si 〇 2 ' 9:1 (v/v) hexane: EtOAc - 7:3 (v/v) hexane: EtO Ac) Colorless oil. Step 3: 5-[3-(indolyl)propyl]_2_(indolyl)-alcohol allows 5_[3_(decyloxy)propyl]·2_(methylthio)benzoic acid from the previous step Methyl vinegar (1 eq.) was dissolved in THF (0.1 Torr) and then lithium aluminum hydride (1 eq.) was added. 143482-1 -126- 201111364 The reaction mixture thus obtained was stirred at room temperature for 16 hours. The reaction was then quenched with aqueous <RTI ID=0.0> IN </RTI> </RTI> <RTIgt; The combined organic extracts were further washed with water and brine, dried over NkSO4 and filtered. The filtrate was concentrated in vacuo to give crystallite crystallite Step 4: 5-[3-(Methoxy)propyl]-2-(methylthio)benzoquinone is obtained from 5-[3-(methoxy)propyl]_2•(曱) obtained from the previous step. To a solution of thio)hanol (1 equivalent) in dioxane, sodium hydrogencarbonate (5 equivalents) and DMp (11 equivalents) were added. The resulting reaction suspension was stirred at room temperature for 1.5 hours. The reaction was quenched with saturated aqueous Na.sub.3 solution and then extracted with dichloromethane. The combined organic extracts were further washed with aqueous INNaOH, water and brine to

MgS〇4脫水乾燥,及過濾。濾液在真空中之濃縮,獲得粗製 標題化合物,為無色油。 步驟5 :胺75 將得自前一步驟之5-[3-(甲氧基)丙基]_2_(曱硫基)苯甲醛(1 當量)與環丙基胺(2當量)合併於CH2C12(〇1m)中。然後,於 • 其中添加MgS〇4(2當量)與曱酸(αΐ當量),接著將所形成之 懸浮液在室溫下攪拌20小時。然後,經由過濾,經過矽藻 土塾移除不溶物’及使濾液在真空中濃縮。接著,使如此 獲得之粗製亞胺再溶於MeOH (0.1Μ)中。於此溶液中,分次 添加硼氫化鈉(5當量),並將所形成之混合物在室溫下攪拌 16小時。以1NHC1水溶液使反應淬滅,以1NNa0H水溶液中 和,且以醚萃取。然後,將合併之有機萃液以水與鹽水進 一步洗滌,以MgS〇4脫水乾燥,過濾,及使濾液在真空中濃 縮。粗產物經由急驟式層析之純化(Si〇2,3:2 (v/v)己燒:Et〇Ac )43482-1 -127- 201111364 —1:4 (v/v)己烷:EtOAc) ’獲得標題化合物,為無色油。 胺76 N-[3-溴基-5-(3-甲氧基丙基)-冬甲苄基]環丙胺 步驟1 : 3,5-二溴-N-環丙基:4-甲基苯曱醯胺 於3,5-二溴基-4-曱基苯曱酸q當量)在DMF (〇 4M)中之經攪 拌浴液内,添加HATU (1.3當量)、環丙基胺(丨丨當量)及Hunig 氏驗(3當量)。將所形成之黃色混合物於室溫下攪拌π小時 。然後,以飽和氣化銨水溶液使反應淬滅,並以醋酸乙酯 萃取。將合併之有機萃液以水與鹽水進一步洗滌,以Na2S〇4 脫水乾燥,過濾,及使濾液在真空中濃縮。如此獲得之粗 產物在醚與己烷之混合物中之研製,獲得標題化合物,為 灰白色固體。 步驟2 : 3-溴-N-環丙基-5-[(1Ε)-3-甲氧基丙d•烯小基]冬曱基苯 甲醯胺 於得自前一步驟之3,5-二溴-N-環丙基_4-甲基笨甲醯胺(1 當量)與4,4,5,5-四曱基-2-[(1Ε)-3-(曱氧基)_!•丙烯小基]_13,2_二 氧石朋伍園(1.1當量)在DMF (0.1M)中之溶液内,添加反式_雙 (三苯膦鳩化鈀(IIX0.05當量)。將容器重複抽氣,並以氮逆 充填。最後,添加2M NaaCO3水溶液(3當量),且將所形成 之混合物於l〇〇°C下加熱1小時。使目前黑色懸浮液冷卻至 至溫’以水稀釋’並以醋酸乙酯萃取。將合併之有機萃液 以水與鹽水進一步洗滌’以NadO4脫水乾燥,過濾,及使 壚液在真空中濃縮。粗產物經由急驟式層析之純化(Si〇2, 9:1 (v/v)己烷:EtOAc— EtOAc) ’獲得標題化合物,為黃橘色 143482-1 -128- 201111364 油0 步驟3 : 3-溴-N-環丙基-5-(3-甲氧基丙基)-4-甲基苯甲醯胺 於得自前一步驟之3-溴-N-環丙基-5-[(1Ε)-3-曱氧基丙-1-烯 -1-基]-4-曱基苯曱醯胺(1當量)在回流之甲苯(〇·ΐΜ)中之溶液 内’分次添加苯項醯醯肼(6當量),歷經2小時。於回流下 再加熱一小時後,使目前黑色反應懸浮液冷卻至室溫,以 飽和碳酸氫鈉水溶液使反應淬滅,並以醋酸乙酯萃取。然 後,將合併之有機萃液以鹽水洗滌,以Na2S04脫水乾燥, _ 過濾’及使濾液在真空中濃縮。粗產物經由急驟式層析之 純化(Si〇2 ’ 9:1 (v/v)己烷:EtOAc— EtOAc),獲得標題化合物, 為黃色油。 步驟4 :胺76 於得自前一步驟之3-溴-N-環丙基-5-(3-甲氧基丙基)_4-曱基 苯曱醯胺(1當量)在THF (0.2M)中之經攪拌溶液内,相繼地添 加硼氫化鈉(4當量)與BF3_THf複合物(4 5當量)。將如此獲 φ 得之反應溶液於40°C下加熱5小時,冷卻至0。(:,然後慢慢 地倒入6N HC1水溶液(4.5當量)中。將所形成之混合物於5〇 c下再加熱1小時,冷卻至室溫,以1〇N Na〇H水溶液鹼化, 且最後以醚萃取《接著,將合併之有機萃液以水與鹽水進 一步洗滌,以NazSO4脫水乾燥,過濾,及使濾液在真空中 濃縮,而得標題化合物,為無色油。 胺76甲烷磺酸鹽 N-[3-溴基-5-(3-曱氧基丙基)斗甲芊基]環丙胺甲烷磺酸鹽 143482-1 •129· 201111364The MgS〇4 was dehydrated and dried, and filtered. The filtrate was concentrated in vacuo to give the crude title compound. Step 5: Amine 75 Combine 5-[3-(methoxy)propyl]_2-(indolyl)benzaldehyde (1 eq.) from the previous step with cyclopropylamine (2 eq.) in CH2C12 (〇 1m). Then, MgS〇4 (2 equivalents) and citric acid (αΐ equivalent) were added thereto, and the resulting suspension was stirred at room temperature for 20 hours. Then, via infiltration, the insoluble matter was removed through the diatomaceous earth and the filtrate was concentrated in vacuo. Next, the crude imine thus obtained was redissolved in MeOH (0.1 Torr). To the solution, sodium borohydride (5 eq.) was added portionwise, and the resulting mixture was stirred at room temperature for 16 hr. The reaction was quenched with 1N aq. Then, the combined organic extracts were further washed with water and brine, dried over MgSO 4 , filtered, and concentrated in vacuo. Purification of the crude product by flash chromatography (Si 〇 2, 3:2 (v/v) hexanes: Et sAc) 43482-1 -127 - 201111364 -1:4 (v/v) hexane: EtOAc) 'The title compound was obtained as a colorless oil. Amine 76 N-[3-Bromo-5-(3-methoxypropyl)-m-methylbenzyl]cyclopropylamine Step 1: 3,5-Dibromo-N-cyclopropyl: 4-methylbenzene Addition of HATU (1.3 eq.), cyclopropylamine (丨丨) to a stirred bath of 3,5-dibromo-4-indolylbenzoic acid (q equivalent) in DMF (〇4M) Equivalent) and Hunig's test (3 equivalents). The resulting yellow mixture was stirred at room temperature for π hours. Then, the reaction was quenched with a saturated aqueous solution of ammonium sulfate and extracted with ethyl acetate. The combined organic extracts were further washed with water and brine, dried over Na 2 EtOAc, filtered, and evaporated. The crude product thus obtained was triturated in a mixture of ether and hexane to give the title compound as pale white solid. Step 2: 3-Bromo-N-cyclopropyl-5-[(1Ε)-3-methoxypropane d- ene small base] mercaptobenzamide is obtained from the previous step 3,5-two Bromo-N-cyclopropyl-4-methyl carbamide (1 eq.) and 4,4,5,5-tetradecyl-2-[(1Ε)-3-(decyloxy)_! Propylene small base]_13,2_dioxite Pengwuyuan (1.1 equivalent) in a solution of DMF (0.1M), add trans-bis (triphenylphosphine palladium (IIX 0.05 equivalent). Repeat the pump Gas, and reversed with nitrogen. Finally, 2M NaaCO3 aqueous solution (3 eq.) was added, and the resulting mixture was heated at 1 ° C for 1 hour. The current black suspension was cooled to a temperature 'diluted with water' And extracted with ethyl acetate. The combined organic extracts were further washed with water and brine, dried over NadO4, filtered, and concentrated in vacuo. The crude product was purified by flash chromatography (Si? 9:1 (v/v) Hexane: EtOAc - EtOAc (m.) EtOAc EtOAc EtOAc EtOAc -Methoxypropyl)-4-methylbenzamide in 3-bromo-N-cyclopropyl-5-[(s) from the previous step 1-Ε)-3-decyloxyprop-1-en-1-yl]-4-mercaptophenylguanamine (1 equivalent) in a solution of refluxing toluene (〇·ΐΜ) The reaction mixture was quenched with EtOAc (EtOAc)EtOAc. The combined organic extracts were then washed with brine, dried over Na2SO4, filtered, and filtered and evaporated in vacuo. The crude product was purified by flash chromatography (Si 〇 2 ' 9:1 (v/v) Hexane: EtOAc - EtOAc (EtOAc) The sodium borohydride (4 equivalents) and the BF3_THf complex (45 equivalents) were successively added to the stirred solution of decyl benzoguanamine (1 equivalent) in THF (0.2 M). The solution was heated at 40 ° C for 5 hours and cooled to 0. (:, then slowly poured into a 6 N aqueous HCl solution (4.5 eq.). After heating for 1 hour, cooling to room temperature, basifying with 1 〇N Na〇H aqueous solution, and finally extracting with ether. Then, the combined organic extracts were further washed with water and brine, dried over NazSO4, filtered, and The filtrate was concentrated in vacuo to give the title compound as a colourless oil. s s s s s s s s s s s s s s s s s s s s s s s s Salt 143482-1 •129· 201111364

丁 PdCI2(PPh3)2 。入 OH THFD. PdCI2(PPh3)2. OH THF

步驟1 : 3-溴基-5-碘基-4-甲基-苯曱酸 於3-溴基-4-曱基苯曱酸在96%硫酸中之經攪拌溶液 (〜0.58M反應濃度)内,添加N-碘基琥珀醯亞胺(1.1當量),歷 經1小時,保持溫度在10與30°C之間。使反應混合物熟成10 分鐘,然後於水中使反應淬滅。將漿液過濾,並以水、亞 硫酸氫鈉溶液,接著最後以水洗蘇,而得標題化合物,為 灰白色固體。1 H NMR (400 MHz,dmso-d6) : (5 13.4 (br s,1H) ; 8.30 (s,1H); 8.00 (s,1H); 2.64 (s,3H)。HRMS (ES,M-Η)計算值 338.8518. 實測值338.8516。 步驟2 : 3-溴基-5-(3-曱氧基-丙-1-炔基)-4-曱基-苯曱酸 於3-溴基-5-碘基-4-曱基-苯曱酸在THF (0.98M)中之經攪拌 溶液内,添加三乙胺(7.5當量)與碘化銅(0.01當量),接著為 PdCl2(PPh3 )2(0.005當量)。然後,添加炔丙基曱基醚(1.5當量), 並將混合物加熱至~65°C,歷經~24小時。使混合物冷卻至20 °C,接著以MTBE與水稀釋。將液層切割,並將有機物質以 另外之水洗滌。將合併之水層與另外之MTBE及5N HC1混 合。將有機層以1M HC1,以3% w/v亞硫酸氫鈉(兩次),及 143482-1 -130- 201111364 最後以水洗滌。使所形成之溶液濃縮至〜〇 38M,並以THF 中之溶液使用於下一步驟。iH NMR (4〇〇 MHz,丙酮_d6):占 8·13 (s,1Η) ; 8.00 (s,1Η) ; 4.40 (s,2Η) ; 3·41 (s,3Η) ; 2.59 (s,3Η)。 HRMS (ES,M-H)計算值 280.9813.實測值 280.9820。 步驟3: 3-溴-N-環丙基-5-(3-甲氧基-丙小炔基)_4_曱基_苯甲醯胺 於3-/臭基-5-(3-甲氧基-丙炔基)_4_甲基_苯曱酸(在THF中 之0.38M溶液)中,添加N,N_二異丙基乙胺(1 8當量)與環丙基 φ 胺(1.35當量),保持内部溫度低於25°C。使混合物冷卻至5 °C,並添加2-丙烷磷酸酐(50重量%,在Et〇Ac中,15當量), 同時保持内部溫度低於25t。使反應混合物在〜2〇t:下熟成 1小時,接著冷卻至2°C,並添加1〇重量% NH4C1水溶液,保 持内部溫度&lt;3(TC。添加醋酸異丙酯,且使液層沉降。移除 下方水層。然後,將有機物質以1Μ Ηα ,接著以 溶液,及最後以10% Naa溶液洗滌。使有機層濃縮至〜1M, 接著添加甲苯。然後,使此批料再濃縮至〜2M,並使所形 • 成之水液沾成18小時。接著,添加庚烷,且將固體過濾., 以U甲苯/庚烷之混合物洗滌,及乾燥,而得標題化合物, 為灰白色固體。1 H NMR (500 MHz’ 丙酮·d6):占 8 〇1 (s,m),7% (» 1H), 7.86 (s, 1H), 4.37 (s, 2H), 3.39 (s, 3H), 2.95-2.89 (m, 1H), 2.53 (s, H), 0.76 0.67 (m, 2H), 0.68-0.60 (m,2H)。HRMS (ES, M+H)計算值 322Ό443.實測值 322.0457。 步驟4 : 3-漠-N_環丙基-5_(3_甲氧基_丙基)冰甲基-苯甲酿胺 於3溴-N-%丙基_5·(3-甲氧基_丙炔基)斗曱基-苯甲醯胺 與氧化翻(_當量)在甲苯(仙Μ)中之經授拌溶液内,添 143482· 1 -131 - 201111364 加三乙胺(〇·2當量)。使所形成之溶液於丨8計示巴下氫化3 小時’然後過濾,以移除觸媒。使溶液濃縮至〜4份體積, 接著添加庚烷(8份體積)。將所形成之漿液過濾,而得產物, 為灰白色固體。1 H NMR (500 MHz,丙酮-4): 5 7.87 (m,2H),7.65 (s, 1H), 3.35 (t, J = 6.12 Hz, 2H), 3.27 (s, 3H), 2.93-2.86 (m, 1H), 2.75 (t, J = 7.91 Hz, 2H) ; 2.39 (s, 3H), 1.80-1.72 (m, 2H), 0.75-0.67 (m, 2H), 0.61-0.56 (m,2H)。HRMS (ES,M+H)計算值 326.0767.實測值 326.0756。 步驟5 :胺76 ❿ 於硼氫化鈉(2.0當量)在Thf (8份體積)中之經攪拌溶液 内,添加三氟化硼THF複合物(2.5當量),保持溫度&lt;3〇t。 然後,添加3-溴-N-環丙基-5-(3-曱氧基-丙基)冰曱基-苯曱醯胺 在THF中之溶液(3份體積),並使溶液於35。〇下熟成18小時。 藉由添加至5M鹽酸溶液中使反應混合物淬滅,接著使混合 物溫熱至50°C,且熟成90分鐘。於冷卻至2〇t後,添加庚烷 (3份體積)與甲基第三-丁基醚(3份體積)。使液層沉降,並 將下層切除。以5M HC1洗滌上層有機物質,且將下層水溶_ 液與第一個水層合併。使合併之水層冷卻至,然後添加 48% NaOH,以調整阳至14。添加甲基第三丁基醚(68份體 積),並分離液層。將水層以MTBE逆萃取。使合併之有機 物質濃縮至〜4份體積,接著添加THF(3份體積)。使溶液溫 熱至40°C,且添加曱烷磺酸(〇_95當量)。使所形成之漿液冷 卻至環境溫度,然後過濾,及將固體以MTBE洗滌,而得標 題化合物,為灰白色固體。1H NMR (5〇〇 MHz,DMS〇d6) 5 8 87 143482-1 -132- 201111364 (s, 2H), 7.61 (s, 1H), 7.30 (s, 1H), 4.17 (s, 2H), 3.35 (m, J = 6.23 Hz, 2H), 3.24 (s, 3H), 2.71-2.64 (m, 3H), 2.34 (s, 3H), 2.30 (s, 3H), 1.77-1.69 (m, 2H), 0.82-0.77 (m’ 2H), 0.77-0.70 (m, 2H)。HRMS (ES,M+H)計算值 312.0963.實測值 312.0978。 胺77 N-({3,5-雙[3-(甲氧基)丙基]苯基丨曱基)環丙胺 步驟1 : N-[(3,5-二溴苯基)甲基]環丙胺 將3,5-二溴基苯甲醛(1當量)、環丙基胺(2當量)及硫酸鎂 (1當I)在二氯甲烷(0.1M)中攪拌2〇小時。然後,經由過濾, 經過矽藻土墊移除不溶物,並以二氯曱烷進一步洗滌。使 濾液在真空中濃縮,而得粗製亞胺,接著使其立即再溶於 MeOH (0.1M)中。於此溶液中,分次添加硼氫化鈉(5當量), 且將所形成之混合物在室溫下攪拌4小時。以1Ν Ηα水溶液 使反應淬滅,以IN NaOH水溶液中和,並以醚萃取。然後, 將合併之有機卒液以水與鹽水進一步洗滌,以MgS〇4脫水乾 燥,及過濾。濾液在真空中之濃縮,獲得標題化合物,為 淡黃色油。 步驟2 :環丙基(3,4-二溴基苄基)胺基曱酸第三_丁酯 使得自前一步驟之队[(3,5_二溴苯基)曱基]環丙胺(1當量) 與一碳酸一-第三-丁酯(1當量)溶於二氣曱烷(〇12M)中。然 後,於其中添加Hunig氏鹼(1.3當量),並將所形成之混合物 在室溫下攪拌16小時。於真空中移除揮發性物質,且使所 形成之殘留物溶於己烷與醚之1:1(v/v)混合物中。接著,將 此懸浮液以ιο%Ηα水溶液 '水及鹽水洗滌,以Na2S〇4脫水 143482-1 •133· 201111364 乾燥丄過渡,及使渡液在真空中漢縮。如此獲得之粗產物 經由管柱層析之純化(Si〇2,己烷—1:1 (v/v)己烷:Et〇Ac), 獲得標題化合物,為淡黃色油。 步驟3 : {3,5-雙[(1E&gt;3_甲氧基小丙烯小基]节基丨環丙基胺基甲 酸第三-丁酯 於付自前一步驟之環丙基(3,4·二溴基芊基)胺基甲酸第三_ 丁酯(1當量)與4,4,5,5-四甲基_2-[(1E)_3-(曱氧基)·μ丙烯+ 基]-1’3,2-二氧硼伍圜(2.2當量)在DMF (0.14Μ)中之溶液内,添 加反式-雙(三苯膦)、;臭化鈀(11)(〇1當量ρ將容器重複抽氣,籲 並以氮逆充填。最後,添加2M Na2c〇3水溶液(6當量),且 將所形成之混合物於90°C下加熱6小時。使目前黑色懸浮液 冷卻至室溫,以水稀釋,並以醚萃取。將合併之有機萃液 以10% HC1水溶液' IN NaOH水溶液、水及鹽水進一步洗滌, 以NaaSO4脫水乾燥,過濾’及使濾液在真空中濃縮。粗產 物經由急驟式層析之純化(Si〇2,己烷-&gt; 1:i (v/v)己烧:Step 1: 3-Bromo-5-iodo-4-methyl-benzoic acid in 3-bromo-4-indolylbenzoic acid in 96% sulfuric acid, stirred solution (~0.58M reaction concentration) N-iodoylsuccinimide (1.1 equivalents) was added, and the temperature was maintained between 10 and 30 ° C over 1 hour. The reaction mixture was allowed to mature for 10 minutes and then quenched in water. The syrup was filtered and washed with water, sodium bisulfite, and then water, and the title compound was obtained as an off white solid. 1 H NMR (400 MHz, dmso-d6): (5 13.4 (br s, 1H); 8.30 (s, 1H); 8.00 (s, 1H); 2.64 (s, 3H). HRMS (ES, M-Η) Calculated value 338.8518. Found 338.8516. Step 2: 3-Bromo-5-(3-decyloxy-prop-1-ynyl)-4-mercapto-benzoic acid on 3-bromo-5- To a stirred solution of iodo-4-indolyl-benzoic acid in THF (0.98 M), triethylamine (7.5 eq.) and copper iodide (0.01 eq.), followed by PdCl2 (PPh3)2 (0.005) Then, add propargyl decyl ether (1.5 eq.), and heat the mixture to ~65 ° C for ~24 hours. Allow the mixture to cool to 20 ° C, then dilute with MTBE and water. The organic material was washed with additional water. The combined aqueous layers were mixed with additional MTBE and 5N HCl. The organic layer was 1 M HCl, 3% w/v sodium bisulfite (twice), and 143482 -1 -130- 201111364 Finally, it was washed with water. The resulting solution was concentrated to ~ 〇 38M, and used in THF in the next step. iH NMR (4 〇〇 MHz, acetone _d6): 8% 13 (s,1Η) ; 8.00 (s,1Η) ; 4.40 (s,2Η) ; 3·41 (s,3Η) ; 2.59 (s 3 Η). HRMS (ES, MH) calc. 280.9813. Found: 280.9820. Step 3: 3-bromo-N-cyclopropyl-5-(3-methoxy-propi-propynyl)_4-fluorenyl-benzene Addition of N,N-diisopropyl to metoamine in 3-/odoryl-5-(3-methoxy-propynyl)-4-methyl-benzoic acid (0.38 M solution in THF) Ethylethylamine (18 equivalents) and cyclopropyl φ amine (1.35 equivalents), keeping the internal temperature below 25 ° C. The mixture was cooled to 5 ° C and 2-propane phosphoric anhydride (50% by weight, at Et) 〇Ac, 15 equivalents) while maintaining the internal temperature below 25 t. The reaction mixture was aged at ~2 〇t: for 1 hour, then cooled to 2 ° C, and 1 〇 wt% NH4C1 aqueous solution was added to maintain the internal temperature &lt; 3 (TC. Add isopropyl acetate and settling the liquid layer. Remove the lower aqueous layer. Then, the organic material is washed with 1 Μ Η α, followed by solution, and finally with 10% Naa solution. The organic layer is concentrated to ~1M, then add toluene. Then, the batch was re-concentrated to ~2M, and the formed liquid was immersed for 18 hours. Then, heptane was added, and the solid was filtered. U toluene / g Alkane The mixture was washed and dried to give the title compound m. 1 H NMR (500 MHz 'acetone·d6): 8 〇 1 (s, m), 7% (» 1H), 7.86 (s, 1H), 4.37 (s, 2H), 3.39 (s, 3H), 2.95-2.89 (m, 1H), 2.53 (s, H), 0.76 0.67 (m, 2H), 0.68-0.60 (m, 2H). HRMS (ES, M+H) calculated 322 Ό 443. Found 322.0457. Step 4: 3-Di-N-cyclopropyl-5-(3-methoxy-propyl)-glacial methyl-benzamide in 3 bromo-N-% propyl _5·(3-methoxy _propynyl), fluorenyl-benzamide and oxidized ruthenium (_equivalent) in toluene (sand) in a mixed solution, add 143482 · 1 -131 - 201111364 plus triethylamine (〇·2 equivalent). The resulting solution was hydrogenated at 丨8 for 3 hours and then filtered to remove the catalyst. The solution was concentrated to ~4 parts by volume followed by heptane (8 parts by volume). The resulting slurry was filtered to give the product as an off white solid. 1 H NMR (500 MHz, Acetone-4): 5 7.87 (m, 2H), 7.65 (s, 1H), 3.35 (t, J = 6.12 Hz, 2H), 3.27 (s, 3H), 2.93-2.86 ( m, 1H), 2.75 (t, J = 7.91 Hz, 2H); 2.39 (s, 3H), 1.80-1.72 (m, 2H), 0.75-0.67 (m, 2H), 0.61-0.56 (m, 2H) . HRMS (ES, M+H) calcd. 326.0767. Found. Step 5: Amine 76 ❿ In a stirred solution of sodium borohydride (2.0 eq.) in Thf (8 vol.), boron trifluoride THF complex (2.5 eq.) was added, maintaining the temperature &lt;3 〇t. Then, a solution of 3-bromo-N-cyclopropyl-5-(3-decyloxy-propyl) halocyl-benzoguanamine in THF (3 parts by volume) was added, and the solution was allowed to be 35. Cooked for 18 hours. The reaction mixture was quenched by addition to a 5M aqueous solution of hydrochloric acid, then the mixture was warmed to 50 &lt After cooling to 2 Torr, heptane (3 parts by volume) and methyl third-butyl ether (3 parts by volume) were added. The liquid layer is allowed to settle and the lower layer is cut. The upper organic material was washed with 5 M HCl and the lower aqueous solution was combined with the first aqueous layer. The combined aqueous layers were allowed to cool to and then 48% NaOH was added to adjust the yang to 14. Methyl tertiary butyl ether (68 parts by volume) was added, and the liquid layer was separated. The aqueous layer was back extracted with MTBE. The combined organic material was concentrated to ~4 parts by volume followed by THF (3 parts by volume). The solution was allowed to warm to 40 ° C and decanesulfonic acid (〇_95 equivalent) was added. The resulting slurry was allowed to cool to ambient temperature then filtered and the solid was washed with &lt 1H NMR (5〇〇MHz, DMS〇d6) 5 8 87 143482-1 -132- 201111364 (s, 2H), 7.61 (s, 1H), 7.30 (s, 1H), 4.17 (s, 2H), 3.35 (m, J = 6.23 Hz, 2H), 3.24 (s, 3H), 2.71-2.64 (m, 3H), 2.34 (s, 3H), 2.30 (s, 3H), 1.77-1.69 (m, 2H), 0.82-0.77 (m' 2H), 0.77-0.70 (m, 2H). HRMS (ES, M+H) calculated 312.0963. Found 312.0978. Amine 77 N-({3,5-bis[3-(methoxy)propyl]phenylindenyl)cyclopropylamine Step 1: N-[(3,5-Dibromophenyl)methyl] ring The propylamine was stirred for 3 hours in dichloromethane (0.1 M) in 3,5-dibromobenzaldehyde (1 eq.), cyclopropylamine (2 eq.) and magnesium sulfate (1). The insolubles were then removed via filtration through a pad of diatomaceous earth and further washed with dichloromethane. The filtrate was concentrated in vacuo to give crude imamine, which was then taken again in MeOH (0.1M). To the solution, sodium borohydride (5 eq.) was added portionwise, and the resulting mixture was stirred at room temperature for 4 hr. The reaction was quenched with aqueous 1 Η Ηα, neutralized with aqueous 1 N NaOH and extracted with ether. Then, the combined organic strokes were further washed with water and saline, dehydrated with MgS 4 and filtered. The filtrate was concentrated in vacuo to give the title compound. Step 2: Cyclopropyl (3,4-dibromobenzyl)amine decanoic acid tert-butyl ester from the previous step of the team [(3,5-dibromophenyl)indolyl]cyclopropylamine (1 Equivalent) is dissolved in dioxane (〇 12M) with mono-tri-butyl acrylate (1 equivalent). Then, Hunig's base (1.3 equivalents) was added thereto, and the resulting mixture was stirred at room temperature for 16 hours. The volatiles were removed in vacuo and the residue formed was dissolved in a 1:1 (v/v) mixture of hexanes and ether. Next, the suspension was washed with water and brine of ιο% Ηα, dehydrated with Na2S〇4, 143482-1 • 133·201111364, and the mixture was hanked in a vacuum. The crude product thus obtained was purified by EtOAc EtOAcjjjjjjj Step 3: {3,5-bis[(1E&gt;3_methoxypropenyl small group] benzylidene Cyclopropylaminocarbamic acid tert-butyl ester in the cyclopropyl group from the previous step (3,4 Di-tert-butyl ester (1 equivalent) and 4,4,5,5-tetramethyl-2-[(1E)_3-(decyloxy)·μpropene + base -1'3,2-dioxaboron (2.2 equivalents) in a solution of DMF (0.14 Torr), adding trans-bis(triphenylphosphine), palladium (11) (〇1 equivalent) ρ The vessel was repeatedly evacuated and flushed with nitrogen. Finally, 2M Na2c〇3 aqueous solution (6 equivalents) was added, and the resulting mixture was heated at 90 ° C for 6 hours. The current black suspension was cooled to room. The mixture was diluted with water and extracted with ether. The combined organic extracts were further washed with 10% aqueous HCl solution &lt;RTI ID=0.0&gt; Purification by flash chromatography (Si〇2, hexane-&gt; 1:i (v/v) hexane:

EtOAc) ’獲得標題化合物,為淡黃色油。 步驟4 : [3,5-雙(3-甲氧基丙基);基]環丙基胺基曱酸第三丁酉旨 使得自前一步驟之{3,5-雙[(1Ε)-3-曱氧基-1-丙烯-μ基;基} 環丙基胺基甲酸第三-丁酯(1當量)與10% w/w鈀/炭(〇1當 量)懸浮於EtOAc (0.05M)中。然後,將容器抽氣,並以叫條 氣。在經充填%大氣之氣瓶下,將反應懸浮液於室溫下授 拌3小時。接著’以二氯甲烷使反應懸浮液淬滅,且經過石夕 藻土床過濾。濾液在真空中之濃縮,獲得標題化合物,為 黃色油。 143482-1 -134- 201111364 步驟5 :胺77 於付自則—步驟之[3,5_雙(3-曱氧基丙基)罕基]環丙基-胺 基曱酸第二-丁酯(1當量)在CH2C12(0.1M)中之溶液内,添加 HC1 (4ΌΜ ’在—氧陸園中,3〇當量)。將所形成之溶液於室 下攪拌2小時。接著,以m Ν&amp;〇Η水溶液使反應淬滅,且 以醚萃取。然後’將合併之有機萃液以水與鹽水進一步洗 務,以Na2S〇4水乾燥,過渡,及使 濾液在真空47濃縮。 φ 粗產物經由急驟式層析之純化(Si02,4:1 (v/v)己烷:EtOAc— EtOAc),獲得標題化合物,為無色油。 胺78 N-[3-(3-甲氧基丙基)_5_甲芊基]環丙胺 步驟1 . (3-漬基_5-甲醯基苄基)環丙基胺基甲酸第三丁酯 在-ίο c下,於正_丁基鋰(2 5M,在己烷中,12當量)之甲 苯(〇.1M)溶液中,添加正-丁基溴化鎂(2.0M,在THF中,0.4 當罝)。將所形成之懸浮液於_1(rc下攪拌2〇分鐘,然後添加 • %丙基(3,4-二溴基苄基)胺基曱酸第三-丁酯(1當量,胺77步 驟2),使目前黃紅色懸浮液在〇β(:下攪拌3〇分鐘,接著於_78 C下逐滴添加純DMF (30當量)。使反應混合物慢慢地溫熱 至室溫,歷經3小時。以i〇% HC1水溶液使目前黑色懸浮液 泮滅’然後以醚萃取。將合併之有機萃液以水與鹽水進一 步洗條,以NadO4脫水乾燥,過濾,及使濾液在真空中濃 縮。粗產物經由急驟式層析之純化(Si〇2,己烷—1:1 (v/v)己 烧:EtOAc) ’獲得標題化合物,為金黃色油。 步驟2 :環丙基{3-曱醯基-5-[(1Ε)-3-曱氧基-1-丙烯小基]罕基} 143482-1 -135- 201111364 胺基曱酸第三-丁酯 於得自前一步驟之(3-溴基-5-曱醯基芊基)環丙基胺基甲 酸第三-丁醋(1當量)與4,4,5,5_四甲基_2_[(1E)各(甲氧基)小丙稀 -1-基]-1,3,2-二氧硼伍圜(1當量)在DMF (〇 2M)中之溶液内,添 加反式-雙(三苯膦)漠化鈀(ΙΙ)(α〇5當量”將容器重複抽氣, 且以氮逆充填。最後,添加2Μ NaaCO3水溶液(3當量),並 將所形成之混合物於90。(:下加熱6小時。使目前黑色懸浮液 冷卻至室溫,以水稀釋,且以醚萃取。將合併之有機萃液 以10% HC1水溶液、1N Na0H水溶液、水及鹽水進一步洗滌, 以NasSO4脫水乾燥’過濾,及使濾液在真空中濃縮。粗產 物經由急驟式層析之純化(Si〇2,己烷—3:7 (v/v)己烧: EtOAc) ’獲得標題化合物,為淡黃色油。 步驟3:環丙基[3-(3-曱氧基丙基)-5-曱苄基]胺基曱酸第三丁醋 使得自前一步驟之環丙基丨3-曱醯基-5-[(lE)-3-曱氧基_ι-丙 烯-1-基]字基}胺基曱酸第三-丁酯(1當量)與10% w/w鈀/炭 (〇.1當量)懸浮於EtOAc (0.1M)中。然後,將容器抽氣,並以 %膝氣。在經充填H2大氣之氣瓶下,將反應懸浮液於室溫 下攪拌3小時。接著,以二氣曱烷使反應懸浮液淬滅,且經 過矽藻土床過濾。濾液在真空中之濃縮,獲得標題化合物, 為黃色油。 步驟5 :胺78 於CH2C12(0.1M)中之得自前一步驟之環丙基[3(3曱氧基丙 基)-5-甲爷基]胺基甲酸第三-丁醋(1當量)内,添加Ηα (4 〇M, 在二氧陸圜中,30當量)。將所形成之溶液在室溫下攪拌2 143482-1 -136· 201111364 小時。接著,以INNaOH水溶液使反應淬滅,並以喊萃取。 然後,將合併之有機萃液以水與鹽水進一步洗滌,以 脫水乾燥,及過濾。濾液在真空中之濃縮,獲得標題化合 物,為無色油。 胺79 N-[2-溴基-3,5-雙(3-甲氧基丙基)苄基]環丙胺 步驟1 . 3,5-二溴-N-環丙基苯曱酸胺 於3,5-二溴苯曱酸(1當量)在DMF (0.15M)中之經攪拌溶液 内,添加HATU(1.3當量)、環丙基胺(u當量)&amp;Hunig氏鹼(3 當量)。將所形成之黃色混合物於室溫下攪拌18小時。然後, 以飽和氯化銨水溶液使反應淬滅,並以醋酸乙酯萃取。將 合併之有機萃液以水與鹽水進一步洗滌,以N&amp;2 s〇4脫水乾 燥,過濾,及使濾液在真空中濃縮。如此獲得之粗產物在 醚與己烷之混合物中之研製,獲得標題化合物,為白色固 體。 _ 步驟2 : N-環丙基-3,5_雙[(1Ε)-3-曱氧基丙-1-烯-μ基]苯曱醯胺 於得自前一步驟之3,5-二溴-Ν-環丙基苯曱醯胺(1當量)與 4,4,5,5-四曱基-2-[(1Ε)-3-(甲軋基)-1-丙稀小基]_ι,3,2_二氧硼伍圜 (2.3當量)在DMF (0.13Μ)中之溶液内,添加反式_雙(三苯膦) 溴化鈀(πχο.ι當量)。將容器重複抽氣,且以氮逆充填。最 後’添加2Μ NasCO3水溶液(6當量),並將所形成之混合物 於90°C下加熱16小時。使目前黑色懸浮液冷卻至室溫,以 水稀釋’且以醋酸乙醋萃取。將合併之有機萃液以IN NaOH 水溶液、10% HC1水溶液、水及鹽水進—步洗務,以Na2 s〇4 143482-1 -137- 201111364 脫水乾燥,及過濾 化合物’為黑色油 濾液在真空中之濃縮,獲得粗製標題 步驟3 : N-環丙基_3,5_雙(3_甲氧基丙基)苯甲醯胺 使得自前一步驟之N-環丙基_3 5_雙[⑽各甲氡基丙小炼小 基]苯曱醯胺(1當量)之EtOAc (0.15M)溶液經過裝有1〇%鈀/碳 藥筒之H-Cube氫化作用裝置,在!毫升/分鐘之速率下,以 EtOAc作為溶離劑進行溶離。氫化作用係在室溫下,使用全 氫設定進行。如此獲得之粗產物經由急驟式層析之純化 (Si〇2,9:1 (v/v)己烷:Et〇Ac~&gt;EtOAc),獲得標題化合物,為 無色油。 步驟4: 2-溴-Ν-環丙基-3,5-雙(3-曱氧基丙基)苯甲醯胺 在-78°C下,於得自前一步驟之Ν_環丙基_3 5_雙(3甲氧基丙 基)苯曱醯胺(1當量)與剛蒸餾TMEDA (1當量)之THF (0.1Μ) 溶液中’逐滴添加第三-丁基鋰(17Μ,在戊烷中,1當量), 歷經10分知。然後,將所形成之反應混合物慢慢地溫熱至〇 °c,歷經1小時,並於〇t下攪拌i小時。其中使目前橘色反 應溶液再冷卻至-78°c ’不含溶劑逐滴添加i,2-二溴基四氟基 乙院’歷經10分鐘。移除冷卻浴,且將反應混合物在室溫 下攪拌18小時。然後’以IN NaOH水溶液使反應淬滅,並以 EtOAc萃取。將合併之有機萃液以10% HC1水溶液、水及鹽 水進一步洗滌’以Naz S04脫水乾燥,過濾,及使濾液在真 空中濃縮。如此獲得之粗產物經由急驟式層析之純化(Si02, 9:1 (v/v)己烷:EtOAc— EtOAc) ’獲得標題化合物,為淡黃色 油0 143482-1 •138· 2011Π364 步驟5 :胺79 於得自前一步驟之2-溴-N-環丙基-3,5-雙(3-甲氧基丙基)苯 甲醯胺(1當量)在THF (0.16M)中之經攪拌溶液内,相繼地添 加硼氫化鈉(4當量)與bf^thf複合物(4 5當量)。將如此獲 得之反應溶液於40°C下加熱5小時,冷卻至〇。(:,然後慢慢 地倒入6N HC1水溶液(4.5當量)中◊將所形成之混合物於5〇 。(:下再加熱1小時,冷卻至室溫,以10N NaOH水溶液鹼化, 且最後以醚萃取。接著’將合併之有機萃液以水與鹽水進 籲一步洗滌,以NaeO4脫水乾燥,過濾,及使濾液在真空中 濃縮。如此獲得之粗產物經由急驟式層析之純化(Si〇2,4:1 (v/v)己烧:Et〇Ac-&gt; EtOAc),獲得標題化合物,為無色油。 胺80 N-[2-氣基-3,5-雙(3-曱氧基丙基)芊基μ裒丙胺 步驟1 : 2-氯-Ν-環丙基-3,5-雙(3-曱氧基丙基)笨曱醢胺 於2-溴-Ν-環丙基-3,5-雙(3-甲氧基丙基)苯甲醯胺Q當量,胺 φ 79步驟4)之DMF (〇.13Μ)溶液中,添加氣化銅φ (2當量)。將 此懸浮液密封’並在微波中,於BOt下加熱1〇分鐘。然後, 以10% HC1水溶液使反應淬滅,且以Et〇Ac萃取。將合併之 有機萃液以IN NaOH水溶液、水及鹽水進一步洗滌,以 NaaSO4脫水乾燥’過濾’及使濾液在真空中濃縮^如此獲 得之粗產物經由急驟式層析之純化(si〇2,4:1 (v/v)己烷: EtOAc— EtOAc),獲得標題化合物,為淡黃色油。 步驟2 :胺80 於得自前一步驟之2-氣-N-環丙基-3,5-雙(3-曱氧基丙基)笨 143482· 1 -139- 201111364 甲醯胺(1當量)在THF (0.06M)中之經攪拌溶液内,相繼地添 加硼氫化鈉(4.2當量)與BFg-THF複合物(45當量)^將如此獲 知之反應溶液於40 C下加熱5小時,冷卻至〇°C,然後慢慢 地倒入6N HC1水溶液(4.5當量)中。將所形成之混合物於5〇 C下再加熱1小時’冷卻至室溫’以1〇N Na〇H水溶液鹼化, 且最後以醚萃取。接著,將合併之有機萃液以水與鹽水進 一步洗滌,以Nas SO4脫水乾燥,過濾,及使濾液在真空中 濃縮。如此獲得之粗產物經由急驟式層析之純化(Si〇2,4:1 (v/v)己烷:EtOAc— EtOAc) ’獲得標題化合物,為無色油。 胺81 N-[2-曱氧基-3,5-雙(3-曱氧基丙基)爷基]環丙胺 步驟1 : 2-甲氧基-3,5-雙[(lE)-3-曱氧基丙小烯小基]苯甲醛 於3,5-二溴基-2-曱氧基苯甲醛(1當量)與4,4,5,5四曱基 -2-[(1Ε)-3-(曱氧基)-1-丙烯-1-基]_13 2_二氧硼伍圜2當量)在 DMF (0.1M)中之溶液内,添加反式_雙(三苯膦)漠化鈀⑼(〇] 當里)。將谷器重複抽氣,且以氮逆充填。最後,添加2M c〇3 水溶液(6.5當量),並將所形成之混合物於9〇χ:下加熱16小 時。使目則黑色懸浮液冷卻至室溫,以水稀釋,且以醚萃 取。將合併之有機萃液以INNaOH水溶液、1〇%HC1水溶液、 水及鹽水進一步洗滌,以N^SO4脫水乾燥,及過濾。濾液 在真空中之濃縮,獲得粗製標題化合物’為褐色油。 步驟2: 2-曱氧基-3,5-雙(3-甲氧基丙基)苯甲越 使%自刖一步驟之2-曱氧基_3,5-雙[(1Ey3_甲氧基丙小烯小 基]苯甲齡(1當1)與ίο% w/w I巴/炭(〇a當量)懸浮於Et〇Ac 143482-1 •140- 201111364 並以H2滌氣。在經充填% 室溫下授拌4小時。接著, (0.1M)中。然後,將容器抽氣, 大氣之氣瓶下,將反應懸浮液於 以二氣甲烧使反應懸浮液淬滅’且經過珍薄土床過減。據 液在真空中之濃縮’獲得粗產物,為黃色油。經由急驟式 層析之進—步純化(Si〇2,己^邮岭獲得標題化合物, 為無色油。 步驟3 :胺81 將得自前一步驟之2-甲氧基_3,5_雙(3_甲氧基丙基)苯甲醛 (1當量)與環丙基胺(2當量)合併於〇^〇2(〇1_中。然後, 於其中添加MgS〇4 (1.2當量),並將所形成之懸浮液在室溫下 攪拌20小時。然後,經由過濾,經過矽藻土墊移除不溶物, 及使;慮液在真空中浪縮。接著,使如此獲得之粗製亞胺再 溶於MeOH (0.1M)中。於此溶液中,分次添加硼氫化鈉(2當 量),並將所形成之混合物在室溫下攪拌2 5小時。以1Ν Ηα 水溶液使反應淬滅’以IN NaOH水溶液中和,且以醚萃取。 然後,將合併之有機萃液以水與鹽水進一步洗滌,以MgS〇4 脫水乾燥’及過濾。濾液在真空中之濃縮’獲得標題化合 物,為淡黃色油。 胺82 N-[3-(3-曱氧基丙基)-5-(三氟曱基)芊基]環丙胺 步驟1 : 3-演基-5-(三I甲基)苯曱酸 在-15°C下’於正-丁基鋰(2.5M,在己烷中’ 〇.8當量)在甲 苯(0.2M)中之經攪拌溶液内,逐滴添加正-丁基氯化鎂 (2.0M,在THF中’ 0.4當量)。於20分鐘後,添加1,3-二漠基-5-(三 143482-1 -141 - 201111364 氟曱基)苯(1當量)在曱苯中之溶液’歷經1〇分鐘。將如此獲 得之反應混合物在-15 C下攪拌2小時,然後添加DMF (3當 量)。使反應物溫熱至〇°C。於45分鐘後,添加飽和氣化銨 水溶液。將反應混合物以醋酸乙酯萃取。接著,將合併之 有機萃液以鹽水洗滌,以N^SO4脫水乾燥,過濾,及使濾 液在真空中濃縮。粗產物經由急驟式層析之純化(Si〇2,己 烷—1:1 (v/v)己烷:EtOAc),獲得標題化合物。 步驟2 : 3-[(1Ε)-3-曱氧基丙小烯小基]_5_(三氟甲基)苯曱醛 於得自刖一步驟之3-溴基-5-(三氟曱基)苯曱醛(1當量)與 4,4,5,5-四甲基-2-[(1Ε)-3-(甲氧基丙烯小基H,3,2二氧硼伍圜 (1.5當量)在DMF(0.2M)中之溶液内,添加反式雙(三苯鱗)漠 化鈀(11)(0.05當量)。將容器重複抽氣,並以氮逆充填。最後, 添加2M Na^O3水溶液(3當量),且將所形成之混合物於1〇〇 °C下搜拌2小時。使目前黑色懸浮液冷卻至室溫,以水稀釋, 並以醋酸乙酯萃取《將合併之有機萃液以水與鹽水洗滌, 以Na2S04脫水乾燥,過渡,及使遽液在真空中濃縮。粗產 物經由急驟式層析之純化(Si〇2,9:1 (v/v)己烷:Et〇Ac— EtOAc) ’獲得標題化合物,為黃色油。 步驟3 . Ν-[3-[(1Ε)-3-甲氧基丙4_烯小基]_5 (三敗曱基)爷基]環 丙胺 將得自前一步驟之3_[(1E)各甲氧基丙小烯小基]·5 (三氟甲 基)笨甲醛(1當S )與環丙基胺(2當量)合併於CH2Cl2(〇 2Μ)中 d後於其中添加MgS04 (1.5當量),並將所形成之懸浮液 在室溫下攪拌18小時。接著,經由過濾,經過矽藻土墊移 143482-] •142· 201111364 除不溶物,及使濾液在真空中濃縮。然後,使如此獲得之 粗製亞胺再溶於THF : MeOH之2:1 (Wv)混合物(〇 2M)中。於此 浴液中,分次添加硼氫化鈉當量),且將所形成之混合物 在室溫下攪拌18小時。以飽和碳酸氫鈉水溶液使反應淬滅, 並以醋酸乙酯萃取。接著,將合併之有機萃液以鹽水洗滌, 以NajO4脫水乾燥,過濾,及使濾液在真空中濃縮。粗產 物經由急驟式層析之純化(Si〇2,9:1 (v/v)己烷:Et0Ac— EtOAc),獲得標題化合物。 ®步驟5 :胺82 使得自前一步驟之Ν-[3-[(1Ε)-3-甲氧基丙-1_烯小基]„5_(三氟 甲基)下基]環丙胺(1當量)與1〇% w/w把/炭(〇 1當量)懸浮於 EtOAc (0.03M)中。然後,將容器抽氣,並以士滌氣。在經充 填H2大氣之氣瓶下,將反應懸浮液於室溫下攪拌過夜。接 著,使反應物經過矽藻土床過濾,及使濾液在真空中濃縮。 粗產物經由急驟式層析之純化(Si〇2,己烷—丨9 己烷: φ EtOAcO,獲得標題化合物,為無色油。 胺83 3-[(環丙胺基)曱基]_5_(3_甲氧基丙基)酚 胺83係根據已公告之專利申請案w〇 2〇〇7/⑽%邠中所 述之程序製成。 胺84 N-(3-溴基-5-碘基芊基)環丙胺 步驟1 : (3-溴基峨苯基)甲醇 在至μ下,於3-〉臭基_5_碘苯曱酸Q 〇當量)在THF (〇 2M)中 143482-1 • 143 - 201111364 之溶液内’添加蝴烧-硫化曱院複合物(1.5當量)。於室溫下 攪拌3天後’以2N HC1水溶液謹慎地使反應混合物淬滅,並 以醚萃取。將合併之有機萃液以1N NaOH水溶液、水及鹽水 洗)條’以MgS〇4脫水乾燥,及過渡。濾液在真空中之濃縮, 獲得標題化合物,為無色油。 步驟2 : 3-溴基-5-埃基苯甲醛 將得自前一步驟之(3-溴基-5-碘苯基)曱醇(ι·〇當量)與 Dess-Martin過蛾烷(1.18當量)之混合物在室溫下,於二氣曱烧 (0.1M)中攪拌45分鐘。將反應混合物以醚稀釋,經過Si〇2填 充柱過濾,並將矽膠以己烷:Et〇Ac之3:1 (v/v)混合物洗務。 使;慮液在真空中濃縮,且再一次通過Si〇2填充柱,以己烧: EtOAc之3:1 (v/v)混合物溶離’而得標題化合物,為淡黃色固 體。 步驟3 :胺84 將得自前一步驟之3-溴基_5-碘基苯甲醛(1當量)與環丙基 胺(2虽量)合併於CH2 (¾ (0.1M)中。然後,於其中添加MgS〇4 (j 當量),並將所形成之懸浮液在室溫下攪拌2〇小時。然後, 經由過濾,經過矽藻土墊移除不溶物,及使濾液在真空中 /辰縮。接著,使如此獲得之粗製亞胺再溶於Μ&amp;〇Η (〇 5M)中^ 於此溶液中,分次添加硼氫化鈉(l 5當量),並將所形成之 混合物在0C下攪拌30分鐘,然後於室溫下2小時。藉由與 2N HC1水,合液一起攪拌25分鐘而使反應淬滅,以Μ Na〇H水 /谷液驗化及在真空中濃縮。將殘留物自水以醚萃取,以 Na2S04脫水乾燥,過濾,並使濾液在真空中濃縮,而得標 143482-1 201111364 題化合物,為淡黃色油。 胺85 N-環丙基-6-(3-甲氧基丙基)氫茚小胺 步驟1 : 6-[(1E)-3-甲氧基丙-1-稀-1-基]氫茚-1-酮 於6-漠基氫茚小酮(1當量)與4,4,5,5_四曱基_2_[(1e)_3 (甲氧 基)-1-丙稀-1-基]-1,3,2-二氧硼伍圜(1.3當量)在DMF (0.1M)中之 溶液内’添加反式_雙(三苯膦)漠化鈀⑼(〇 〇5當量)。將容器 重複抽氣,並以氮逆充填。最後,添加2M Na2C〇3水溶液 當量),且將所形成之混合物於1〇crc下攪拌丨小時。使目前 黑色懸浮液冷卻至室溫’以水稀釋,及以醋酸乙酯萃取。 將合併之有機卒液以水與鹽水洗滌,以Na〗s〇4脫水乾燥, 過濾,及使濾液在真空中濃縮。粗產物經由急驟式層析之 純化(si〇2,己烷—1:1 (v/v)己烷:Et〇Ac),獲得標題化合物, 為米黃色固體。 步驟2 ·· N-環丙基各[(1E)各曱氧基丙小烯小基]氫茚小胺 於得自前一步驟之6-[(1E)各甲氧基丙·烯小基]氫茚小酮 (1 s里)在MeOH (2M)中之溶液内,'添加環丙基胺(2當量)與 異丙醇鈦(ιν)(ι·3當量)。將此溶液於室溫下攪拌1小時,然 後在〇°c下添加删氫化鈉(1當量)。於3〇分鐘後添加水, 並將混合物以醋酸乙酷萃取。接著,將合併之有機萃液以 水與鹽水《,以㈣抑脫水乾燥,過渡,及使濾液在真 空中濃縮。粗產物經由急驟式層析之純化⑽,己烷 (v/v)己烷:EtOAc),獲得標題化合物。 步驟3 :胺85 143482-1 -145· 201111364 使得自前一步驟之N-環丙基-6-[(1E)-3-甲氧基丙小烯基] 氫茚-1-胺(1當量)與10% w/w鈀/炭(〇.1當量)懸浮於Et〇Ac (0.2M)中。然後,將容器抽氣,並以%滌氣。在經充填咏大 氣之氣瓶下,將反應懸浮液於室溫下攪拌3小時。接著,使 反應物經過矽藻土床過濾’及使濾液在真空中濃縮,而得 標題化合物。 胺86 Ν-環丙基-7-(3-曱氧基丙基)-1,2,3,4-四氫茶-1-胺 胺86係根據胺85中所述之程序製成,但替代地使用7_漠 基-3,4-二氫莕·1(2Η)-酮作為起始物質。 胺87 3-{3·溴基-5-[(環丙胺基)曱基]-2-甲基笨基卜ι_丙醇 於胺76 (1當量)之氯仿(0.1Μ)溶液中,添加碘基三曱基石夕 烧(6當量)。將所形成之紅色溶液在室溫下,於黑暗中授掉 18小時。以甲醇使反應淬滅,然後在真空中移除揮發性物 質。接著,使所形成之殘留物於醚與10% HC1水溶液之間作 分液處理。分離水層,以IN NaOH水溶液小心地達到ρΗ值 為〜8,並以EtOAc萃取。將合併之EtOAc萃液以水與鹽水進 一步洗條,以Na〗S〇4脫水乾燥,過渡,及使漉液在真空中 濃縮。粗產物經由急驟式層析之純化⑸〇2,97:3 (v/v) CH2 α2 :The title compound was obtained as a pale yellow oil. Step 4: [3,5-bis(3-methoxypropyl); yl]cyclopropylamino decanoic acid tributyl hydrazine is made from the previous step of {3,5-bis[(1Ε)-3-曱oxy-1-propenyl-μ; aryl cyclopropylaminocarbamic acid tert-butyl ester (1 equivalent) and 10% w/w palladium on charcoal (〇1 equivalent) suspended in EtOAc (0.05 M) . Then, pump the container and call it a gas. The reaction suspension was stirred at room temperature for 3 hours under a cylinder filled with % atmosphere. The reaction suspension was then quenched with dichloromethane and filtered through a bed of celite. The filtrate was concentrated in vacuo to give the title compound. 143482-1 -134- 201111364 Step 5: Amine 77 from [3,5-bis(3-decyloxypropyl)hanyl]cyclopropyl-aminopyruic acid second-butyl ester (1 eq.) In a solution of CH2C12 (0.1 M), HCl (4 ΌΜ 'in-oxan, 3 〇 equivalent) was added. The resulting solution was stirred under the chamber for 2 hours. Next, the reaction was quenched with m Ν &amp; aqueous solution and extracted with ether. The combined organic extracts were then further washed with water and brine, dried over Na.sub.2.sub.4 water, and then filtered and concentrated. The crude product was purified by flash chromatography (EtOAc: EtOAc:EtOAc: Amine 78 N-[3-(3-methoxypropyl)_5-methylindenyl]cyclopropylamine Step 1. (3-Sodium _5-methylbenzylidene benzyl) cyclopropyl carbamic acid tert-butyl Add the n-butylmagnesium bromide (2.0 M in THF) to a solution of n-butyllithium (2 5 M in hexanes, 12 eq.) in toluene (1 M). , 0.4 when 罝). The resulting suspension was stirred at _1 (rc) for 2 min, then added • % propyl (3,4-dibromobenzyl)amine decanoic acid tert-butyl ester (1 equivalent, amine 77 steps) 2), the current yellow-red suspension was stirred under 〇β (: 3 〇, then pure DMF (30 eq.) was added dropwise at _78 C. The reaction mixture was slowly warmed to room temperature over 3 Hour. The current black suspension was quenched with aqueous solution of HCl and then extracted with ether. The combined organic extracts were further washed with water and brine, dried over NadO4, filtered and concentrated in vacuo. The crude product was purified by flash chromatography (EtOAc EtOAc (EtOAc) Mercapto-5-[(1Ε)-3-decyloxy-1-propenyl]-yl} 143482-1 -135- 201111364 Aminobutyric acid tert-butyl ester obtained from the previous step (3- Bromo-5-indenyl)cyclopropylaminocarbamic acid tert-butyl vinegar (1 equivalent) and 4,4,5,5-tetramethyl-2_[(1E) each (methoxy) Small propylene-1-yl]-1,3,2-dioxaboron (1 equivalent) in DMF ( In the solution in 〇2M), the trans-bis(triphenylphosphine) desertified palladium (ΙΙ) (α〇5 equivalent) was added to repeatedly evacuate the vessel, and the nitrogen was reversely packed. Finally, 2Μ NaaCO3 aqueous solution was added (3) Equivalent), and the resulting mixture was heated at 90 ° (.: 6 hours. The current black suspension was cooled to room temperature, diluted with water and extracted with ether. The combined organic extracts were taken in 10% aqueous HCl. 1N aqueous solution of Na0H, water and brine were further washed, dried over NasSO4, filtered, and the filtrate was concentrated in vacuo. The crude product was purified by flash chromatography (Si 2 , hexane - 3:7 (v/v) Ethyl alcohol: EtOAc) 'Yield of the title compound as a pale yellow oil. Step 3: </RTI> </RTI> <RTIgt; </RTI> </RTI> </RTI> <RTIgt; One step of cyclopropyl hydrazino 3-mercapto-5-[(lE)-3-decyloxy_ι-propen-1-yl]-yl}amino decanoic acid tert-butyl ester (1 equivalent) Suspended in 10% w/w palladium on charcoal (〇.1 eq.) in EtOAc (0.1 M). Then, the vessel was evacuated and ventilated in %. The reaction was suspended in a gas cylinder filled with H2 atmosphere. Stirring at room temperature After 3 hours, the reaction suspension was quenched with dioxane and filtered over a pad of celite. The filtrate was concentrated in vacuo to give the title compound as yellow oil. Step 5:amine 78 in CH2C12 (0.1M环α (4 〇M, in the cyclopropyl [3(3 methoxypropyl)-5-methyl-yl] carbamic acid tri-butyl vinegar (1 eq.) obtained from the previous step In the dioxane, 30 equivalents). The resulting solution was stirred at room temperature for 2 143482-1 -136·201111364 hours. Next, the reaction was quenched with a 1 N aqueous solution of NaOH and extracted with a mixture. The combined organic extracts were then further washed with water and brine, dried with dehydration, and filtered. The filtrate was concentrated in vacuo to give the title compound. Amine 79 N-[2-bromo-3,5-bis(3-methoxypropyl)benzyl]cyclopropylamine Step 1. 3,5-Dibromo-N-cyclopropylbenzoic acid amine in 3 To a stirred solution of 5-dibromobenzoic acid (1 eq.) in DMF (0.15 M), HATU (1.3 eq.), cyclopropylamine (u eq.) &amp;Hunig's base (3 eq.). The resulting yellow mixture was stirred at room temperature for 18 hours. Then, the reaction was quenched with saturated aqueous ammonium chloride and extracted with ethyl acetate. The combined organic extracts were further washed with water and brine, dried and dried with N &amp; The crude product thus obtained was triturated in a mixture of ether and hexane to give the title compound as white solid. _ Step 2: N-cyclopropyl-3,5-bis[(1Ε)-3-decyloxyprop-1-en-yl]benzamide in 3,5-dibromo obtained from the previous step - Ν-cyclopropyl benzoguanamine (1 equivalent) and 4,4,5,5-tetradecyl-2-[(1Ε)-3-(methyl-rollyl)-1-propanyl]- 3,2-dioxaboron (2.3 eq.) In a solution of DMF (0.13 Torr), trans-bis(triphenylphosphine)palladium bromide (πχο.ι equivalent) was added. The vessel was repeatedly evacuated and counter-filled with nitrogen. Finally, 2 Μ aqueous NasCO 3 (6 equivalents) was added, and the resulting mixture was heated at 90 ° C for 16 hours. The current black suspension was allowed to cool to room temperature, diluted with water and extracted with ethyl acetate. The combined organic extracts were washed with IN NaOH aqueous solution, 10% aqueous HCl solution, water and brine, dried over Na 2 s 〇 4 143482-1 -137- 201111364, and filtered as 'black oil filtrate in vacuum Concentration in the middle to obtain the crude title step 3: N-cyclopropyl_3,5-bis(3-methoxypropyl)benzamide from the previous step of N-cyclopropyl_3 5_double [ (10) Each of the thioglycolate (1 eq.) EtOAc (0.15 M) solution was passed through a H-Cube hydrogenation apparatus equipped with a 1% palladium/carbon cartridge. The solution was eluted with EtOAc as a dissolving agent at a rate of cc/min. The hydrogenation was carried out at room temperature using a hydrogenation setting. The crude product thus obtained was purified by flash chromatography eluting elut elut elut elut elut Step 4: 2-Bromo-indole-cyclopropyl-3,5-bis(3-decyloxypropyl)benzamide at -78 ° C in the previous step from Ν_cyclopropyl_ 3 5_bis(3methoxypropyl)phenyl hydrazide (1 eq.) with a freshly distilled TMEDA (1 eq.) in THF (0.1 Μ) solution, 'DTH-butyllithium was added dropwise (17 Μ, at In pentane, 1 equivalent), after 10 minutes. The resulting reaction mixture was then slowly warmed to 〇 °c over 1 hour and stirred at 〇t for 1 hour. Here, the current orange reaction solution was again cooled to -78 ° C ', and the i,2-dibromotetrafluoro phenyl group was added dropwise without solvent for 10 minutes. The cooling bath was removed and the reaction mixture was stirred at room temperature for 18 h. The reaction was then quenched with aqueous EtOAc (EtOAc)EtOAc. The combined organic extracts were further washed with a 10% aqueous HCl solution, water and brine, dried over Naz S04, filtered and concentrated in vacuo. The crude product thus obtained was purified by flash chromatography (EtOAc, EtOAc (EtOAc): EtOAc (EtOAc) Amine 79 was stirred from the previous step in 2-bromo-N-cyclopropyl-3,5-bis(3-methoxypropyl)benzamide (1 eq.) in THF (0.16M) Sodium borohydride (4 equivalents) and bf^thf complex (45 equivalents) were successively added to the solution. The reaction solution thus obtained was heated at 40 ° C for 5 hours and cooled to hydrazine. (:, then slowly pour into a 6N HCl solution (4.5 eq.) and pour the resulting mixture at 5 Torr. (: further heat for 1 hour, cool to room temperature, basify with 10 N aqueous NaOH, and finally Ether extraction. Then the combined organic extracts were washed with water and brine, dried over NaeO4, filtered, and the filtrate was concentrated in vacuo. The crude product thus obtained was purified by flash chromatography (Si. 2,4:1 (v/v) hexanes: Et.Ac-&gt; EtOAc. Propyl) mercapto-pyridylamine step 1: 2-chloro-indole-cyclopropyl-3,5-bis(3-decyloxypropyl) azelaamine in 2-bromo-indole-cyclopropyl -3,5-bis(3-methoxypropyl)benzamide Q equivalent, amine φ 79 Step 4) in DMF (〇.13Μ) solution, adding vaporized copper φ (2 equivalents). The suspension was sealed and heated in a microwave at BOt for 1 Torr. Then, the reaction was quenched with 10% aqueous HCl solution and extracted with Et.sub.Ac. The combined organic extracts were taken from aqueous solution of IN NaOH, water and brine. Further washing, taking NaaSO4 off The title compound was obtained by EtOAc (EtOAc) elute It is a light yellow oil. Step 2: Amine 80 is obtained from the previous step of 2-gas-N-cyclopropyl-3,5-bis(3-methoxypropyl) stupid 143482·1 -139- 201111364 formazan A solution of the amine (1 equivalent) in THF (0.06 M) in a stirred solution, sodium borohydride (4.2 eq.) and BFg-THF complex (45 eq.) were added sequentially. The reaction solution thus obtained was heated at 40 C. After 5 hours, cool to 〇 ° C, then slowly pour into a 6 N aqueous HCl solution (4.5 eq.). The resulting mixture was heated at 5 ° C for an additional 1 hour 'cooling to room temperature' at 1 〇N Na〇 The H aqueous solution is basified and finally extracted with ether. The combined organic extracts are further washed with water and brine, dried over NasSO4, filtered, and the filtrate is concentrated in vacuo. Purification by chromatography (Si2, 4:1 (v/v) hexanes:EtOAcEtOAcEtOAc 81 N-[2-decyloxy-3,5-bis(3-decyloxypropyl) aryl]cyclopropylamine Step 1: 2-methoxy-3,5-bis[(lE)-3-曱oxypropene small base] benzaldehyde to 3,5-dibromo-2-indolylbenzaldehyde (1 equivalent) and 4,4,5,5 tetradecyl-2-[(1Ε)- 3-(decyloxy)-1-propen-1-yl]_13 2_dioxaboron 2 equivalents) in a solution in DMF (0.1M), adding trans-bis(triphenylphosphine) desertification Palladium (9) (〇) when). The trough was repeatedly evacuated and counter-filled with nitrogen. Finally, 2 M c 3 aqueous solution (6.5 eq.) was added, and the resulting mixture was heated at 9 Torr: for 16 hours. The desired black suspension was cooled to room temperature, diluted with water and extracted with ether. The combined organic extracts were further washed with aqueous 1 N NaOH, 1% aqueous HCl solution, water and brine, dried over N?SO? The filtrate was concentrated in vacuo to give crude title compound <RTI ID=0.0> Step 2: 2-Methoxy-3,5-bis(3-methoxypropyl)benzene is added to the 2-methoxy group of 3,5-bis[(1Ey3_methoxy) Propylene small base] benzoate (1 when 1) and ίο% w/w I bar / charcoal (〇a equivalent) suspended in Et〇Ac 143482-1 • 140- 201111364 and scrubbed with H2. Filling % The mixture was stirred for 4 hours at room temperature. Then, (0.1M). Then, the vessel was evacuated, and the reaction suspension was quenched with a second gas to make the reaction suspension quenched under the atmosphere of a gas cylinder. The rare soil bed was depleted. The crude product was obtained as a coloured oil (yield: EtOAc). Step 3: Amine 81 Combine 2-methoxy-3,5-bis(3-methoxypropyl)benzaldehyde (1 equivalent) from the previous step with cyclopropylamine (2 equivalents) in 〇^ 〇2 (〇1_. Then, MgS〇4 (1.2 eq.) was added thereto, and the resulting suspension was stirred at room temperature for 20 hours. Then, through filtration, the insoluble matter was removed through a diatomaceous earth pad. And let the liquid shrink in a vacuum. Then, make The crude imine thus obtained was redissolved in MeOH (0.1 M). To this was added sodium borohydride (2 eq.), and the mixture was stirred at room temperature for 25 hr. The aqueous solution quenched the reaction and was neutralized with aq. NaOH aqueous solution and extracted with ether. The combined organic extracts were further washed with water and brine, dried and dried with &lt;RTI ID=0.0&gt; The title compound is obtained as a light yellow oil.amine 82 N-[3-(3-decyloxypropyl)-5-(trifluoromethyl)indolyl]cyclopropylamine Step 1 : 3-Amino-5-( Tri-Imethyl)benzoic acid at -15 ° C in a stirred solution of n-butyllithium (2.5 M in hexanes '8 eq.) in toluene (0.2 M) Add n-butylmagnesium chloride (2.0 M, '0.4 equivalents in THF). After 20 minutes, add 1,3-di-mial-5-(three 143482-1 -141 - 201111364 fluoroindolyl)benzene (1 Equivalent) solution in toluene was carried out for 1 minute. The reaction mixture thus obtained was stirred at -15 C for 2 hours then DMF (3 eq.) was added. The reaction was allowed to warm to 〇 ° C. After the addition, a saturated aqueous solution of ammonium sulphate was added, and the mixture was extracted with ethyl acetate. The combined organic extracts were washed with brine, dried with N?SO?, filtered, and concentrated. Purification by flash chromatography (Si 2 , hexanes 1:1 (v/v) hexanes:EtOAc) Olefinyl]_5_(trifluoromethyl)benzofural in 3-bromo-5-(trifluoromethyl)benzaldehyde (1 equivalent) and 4,4,5,5- Tetramethyl-2-[(1Ε)-3-(methoxypropenyl H,3,2 dioxaboron (1.5 eq.) in DMF (0.2 M) solution, add trans bis ( Triphenyl scales are desertified palladium (11) (0.05 equivalents). The vessel was repeatedly evacuated and counter-filled with nitrogen. Finally, 2 M aqueous Na^O3 (3 eq.) was added, and the resulting mixture was stirred at 1 ° C for 2 hours. The current black suspension was cooled to room temperature, diluted with water and extracted with ethyl acetate. The combined organic extracts were washed with water and brine, dried with Na2SO4, and then evaporated and evaporated. The crude product was purified by flash chromatography eluting elut elut elut elut elut Step 3. Ν-[3-[(1Ε)-3-methoxypropan-4-ene small group]_5 (tris-decyl) yl) propylamine will be obtained from the previous step of 3_[(1E) each Addition of MgS04 (1.5 equivalents) to oxypropione small group]·5 (trifluoromethyl)benzaldehyde (1 when S) and cyclopropylamine (2 equivalents) in CH2Cl2 (〇2Μ) The resulting suspension was stirred at room temperature for 18 hours. Then, through filtration, the insoluble matter was removed by diatomaceous earth pad 143482-] • 142·201111364, and the filtrate was concentrated in a vacuum. The crude imine thus obtained was then redissolved in a 2:1 (Wv) mixture of THF:MeOH (〇 2M). To the bath, sodium borohydride equivalent was added in portions, and the resulting mixture was stirred at room temperature for 18 hr. The reaction was quenched with saturated aqueous sodium bicarbonate and extracted with ethyl acetate. Then, the combined organic extracts were washed with brine, dried over Naj.sub.4, filtered, and concentrated. The crude product was purified by flash chromatography eluting elut elut elut elut elut ® Step 5: Amine 82 is obtained from the previous step - [3-[(1Ε)-3-methoxyprop-1-1-ene small group] „5_(trifluoromethyl) yl]cyclopropylamine (1 equivalent And suspending / charcoal (〇1 equivalent) in EtOAc (0.03 M) with 1% w/w. Then, the vessel was evacuated and scrubbed with a gas. The reaction was carried out under a gas cylinder filled with H2 atmosphere. The suspension was stirred overnight at room temperature. The reaction was then filtered through a pad of Celite, and the filtrate was concentrated in vacuo. The crude product was purified by flash chromatography (Si2, hexane-hexane 9 hexane : φ EtOAcO, the title compound is obtained as a colorless oil. Amine 83 3-[(cyclopropylamino)indolyl]_5_(3-methoxypropyl)phenolamine 83 is based on the published patent application w〇2〇 Prepared by the procedure described in 〇7/(10)%邠. Amine 84 N-(3-Bromo-5-iodohydrazinyl)cyclopropylamine Step 1: (3-Bromophenylphenyl)methanol to μ , in the solution of 3->Smelly _5_iodobenzoic acid Q 〇 equivalent) in THF (〇2M) 143482-1 • 143 - 201111364 'Adding a simmer-sulfurized broth compound (1.5 eq.). After stirring at room temperature for 3 days, 'carefully use 2N HCl solution The reaction mixture was quenched and extracted with EtOAc EtOAc (EtOAc m. Colorless oil. Step 2: 3-Bromo-5-E-benzaldehyde will be obtained from the previous step (3-bromo-5-iodophenyl)nonanol (I··e equivalent) and Dess-Martin peremoline A mixture of (1.18 eq.) was stirred at room temperature for 45 minutes in dioxane (0.1 M). The reaction mixture was diluted with ether, filtered over a pad of EtOAc, and EtOAc: 3:1 (v/v) mixture was washed. The solution was concentrated in vacuo, and the column was again filled with Si〇2, and hexanes: 3:1 (v/v) mixture of EtOAc was dissolved. The title compound is obtained as a pale yellow solid. Step 3:amine 84 3-bromo-5-iodobenzaldehyde (1 eq.) from the previous step and cyclopropylamine (2) combined with CH2 (3⁄4) (0.1 M). Then, MgS〇4 (j equivalent) was added thereto, and the resulting suspension was stirred at room temperature for 2 hours. Then, through filtration, passed through The algae pad removes the insoluble matter, and the filtrate is vacuumed/shrinked. Then, the crude imine thus obtained is redissolved in hydrazine &amp; 〇Η (〇5M) in this solution, and hydroboration is added in portions. Sodium (15 equivalents), and the resulting mixture was stirred at 0 C for 30 minutes and then at room temperature for 2 hours. The reaction was quenched by stirring with 2N HCl water and stirring for 25 minutes. 〇H water / gluten liquid was tested and concentrated in vacuum. The residue was extracted with water from EtOAc (EtOAc)EtOAc. Amine 85 N-cyclopropyl-6-(3-methoxypropyl)hydroquinone small amine Step 1: 6-[(1E)-3-methoxyprop-1--1-yl-1-hydroquinone 1- Ketone in 6-Moalhydroquinone ketone (1 equivalent) and 4,4,5,5-tetradecyl_2_[(1e)_3 (methoxy)-1-propan-1-yl ]-1,3,2-Dioxaboron (1.3 eq.) in a solution in DMF (0.1 M) was added 'trans-bis(triphenylphosphine) desertified palladium (9) (〇〇5 equivalent). The vessel was repeatedly evacuated and counter-filled with nitrogen. Finally, 2 M Na 2 C 〇 3 aqueous solution equivalent) was added, and the resulting mixture was stirred at 1 〇 crc for 丨 hr. The current black suspension was allowed to cool to room temperature&apos; diluted with water and extracted with ethyl acetate. The combined organic strokes were washed with water and brine, dried over Na s s 4, filtered, and concentrated. The crude product was purified by EtOAc EtOAcjjjj: Step 2 · N-cyclopropyl each [(1E) decyloxypropenyl small group] hydroquinone small amine in the previous step 6-[(1E) each methoxypropenyl small group] In a solution of hydroquinone ketone (1 s) in MeOH (2M), &lt;RTI ID=0.0&gt;&gt; This solution was stirred at room temperature for 1 hour, then sodium hydride (1 eq.) was added at EtOAc. Water was added after 3 minutes and the mixture was extracted with ethyl acetate. Next, the combined organic extracts were washed with water and brine, dehydrated and dried, and the filtrate was concentrated in the air. The crude product was purified by EtOAc (EtOAc) Step 3: Amine 85 143482-1 -145· 201111364 N-cyclopropyl-6-[(1E)-3-methoxypropenyl]hydroquinone-1-amine (1 equivalent) from the previous step It was suspended in Et 〇Ac (0.2 M) with 10% w/w palladium on charcoal (〇.1 eq.). The container is then evacuated and scrubbed in %. The reaction suspension was stirred at room temperature for 3 hours under a gas cylinder filled with helium. Next, the reaction was filtered through a pad of Celite, and the filtrate was concentrated in vacuo to give the title compound. Amine 86 Ν-cyclopropyl-7-(3-decyloxypropyl)-1,2,3,4-tetrahydrocha-1-amineamine 86 was prepared according to the procedure described for amine 85, but Instead of 7-glycine-3,4-dihydroindole·1(2Η)-one, a starting material is used. Amine 87 3-{3·bromo-5-[(cyclopropylamino)indolyl]-2-methylindolyl i-propanol is added to a solution of amine 76 (1 eq.) in chloroform (0.1 Μ) Iodo-trimethyl sulphate (6 equivalents). The resulting red solution was allowed to stand in the dark for 18 hours at room temperature. The reaction was quenched with methanol and the volatiles were removed in vacuo. Next, the resulting residue was subjected to liquid separation between ether and a 10% aqueous HCl solution. The aqueous layer was separated and aq. The combined EtOAc extracts were further washed with water and brine, dried over Na.sub.4, and then evaporated and evaporated. Purification of the crude product by flash chromatography (5) 〇2,97:3 (v/v) CH2 α2 :

在 MeOH 中之 2.0M NH3—94:6 (Wv) CH2C12 :在 MeOH 中之 2.0M NHS) ’獲得標題化合物,為無色油。 胺88 N-[3-、;臭基-5-(3-乙氧基丙基)-4-曱苄基]環丙胺 143482-1 -146- 201111364 步驟1’ 3-溴基氧基+丙烯小基]_4_f基苯甲酸甲酯 於3’5-—漠基-4-甲基苯甲酸甲酯(1當量)與4,4,5,5四甲基 2 [(1Ε) 3_(Τ氧基)-1_丙烯-1-基]-1,3,2-二氧硼伍圜(1.1當量)在 DMF (0.1M)中之溶液内,添加反式雙(三苯膦)漠化鈀⑼(〇 〇2 當罝)。將容器重複抽氣’並以氮逆充填。最後,添加2M Na2c〇3 水溶液(3當量)’且將所形成之混合物於1〇〇&lt;t下加熱2小時。 使目前黑色懸浮液冷卻至室s,以水豨釋,並以醚萃取。 將合併之有機萃液以水與鹽水進一步洗滌,以脫水 乾燥過濾,及使濾液在真空中濃縮。粗產物經由急驟式 層析之,,、屯化(Si02,9:1 (v/v)己炫:EtOAc~M:l (v/v)己烧:EtOAc) ’獲得標題化合物,為無色油。 步驟2 · 3-溴基-5-(3-甲氧基丙基甲基苯甲酸甲酯 於得自前一步驟之3-溴基-5-[(ιΕ)_3·甲氧基小丙烯_丨基]_4_ 甲基苯曱酸甲s旨(1當量)之二氯曱烧(α2Μ)溶液中,添加The title compound was obtained as a colorless oil (yield: 2.0M NH3 - 94: 6 (Wv) CH2C12: Amine 88 N-[3-,; odoryl-5-(3-ethoxypropyl)-4-hydrazinobenzyl]cyclopropylamine 143482-1 -146- 201111364 Step 1' 3-Bromooxy+propene Methyl]_4_f-based benzoic acid methyl ester in methyl 3'5------- 4-methylbenzoate (1 equivalent) and 4,4,5,5-tetramethyl 2 [(1Ε) 3_(Τ? Addition of trans-bis(triphenylphosphine) desertified palladium in a solution of DMF (0.1 M) in a solution of -1 -propen-1-yl]-1,3,2-dioxaborin (1.1 eq.) (9) (〇〇2 when 罝). The vessel was repeatedly evacuated&apos; and backfilled with nitrogen. Finally, 2M Na2c〇3 aqueous solution (3 equivalents) was added and the resulting mixture was heated at 1 Torr &lt;t&gt; for 2 hours. The current black suspension was allowed to cool to chamber s, released with water and extracted with ether. The combined organic extracts were further washed with water and brine, dried over Celite, and concentrated. The title compound was obtained as a colorless oil. EtOAc (EtOAc: EtOAc: EtOAc (EtOAc) . Step 2 · 3-Bromo-5-(3-methoxypropylmethylbenzoic acid methyl ester in 3-bromo-5-[(ιΕ)_3·methoxy propylene 丨 得 from the previous step Base]_4_methylbenzoic acid methyl s (1 equivalent) in dichlorohydrazine (α2Μ) solution, added

Crabtree氏觸媒(〇.〇丨當量)。使所形成之橘紅色溶液以氫起泡 分鐘’以活化觸媒’然後於室溫下,在氫之靜態氣瓶大 氣下授拌3小時。最後’於真空中移除揮發性物質,獲得粗 製標題化合物,為黃色油。 步驟3 : 3-溴基-5-(3-埃基丙基)·4-曱基苯曱酸甲酯 於得自前一步驟之3-溴基-5-(3_曱氧基丙基)斗曱基笨曱酸 甲酷α當量)之氣仿(cum)溶液中,添加碘基三甲基石夕烷(ι〇 當量)。將所形成之紅色溶液在室溫下,於黑暗中攪拌以 小時。以甲醇使反應淬滅,然後在真空中移除揮發性物質。 接著,使所形成之殘留物溶於醚中,以1〇%Ηα水溶液、'w 143482-1 -147· 201111364Crabtree's catalyst (〇.〇丨 equivalent). The resulting orange-red solution was bubbled with hydrogen for a few minutes to activate the catalyst and then allowed to mix for 3 hours at room temperature under a static hydrogen cylinder. Finally, the volatile material was removed in vacuo to give the crude title compound as a yellow oil. Step 3: Methyl 3-bromo-5-(3-Ethylpropyl) 4-mercaptobenzoate in 3-bromo-5-(3-methoxypropyl) from the previous step In the gas-like (cum) solution of the cockroach base, the iodine trimethyl oxalate (methane equivalent) is added. The resulting red solution was stirred at room temperature for one hour in the dark. The reaction was quenched with methanol and the volatiles were removed in vacuo. Next, the formed residue is dissolved in ether to a 1%% Ηα aqueous solution, 'w 143482-1 -147· 201111364

NaOH水冷液、水及鹽水相繼洗》條以Ν^〇4脫水乾燥,過 濾’及使濾液在真空中濃縮。粗產物經由急驟式層析之純 化(Si02,己烷—3:7 (v/v)己烷:Et〇Ac),獲得標題化合物, 為橘色油。 步驟4 . 3-溴基-5-(3·乙氧基丙基)冰甲基苯甲酸乙酯 於付自前一步驟之3-溴基-5-(3-碘基丙基)_4-甲基苯曱酸曱 酯(1當量)之乙醇(0.1Μ)溶液中,添加剛製成之乙醇鈉(3當 畺)。將所形成之溶液於回流下加熱18小時。於冷卻至室溫 後,在真空中移除揮發性物質。然後,使所形成之殘留物 溶於醚中,並以10% HC1水溶液、IN Na〇H水溶液、水及鹽 水進一步洗滌,以Nas SO#脫水乾燥,過濾,且使濾液在真 空中濃縮。粗產物經由急驟式層析之純化(si〇2,己烷—1:1 (v/v)己烷:EtOAc) ’獲得標題化合物,為黃色油。 步驟5 : 3-溴基-5-(3-乙氧基丙基)-4-曱基苯甲醛 於得自前一步驟之3-溴基-5-(3-乙氧基丙基)_4_甲基苯曱酸 乙酯(1當量)之二氣甲烷(0.07M)溶液中,添加DIBAL-H (在甲 苯中之1.5M溶液’ 2.2當量)。將所形成之溶液在室溫下攪拌 1.5小時’然後以1〇% hci水溶液小心地使反應泮滅。分離水 層’並以醚逆萃取。將合併之有機萃液以鹽水進一步洗滌, 以NaaSO4脫水乾燥,過濾,及使濾液在真空中濃縮。使如 此獲得之粗製醇再一次溶於二氣曱烷(0.07M)中,接著添加 Dess-Martin過碘烷(1.〇當量)與碳酸氫鈉(1.2當量)。在室溫下 攪拌40分鐘後,將反應混合物以醚稀釋,且以飽和NaHS03 水溶液、IN NaOH水溶液、水及鹽水相繼洗滌。使有機萃液 143482-1 -148- 201111364 以Na2S〇4脫水乾燥,過濾,及使濾液在真空中濃縮。粗產 物經由急驟式層析之純化(Si〇2,己烧-ι:ι (v/v)己烧: EtOAc) ’獲得標題化合物,為無色油。 步驟6 :胺88 將得自前一步驟之3-溴基-5-(3-乙氧基丙基)-4-曱基苯曱酸 (1當量)與環丙基胺(2當量)合併於CH2C12(0.1M)中。然後, 於其中添加MgS〇4(l當量),並將所形成之懸浮液在室溫下The NaOH water-cooled liquid, water and brine were successively washed and dried by dehydration, filtered, and the filtrate was concentrated in vacuo. The crude product was purified by EtOAc EtOAc (EtOAc) Step 4. 3-Bromo-5-(3.ethoxypropyl)ethylidene benzoate in 3-bromo-5-(3-iodopropyl)-4-yl from the previous step To a solution of decyl phthalate (1 equivalent) in ethanol (0.1 Torr), freshly prepared sodium ethoxide (3 畺) was added. The resulting solution was heated under reflux for 18 hours. After cooling to room temperature, the volatiles were removed in vacuo. Then, the resulting residue was dissolved in ether and further washed with a 10% aqueous HCl solution, aqueous solution of &lt;RTI ID=0.0&gt;&gt; The crude product was purified by flash chromatography eluting elut elut elut elut Step 5: 3-Bromo-5-(3-ethoxypropyl)-4-mercaptobenzaldehyde in 3-bromo-5-(3-ethoxypropyl)_4_ from the previous step To a solution of ethyl methyl benzoate (1 eq.) in dioxane methane (0.07 M), DIBAL-H (1.5 M solution in toluene &lt; The resulting solution was stirred at room temperature for 1.5 hours. Then the reaction was carefully quenched with a 1% aqueous solution of HCI. The aqueous layer was separated&apos; and back extracted with ether. The combined organic extracts were further washed with brine, dried over Na Na. The crude alcohol thus obtained was once again dissolved in dioxane (0.07 M), followed by addition of Dess-Martin periodinane (1. dec.) and sodium hydrogencarbonate (1.2 eq.). After stirring at room temperature for 40 minutes, the reaction mixture was diluted with ether and washed sequentially with saturated aqueous NaH.sub.3, aqueous EtOAc, water and brine. The organic extract 143402-1 -148- 201111364 was dried over Na2S〇4, filtered, and the filtrate was concentrated in vacuo. The crude product was purified by flash chromatography eluting elut elut elut elut Step 6: Amine 88 combines 3-bromo-5-(3-ethoxypropyl)-4-mercaptobenzoic acid (1 eq.) from the previous step with cyclopropylamine (2 eq.) CH2C12 (0.1M). Then, MgS〇4 (1 equivalent) was added thereto, and the resulting suspension was allowed to stand at room temperature.

攪拌20小時。然後’經由過濾,經過矽藻土墊移除不溶物, 及使濾液在真空中濃縮。接著,使如此獲得之粗製亞胺再 溶於MeOH (0.5M)中。於此溶液中,分次添加硼氫化鈉(1 5 當量),並將所形成之混合物在〇充下攪拌3〇分鐘,然後於 室溫下2小時。藉由與2N Ηα水溶液一起攪拌25分鐘而使反 應淬滅,以INNaOH水溶液鹼化,及在真空中濃縮。將殘留 物自水以醚萃取,以NASA脫水乾燥,過濾,並使濾液在 真二中辰縮,而得標題化合物,為無色油。 胺89 N-{3-/臭基-5-[3-(二氟曱氧基)丙基]_4•曱苄基丨環丙胺 步驟1 : 3-溴基-5-(3-羥丙基)_4_甲基苯甲酸曱酯 於3-溴基-5-(3-甲氧基丙基)_4_曱基苯曱酸甲酯。當量,胺 ,步驟2)之氯仿(0.1M)溶液中1加碘基三甲基;烷。當 量)。將所形成之紅色溶液在室溫下,於黑暗中_18小時。 以曱醇使反應淬滅’然後於真空中移除揮發性物質。接著, 使所形成之殘留物溶於鍵中,以跳m水溶液、則㈣ 水溶液、水及鹽水相繼洗滌’以〜〇4脫水乾燥,過濾, 143482-1 • 149- 201111364 及使濾液在真空中濃縮。粗產物經由急驟式層析之純化 (Μ ’己烷〜3:7 (v/v)己烷:Et〇Ac),獲得標題化合物為 淡黃色油。 ’ 步驟2 . 3_/臭基'5_[3仁敗曱氧基)丙基M-曱基笨甲酸甲醋 在5〇°C下,於得自前一步驟之3-溴基-5-(3-羥丙基)_4_曱基苯 曱酸曱醋(1當量)與硫酸鈉(〇 2 #量)之乙腈(〇綱懸浮液 中,逐滴添加二氟(氟基磺醯基)醋酸(1當量),歷經10分鐘 期間。在添加完成後,將反應懸浮液於5〇〇(:下再加熱比小 時。然後,使反應混合物冷卻至室溫,倒入水中,且以醚 萃取。將合併之有機萃液以水與鹽水進一步洗滌,以Na2s〇4 脫水乾燥,過濾,及使濾液在真空中濃縮。粗產物經由急 驟式層析之純化(Si〇2 ’己烷—1:1 (v/v)己烷:Et〇Ac),獲得 標題化合物,為無色油。 步驟3 : 3-溴基-5-[3-(二氟甲氧基)丙基]-4-曱基苯曱醛 於得自前一步驟之3-溴基-5-[3-(二氟曱氧基)丙基]_4_曱基 苯曱酸曱酯(1當量)之二氣曱烷(0.07M)溶液中,添加DIBAL-H (在甲苯中之1.5M溶液,2.2當量)。將所形成之溶液在室溫 下攪拌1.5小時,然後以10% HC1水溶液小心地使反應淬滅。 分離水層’並以醚逆萃取。將合併之有機萃液以鹽水進一 步洗滌,以Na2S04脫水乾燥,過濾,及使濾液在真空中濃 縮。使如此獲得之粗製醇再一次溶於二氣曱烷(0.07M)中, 接著添加Dess-Martin過碘烷(1.0當量)與碳酸氫鈉(1.2當量)。 在室溫下攪拌40分鐘後,將反應混合物以醚稀釋,並以飽 和NaHS03水溶液、IN NaOH水溶液、水及鹽水相繼洗滌。使 143482-1 •150· 201111364 有機萃液以NaaSO4脫水乾燥,過濾,及使濾液在真空中濃 縮。粗產物經由急驟式層析之純化(Si〇2,己烷—1:1 (v/v)己 烧:EtOAc),獲得標題化合物,為無色油。 步驟6 :胺89 將得自前一步驟之3-溴基_5_[3_(二氟曱氧基)丙基]_4_甲基 笨曱醛(1當量)與環丙基胺(2當量)合併於Ch2 (〇 1M)中。 然後,於其中添加MgS〇4 (1當量),並將所形成之懸浮液在 室溫下攪拌20小時。接著,經由過濾,經過矽藻土墊移除 不溶物,及使濾液在真空中濃縮。然後,使如此獲得之粗 製亞胺再溶於MeOH (0.5M)中。於此溶液中,分次添加硼氫 化鈉(1.5當1 ),並將所形成之混合物在〇它下攪拌3〇分鐘, 接著於室溫下2小時。藉由與2N HC1水溶液一起攪拌25分鐘 而使反應淬滅,以IN NaOH水溶液鹼化,及在真空中濃縮。 將殘留物自水以醚萃取,以脫水乾燥,過濾,並使 濾液在真空中濃縮,而得標題化合物,為無色油。 胺90 Ν-(3-苄基-5-甲苄基)環丙胺 步驟1 : 3-苄基-5-曱基苯甲醛 於(3-甲醯基-5-甲基苯基)二羥基硼烷(1當量)之DME溶液 (0.1M)中,添加氟化鉋(3當量)、肆(三苯膦)把(〇1當量)及溴 化芊(1.2當量)。使混合物回流3小時,冷卻至室溫,並以飽 和碳酸氫鈉水溶液使反應淬滅。將混合物以醋酸乙酯萃取。 然後,將合併之有機萃液以鹽水洗滌,以Na〗s〇4脫水乾燥, 過濾,及使濾液在真空中濃縮。粗產物經由急驟式層析之 143482-1 -151 - 201111364 純化(Si〇2 ’己烷—7:3 (v/v)己烷:EtOAc),獲得標題化合物。 步驟2 :胺90 將得自前一步驟之3-芊基-5-曱基苯甲醛(1當量)與環丙基 胺(2當量)合併於中。然後,於其中添加MgS〇4 (1.5當量),並將所形成之懸浮液在室溫下攪拌18小時。接 著,經由過濾,經過矽藻土墊移除不溶物,及使濾液在真 空中濃縮。然後,使如此獲得之粗製亞胺再溶於丁HF: Me〇H 之2:1 (v/v)混合物(〇·2Μ)中。於此溶液中,分次添加硼氫化鈉 (ίο當量),並將所形成之混合物在室溫下攪拌18小時。以 飽和碳酸氫鈉水溶液使反應淬滅,且以醋酸乙酯萃取。然 後,將合併之有機萃液以鹽水洗滌,以Ν%δ〇4脫水乾燥, 過濾,及使濾液在真空中濃縮。粗產物經由急驟式層析之 純化(Si02,CH2C12—9:1 (v/v) CH2C12 : Et0H),獲得標題化合 物。 胺91 N-[3-溴基-5-(3-氟芊基)_4·曱芊基]環丙胺 步驟1 : 3-溴基-5-曱醯基斗曱基苯曱酸曱酯 於3-溴基-5-[(lE)-3-甲氧基-1-丙烯+基]·4_甲基苯曱酸甲酯 (1當量,胺88步驟1)之二氣甲烷(〇16M)溶液中,在_78&lt;^下, 以剛產生之臭氧起泡,直到發現持久藍色為止。然後,將 反應令器以氮充分地滌氣,接著添加三苯膦(ι ι當量)。使 所形成之混合物慢慢溫熱至室溫,歷經6小時。然後,於真 空中移除揮發性物質,並使所形成之殘留物懸浮於己燒與 鱗之1:1 (Wv)混合物中。經由過據,經過㈣墊片移除不溶 143482-1 -152- 201111364 物。如此獲得之遽液在真空中之、、曲 #兴二〒之痕縮,獲得白色固體。粗 產物經由急驟式層析之進一步紬各^ ”、电化(Si〇2,己烧—· 1:1 (v/v)己 烷:EtOAc),獲得標題化合物,為白色固體。 步驟2 : 3-溴基-5-(羥曱基甲基苯曱酸曱酯 於得自前一步驟之3-漠基-5 _甲酿基_4_甲基苯甲酸甲醋(丄 當量)之f醇(am)溶液中,分次添加删氣化納(4當量)。將 所形成之混合物在室溫下授拌3小時。接著,以冷· mStir for 20 hours. The insolubles were then removed via filtration through a pad of diatomaceous earth and the filtrate was concentrated in vacuo. The crude imine thus obtained was then redissolved in MeOH (0.5 M). To the solution, sodium borohydride (15 eq.) was added portionwise, and the resulting mixture was stirred under stirring for 3 hrs and then at room temperature for 2 hr. The reaction was quenched by stirring with a 2N aqueous solution of EtOAc for 25 minutes, basified with aqueous NaOH solution and concentrated in vacuo. The residue was extracted with water from EtOAc (EtOAc m. Amine 89 N-{3-/Smelly-5-[3-(difluorodecyloxy)propyl]_4•indolebenzyl anthracycline Step 1: 3-Bromo-5-(3-hydroxypropyl _4_Methyl benzoate is methyl 3-bromo-5-(3-methoxypropyl)-4-nonylbenzoate. Equivalent, amine, step 2) in chloroform (0.1M) solution with 1 iodotrimethyl; alkane. When). The resulting red solution was allowed to stand at room temperature for -18 hours in the dark. The reaction was quenched with methanol and then the volatiles were removed in vacuo. Then, the formed residue is dissolved in the bond, and the aqueous solution of m is skipped, then the aqueous solution of (iv), water and brine are successively washed. Dehydrated by ~4, filtered, 143482-1 • 149-201111364 and the filtrate is placed in a vacuum. concentrate. The crude product was purified by flash chromatography eluting elut elut elut ' Step 2 . 3_ / 臭基 '5_[3 仁 曱 曱 oxy) propyl M- fluorenyl formic acid methyl vinegar at 5 ° C, in the previous step 3-bromo-5-(3 -Hydroxypropyl)_4_mercaptobenzoic acid vinegar (1 eq.) and sodium sulphate (〇2 #) of acetonitrile (in the suspension of the guanidine, dropwise addition of difluoro(fluorosulfonyl)acetic acid ( 1 eq.), over a period of 10 minutes. After the addition is complete, the reaction suspension is heated at 5 Torr (reheated to room temperature. Then, the reaction mixture is allowed to cool to room temperature, poured into water and extracted with ether. The combined organic extracts were further washed with water and brine, dried over Na2ssssssssssssssssssssssssssssssssssssssssssss </RTI> </RTI> </RTI> <RTI ID=0.0></RTI> </RTI> <RTI ID=0.0></RTI> An aldehyde in a dioxane (0.07 M) solution of 3-bromo-5-[3-(difluoromethoxy)propyl]-4-indolyl benzoate (1 equivalent) from the previous step. Add DIBAL-H (1.5M solution in toluene, 2.2 when) The resulting solution was stirred at room temperature for 1.5 hours, then the reaction was quenched carefully with a 10% aqueous HCl solution. The aqueous layer was separated and extracted with ether. The combined organic extracts were further washed with brine. The Na2S04 was dried over Celite, filtered, and the filtrate was concentrated in vacuo. The crude alcohol thus obtained was again dissolved in dioxane (0.07M), followed by Dess-Martin periodinane (1.0 eq.) and sodium bicarbonate (1.2 eq.) After stirring at room temperature for 40 minutes, the reaction mixture was diluted with ether and washed successively with saturated aqueous NaH.sub.3 O.sub.3, aqueous NaOH, water and brine. </ RTI> 143482-1 • 150· 201111364 organic extract with NaaSO4 Dehydration and drying, filtration, and concentrating the filtrate in vacuo. EtOAc (EtOAc) Step 6: Amine 89 will be obtained from the previous step of 3-bromo-5-[3_(difluoromethoxy)propyl]-4-methylbenzaldehyde (1 equivalent) and cyclopropylamine (2 equivalents) ) is merged into Ch2 (〇1M). Then, add MgS〇4 (1) Equivalent), and the resulting suspension was stirred at room temperature for 20 hours. Then, the insoluble matter was removed by filtration through a pad of diatomaceous earth, and the filtrate was concentrated in vacuo. Then, the crude imine thus obtained was obtained. Re-dissolved in MeOH (0.5 M). To this solution was added sodium borohydride (1.5 as 1) in portions, and the resulting mixture was stirred under stirring for 3 hrs and then at room temperature for 2 hr. The reaction was quenched by stirring with a 2N aqueous HCl solution for 25 min, basified with aqueous <RTI ID=0.0># </RTI> NaOH and concentrated in vacuo. The residue was extracted with EtOAc (EtOAc)EtOAc. Amine 90 Ν-(3-benzyl-5-methylbenzyl)cyclopropylamine Step 1: 3-Benzyl-5-mercaptobenzaldehyde to (3-methylindolyl-5-methylphenyl)dihydroxyboron A fluorinated planer (3 equivalents), hydrazine (triphenylphosphine) (〇1 equivalent) and cesium bromide (1.2 equivalent) were added to a solution of alkane (1 equivalent) in DME (0.1 M). The mixture was refluxed for 3 hours, cooled to room temperature and then quenched with saturated aqueous sodium hydrogen carbonate. The mixture was extracted with ethyl acetate. The combined organic extracts were then washed with brine, dried over Na~s~~~~~~~~~~~~ The crude product was purified by EtOAc EtOAcjjjjj: Step 2: Amine 90 3-Mercapto-5-mercaptobenzaldehyde (1 eq.) obtained from the previous step was combined with cyclopropylamine (2 eq.). Then, MgS〇4 (1.5 eq.) was added thereto, and the resulting suspension was stirred at room temperature for 18 hr. Then, through filtration, the insoluble matter was removed through a diatomaceous earth pad, and the filtrate was concentrated in the sky. The crude imine thus obtained was then redissolved in a 2:1 (v/v) mixture of HF:Me〇H (〇·2Μ). To the solution, sodium borohydride (yield) was added in portions, and the resulting mixture was stirred at room temperature for 18 hr. The reaction was quenched with saturated aqueous sodium bicarbonate and extracted with ethyl acetate. The combined organic extracts were then washed with brine, dried with EtOAc EtOAc EtOAc. The crude product was purified by flash chromatography (EtOAc:EtOAc:EtOAc: Amine 91 N-[3-Bromo-5-(3-fluoroindolyl)-4(indolyl)cyclopropylamine Step 1: 3-bromo-5-indolyl hydrazinyl benzoate decyl ester in 3 - Dimethyl methane (〇16M) of methyl bromide-5-[(lE)-3-methoxy-1-propenyl+yl]-4-methylbenzoate (1 equivalent, amine 88, step 1) In the solution, under _78 &lt; ^, the ozone just generated is foamed until a persistent blue color is found. Then, the reaction reactor was sufficiently purged with nitrogen, followed by the addition of triphenylphosphine (ι eq). The resulting mixture was allowed to slowly warm to room temperature over 6 hours. The volatiles were then removed in the air and the resulting residue was suspended in a 1:1 (Wv) mixture of burned and scaly. After passing through the (4) gasket, the insoluble 143482-1 -152- 201111364 was removed. The sputum thus obtained was in a vacuum and traced to a white solid. The title compound was obtained as a white solid. m.jjjjjjjjjjjjjjjjjjjjjjjjjjj - bromo-5-(hydroxyindolemethyl benzoic acid decyl ester) in the previous step from 3-meryl-5-methyl-branched 4-methylbenzoic acid methyl vinegar (丄 equivalent) of the f-alcohol ( In the am) solution, the degassing sodium (4 equivalents) was added in portions. The resulting mixture was mixed at room temperature for 3 hours. Then, with cold m

水溶液使反應淬滅’且㈣萃取1後,將合併之有機萃 液以水與鹽水洗務,以Na2s〇4脫水乾燥,及過渡。渡液在 真空中之濃縮,獲得標題化合物,為白色固體。 步驟3 : 3-溴基-5-(埃基曱基)·4呷基苯甲酸甲酯 於三苯膦(U當量)之三氣曱烧(〇細)溶液中,添加換(11 s罝)。將所形成之橘黃色懸浮液在室溫下攪拌3〇分鐘,然 後添加咪唑(1.2當量)與最後得自前一步驟之3_溴基;(羥曱 基M-曱基苯曱酸甲酿(1當量)。將目前淡黃色溶液於室溫下 再攪拌30分鐘。在真空中移除揮發性物質’並將殘留物以 己烷與醚之1:1 (Wv)混合物研製。然後,經由過濾,經過矽 膠墊片移除不溶物。濾液在真空中之濃縮,獲得標題化合 物,為白色固體。 步驟4 : 3-溴基-5-(3-氟苄基)_4_甲基苯曱酸曱酯 在-78°C下,於CuCN(2當量)之THF(0.1M)懸浮液中,添加 3-氟苯基溴化鎂(在THF中之〇·5Μ溶液,4當量),歷經5分鐘 期間。將所形成之混合物於_78t下攪拌2〇分鐘,然後在〇 °C下另外20分鐘。使目前黃色懸浮液再冷卻至,接著 143482· 1 •153· 201111364 添加得自前一步驟之3-溴基-5-(蛾基甲基)-4-曱基苯曱酸曱酯 (1當量)。將所形成之混合物於_781下攪拌20分鐘,在〇。(3 下另外20分鐘,及最後在室溫下16小時。以飽和Nh4C1水溶 液:濃NH4〇H之3:1 (v/v)混合物使粗製反應混合物淬滅,然 後以醚萃取。將合併之有機萃液以水與鹽水進一步洗滌, 以NaaSO4脫水乾燥,過濾,及使濾液在真空中濃縮。粗產 物經由急驟式層析之進一步純化(Si〇2,己烷—u (v/v)己烷:The aqueous solution quenched the reaction&apos; and (4) after extraction 1, the combined organic extracts were washed with water and brine, dried over Na 2 s 4 and dried. The mixture was concentrated in vacuo to give the title compound. Step 3: Methyl 3-bromo-5-(e-ylindenyl)-4-mercaptobenzoate is added to triphenylphosphine (U equivalent) in a three-gas calcined solution (11 罝) ). The resulting orange suspension was stirred at room temperature for 3 minutes, then added with imidazole (1.2 equivalents) and finally obtained from the previous step of 3-bromo; (hydroxyindole M-mercaptobenzoic acid) 1 equivalent). The current pale yellow solution was stirred at room temperature for a further 30 minutes. The volatiles were removed in vacuo and the residue was triturated with a 1:1 (Wv) mixture of hexanes and ether. The insoluble material was removed through a silica gel pad. The filtrate was concentrated in vacuo to give the title compound as a white solid. Step 4: 3-bromo-5-(3-fluorobenzyl)-4-methylbenzoate The ester was added to a suspension of CuCN (2 equivalents) in THF (0.1 M) at -78 ° C, and then added 3-fluorophenylmagnesium bromide (5 Μ solution in THF, 4 equivalents) over 5 minutes. The resulting mixture was stirred at -78 t for 2 min and then at 〇 ° C for an additional 20 min. The current yellow suspension was allowed to cool again, followed by 143482·1 •153·201111364 added from the previous step 3 - bromo-5-(mothylmethyl)-4-mercaptobenzoic acid decyl ester (1 equivalent). The resulting mixture was stirred at -781 for 20 min. The crude reaction mixture was quenched with a saturated aqueous solution of N.sub.2C.sub.1: EtOAc (aq.). The combined organic extracts were further washed with water and brine, dried over Na NaSO 4, filtered, and the filtrate was concentrated in vacuo. The crude product was further purified by flash chromatography (Si〇2, hexane-u (v/) v) Hexane:

EtOAc) ’獲得標題化合物,為無色油。 步驟5 : 3-溴基-5-(3-氟苄基)-4-曱基苯曱酸 修 於得自前一步驟之3-溴基-5-(3-氟苄基)-4-甲基苯曱酸甲酯 (1當量)之一氣曱烧(0.1M)溶液中,添加DIBAL-H (在甲苯中 之1.5M落液’ 2.2當量)。將所形成之溶液在室溫下授拌丄5 小時’然後以10% HC1水溶液小心地使反應淬滅。分離水層, 並以醚逆萃取。將合併之有機萃液以鹽水進一步洗滌,以 NadO4脫水乾燥’過濾,及使濾液在真空中濃縮。使如此 獲得之粗製醇再一次溶於二氯曱烷(〇 1M)中,然後添加 Dess-Martin過碘烷(1.〇當量)與碳酸氫鈉(1 2當量)。在室溫下 ® 攪拌40分鐘後’將反應混合物以醚稀釋,並以飽和NaHS〇3 水溶液、IN NaOH水溶液、水及鹽水相繼洗滌。使有機萃液 以NadO4脫水乾燥,過濾,及使濾液在真空中濃縮。粗產 物經由急驟式層析之純化(Si02,己烷—1:1 (v/v)己烷:The title compound was obtained as a colorless oil. Step 5: 3-Bromo-5-(3-fluorobenzyl)-4-mercaptobenzoic acid was triturated from 3-bromo-5-(3-fluorobenzyl)-4-methyl from the previous step To a solution of methyl benzoate (1 eq.) in a gas smoldering (0.1 M) solution, DIBAL-H (1.5 M drop in toluene '2.2 eq.) was added. The resulting solution was stirred at room temperature for 5 hours' and then the reaction was carefully quenched with a 10% aqueous HCl solution. The aqueous layer was separated and back extracted with ether. The combined organic extracts were further washed with brine, dried <RTI ID=0.0>Aq. The crude alcohol thus obtained was again dissolved in dichloromethane (〇1M), then Dess-Martin periodinane (1. 〇 equivalent) and sodium hydrogencarbonate (12 eq.) were added. After stirring at room temperature for 40 minutes, the reaction mixture was diluted with ether and washed successively with saturated aqueous NaHCI3, aqueous EtOAc, water and brine. The organic extract was dried over NadO4, filtered, and the filtrate was concentrated in vacuo. Purification of the crude product by flash chromatography (SiO 2 , hexane - 1:1 (v/v) hexane:

EtO Ac) ’獲得標題化合物,為無色油。 步驟6 :胺91 將得自前一步驟之3-溴基-5-(3-氟芊基)-4-曱基苯甲醛(1當 143482-1 •154- 201111364 量)與環丙基胺(2當量)合併於CH2Cl2(〇1M)中。然後,於其 中添加MgS〇4(1當量),並將所形成之懸浮液在室溫下搜摔 μ由藻土塾移除不溶物,及 使濾液在真空中濃縮。然後,使如此獲得之粗製亞胺再溶 於Me〇H(〇.1M)中。於此溶液中,分次添加硼氫化鈉(15當量) ,並將所形成之混合物在0°C下攪拌30分鐘,接著於室溫下 2小時。藉由與2N HC1水溶液一起攪拌25分鐘而使反應淬 滅,以1N Na0H水溶液鹼化,及在真空中濃縮。將殘留物自 水以醚萃取,以NaaSO4脫水乾燥,過濾,及使濾液在真空 中濃縮,而得標題化合物,為無色油。 胺92 {3-溴基-5-[(環丙胺基)曱基]-2-甲基笨基K3_氟苄基)曱酮 步驟1 ·· 3-溴基-5-[(1Ε)-3-曱氧基-1-丙烯小基]_4_甲基苯甲醛 於3-溴基-5-[(1Ε)-3-曱氧基-1-丙烯-1-基]_4-曱基苯甲酸甲醋 (1當量’胺88步驟1)之二氣曱烷(0.1Μ)溶液中,添加DIBAL-H 鲁 (在曱本中之1 ·5Μ溶液’ 2.2當量)。將所形成之溶液在室溫 下攪拌1.5小時,然後以10% HC1水溶液小心地使反應淬滅。 分離水層,並以醚逆萃取。將合併之有機萃液以鹽水進— 步洗滌’以Na2S04脫水乾燥,過濾,及使濾液在真空中濃 縮。使如此獲得之粗製醇再一次溶於二氣曱烷(0.1M)中,接 著添加Dess-Martin過破烧(1.0當量)與碳酸氩納(1.2當量)。在 室溫下攪拌40分鐘後,將反應混合物以醚稀釋,並以飽和 NaHS03水溶液、IN NaOH水溶液、水及鹽水相繼洗務。使有 機萃液以Na2S04脫水乾燥,過濾,及使濾液在真空中濃縮。 143482-1 -155- 201111364 粗產物經由急驟式層析之純化(Si〇2,己烷—ι:ι 力己烷:EtO Ac) 'The title compound was obtained as a colorless oil. Step 6: Amine 91 will be obtained from the previous step of 3-bromo-5-(3-fluoroindolyl)-4-mercaptobenzaldehyde (1 when 143482-1 • 154-201111364) and cyclopropylamine ( 2 equivalents) were combined in CH2Cl2 (〇1M). Then, MgS〇4 (1 equivalent) was added thereto, and the resulting suspension was subjected to a drop at room temperature. The insoluble matter was removed from the mash, and the filtrate was concentrated in vacuo. Then, the crude imine thus obtained was redissolved in Me〇H (〇.1M). To this solution, sodium borohydride (15 equivalents) was added portionwise, and the resulting mixture was stirred at 0 ° C for 30 minutes, then at room temperature for 2 hours. The reaction was quenched by stirring with a 2N aqueous HCl solution for 25 min, basified with 1N aqueous NaHH and concentrated in vacuo. The residue was extracted with EtOAc (EtOAc)EtOAc. Amine 92 {3-Bromo-5-[(cyclopropylamino)indolyl]-2-methylindolyl K3_fluorobenzyl)fluorenone Step 1 ·· 3-Bromo-5-[(1Ε)- 3-methoxy-1-propenyl small group]_4_methylbenzaldehyde in 3-bromo-5-[(1Ε)-3-decyloxy-1-propen-1-yl]_4-mercaptobenzene To a solution of methyl formate (1 equivalent of 'amine 88 step 1) in dioxane (0.1 Torr), DIBAL-H ru (1. 5 Μ solution in the sputum '2.2 eq.) was added. The resulting solution was stirred at room temperature for 1.5 hours and then quenched carefully with 10% aqueous EtOAc. The aqueous layer was separated and back extracted with ether. The combined organic extracts were washed with brine and dried over Na.sub.2SO.sub. The crude alcohol thus obtained was again dissolved in dioxane (0.1 M), followed by addition of Dess-Martin over-crushing (1.0 eq.) and argon carbonate (1.2 eq.). After stirring at room temperature for 40 minutes, the reaction mixture was diluted with ether and washed successively with saturated aqueous NaH.sub.3, aqueous NaOH, water and brine. The organic extract was dehydrated and dried over Na 2 SO 4 , filtered, and the filtrate was concentrated in vacuo. 143482-1 -155- 201111364 Purification of crude product by flash chromatography (Si 〇 2, hexane - ι: ι hexane:

EtOAc),獲得標題化合物,為無色油’其係在靜置時固化。 步驟2 : N-{3-漠基州E)_3_甲氧基小丙稀巧基]_4甲爷幻環丙 胺 將2自前一步驟之3·溴基_5·[(1ε) 3甲氧基小丙烯小基]氺 曱土苯甲搭(1虽量)與環丙基胺(2當量)合併於C% C12 (〇 1Μ) 中、然後’於其中添加Mgso4(1當量),並將所形成之縣浮 液在室溫下攪拌20小時。接著,經由過渡,經過石夕藻I塾 移除不溶物,及使渡液在真空中濃縮。然後使如此獲得 之粗製亞胺再溶於Me0H(0·1Μ)中。於此溶液中,分次添加 ^虱化納(1·5當量)’並將所形成之混合物在叱下搜㈣分 鐘,然後於室溫下2小時。藉由與加肥水溶液一起搜摔乃 分鐘而使反應淬滅’幻NNaQH水溶㈣化及在真空中濃 縮。將殘留物自水以趟萃取,以叫沁4脫水㈣,過遽, 及使據液在真空中濃縮,而得標題化合物,為無色油。 步驟3: {3-演基-5__.甲氧基巧·丙稀巧基]冰甲爷基滩丙基 胺基甲酸第三-丁酯 使得自前-步狀N__基_5•[叫3_甲氧基]㈣小基]· 4-甲爷基環丙胺(1當量)與二碳酸二第三丁醋(u當量) ^於二氣甲烧(α_中。然後,於其中添加Humg氏驗㈣ 里)’並將所形成之混合物在室溫下攪拌3小時。於真*中 移除揮發性物質,錢所形成之殘留物溶於己㈣^Η (v/v)混合物中。接著’將此懸浮液以1〇%肥水溶液、水及 鹽水脫水乾燥’過渡,及使遽液在真空中 143482·】 -156- 201111364 濃縮。如此獲得之粗產物經由管柱層析之純化(Si〇2,己烷 —1:1 (v/v)己烧:EtOAc),獲得標題化合物’為無色油。 步驟4: (3-溴基-5-甲醯基-4-甲芊基)環丙基胺基曱酸第三-丁酯 於得自前一步驟之{3-溴基-5-[(1Ε)-3-甲氧基-1-两烯小基]_4_ 甲芊基}環丙基胺基甲酸第三-丁酯(1當量)之二氯曱烷 (0.08M)溶液中,在_78°c下,以剛產生之臭氧起泡,直到發 現持久藍色為止。然後’將反應容器以氮充分地滌氣,接 著添加三苯膦(1當量)。使所形成之混合物慢慢溫熱至室溫 ’歷經16小時。然後,於真空中移除揮發性物質,並使所 形成之殘留物懸浮於己烷與醚之1:1 (v/v)混合物中。經由過 /慮’經過石夕膠塾片移除不溶物。如此獲得之渡液在真空中 之濃縮,獲得無色油。粗產物經由急驟式層析之進一步純 化(Si〇2,己院—i:i (ν/ν)己烧:Et〇Ac),獲得標題化合物, 為無色油。 步驟5: {3-漠基-5-[(3-氟苯基)(經基)曱基]-4-曱芊基卜環丙基胺 基曱酸第三-丁酯 在〇°C下,於得自前一步驟之(3_溴基_5·曱醯基_4_曱苄基) 環丙基胺基曱酸第三-丁酯(1當量)之THF (〇13M)溶液中,添 加3-氟苯基溴化鎂(0·5Μ,在THF中,u當量)。使所形成之 溶液慢慢地溫熱至室溫,歷經2小時,然後以飽和NH4C1水 溶液使反應淬滅。分離水層,並以醚逆萃取,將合併之有 機萃液以水與鹽水進一步洗滌,以N^SO4脫水乾燥,過濾, 及使濾液在真空中濃縮。粗產物經由急驟式層析之進一步 純化(Si〇2,己烷—1:1 (v/v)己烷:Et0Ac),獲得標題化合物, 143482-1 •157· 201111364 為無色油。 步驟6 : [3-溴基-5-(3-氟笨曱醯基)_4_曱芊基]環丙基胺基曱酸 第三-丁酯 於得自前一步驟之丨3-溴基-5-[(3-氟苯基)(羥基)曱基]-4-曱 苄基}環丙基胺基甲酸第三·丁酯(1當量)之二氣曱烷(〇 1M) 溶液中’添加Dess-Martin過碘烷(l.o當量)與碳酸氫鈉(丨2當 1 )。在室溫下授拌1小時後’將反應混合物以醚稀釋,並 以飽和NaHS〇3水溶液、in NaOH水溶液、水及鹽水相繼洗滌。 使有機萃液以Na2S〇4脫水乾燥,過濾,及使濾液在真空中 濃縮,而得標題化合物,為無色油。 步驟7 :胺92 於cH2C12(o.im)中之得自前一步驟之[3_溴基_5_(3_氟苯曱醯 基)-4-曱苄基]環丙基胺基曱酸第三_ 丁酯(1當量)内,添加Ηα (4.0M,在二氧陸圜中,2〇當量)。將所形成之溶液在室溫 下攪拌2小時。然後,以1N Na〇H水溶液使反應淬滅,且以 醚萃取。接著,將合併之有機萃液以水與鹽水進一步洗滌, 以NazSO4脫水乾燥,及過濾。濾液在真空中之濃縮,獲得 標題化合物’為無色油。 在表2中之芳環結構單位係按下述合成而得。 表2 化合物 結構 化合物 結構 芳環1 Br 芳環3 1 143482-1 -158- 201111364 化合物 結構 芳環2 Me^N^OBn MeV Br 化合物 結構 芳環4 Ν^ΟΒη (J Τ Br 芳環1 4-溴基-2-(曱氧基)吡啶 芳環 1 係根據由 Fraley, Μ· E.等人 C/zem/jtryThe title compound was obtained as a colorless oil, which was solidified upon standing. Step 2: N-{3-Mojiki E)_3_methoxy propylene small base]_4 甲幻幻环丙胺2 2 from the previous step 3 · bromo _5 · [(1ε) 3 methoxy Small propylene small base] Benzene benzoate (1) and cyclopropylamine (2 equivalents) are combined in C% C12 (〇1Μ), and then 'Mgso4 (1 equivalent) is added thereto, and The formed county float was stirred at room temperature for 20 hours. Next, through the transition, the insoluble matter was removed through the diarrhea, and the liquid was concentrated in a vacuum. The crude imine thus obtained was then redissolved in MeOH (0.11 Torr). To this solution, sodium hydride (1.5 equivalents) was added in portions and the resulting mixture was searched for a period of four (4) minutes and then at room temperature for 2 hours. The reaction was quenched by searching for a minute with the addition of the aqueous solution of the fertilizer. The phantom NNaQH was hydrolyzed (four) and concentrated in a vacuum. The residue is extracted from water with hydrazine, and the title compound is obtained as a colorless oil. Step 3: {3-基基-5__.methoxy-acrylic-acrylic]Icyl yl propyl propylaminocarbamic acid tri-butyl ester makes the self-step-like N__base _5•[3 _Methoxy](tetra)小基]· 4-Merylcyclopropylamine (1 eq.) and diacetate diacetate (u eq.) ^ in dioxane (α_. Then, add Humg to it) Test (4)) and the resulting mixture was stirred at room temperature for 3 hours. The volatile matter is removed from Yuzhen*, and the residue formed by the money is dissolved in the mixture of (4) and (v/v). Then, the suspension was dehydrated and dried with a 1% aqueous solution of fertilizer, water and brine, and the mash was concentrated in a vacuum 143482·] -156- 201111364. The crude product thus obtained was purified by column chromatography (EtOAc EtOAc (EtOAc) Step 4: (3-Bromo-5-mercapto-4-methylindenyl)cyclopropylamino decanoic acid tert-butyl ester from {3-bromo-5-[(1Ε) obtained from the previous step a solution of 3-methoxy-1-enediyl small group]_4_methylamino}cyclopropylaminocarbamic acid tert-butyl ester (1 equivalent) in dichlorodecane (0.08 M) at -78 At °c, the ozone just generated is foamed until a long-lasting blue color is found. Then, the reaction vessel was sufficiently purged with nitrogen, followed by the addition of triphenylphosphine (1 equivalent). The resulting mixture was allowed to slowly warm to room temperature for 16 hours. The volatiles were then removed in vacuo and the resulting residue was suspended in a 1:1 (v/v) mixture of hexanes and ether. The insoluble matter was removed through the zebra capsules. The thus obtained liquid was concentrated in a vacuum to obtain a colorless oil. The crude product was further purified by flash chromatography (Si </ RTI> </ RTI> </ RTI> </ RTI> </ RTI> </ RTI> </ RTI> </ RTI> <RTIgt; Step 5: {3-Molyl-5-[(3-fluorophenyl)(trans)indolyl]-4-indolylcyclopropylamino decanoic acid tert-butyl ester at 〇°C , in a solution of (3_bromo-5-fluorenyl-4-benzyl)cyclopropylamino decanoic acid tert-butyl ester (1 equivalent) in THF (〇13M) from the previous step, 3-Fluorophenylmagnesium bromide (0.5 Torr in THF, u equivalent) was added. The resulting solution was slowly warmed to room temperature over 2 hours and then quenched with saturated aqueous NH4CI. The aqueous layer was separated and extracted with ether. The combined organic extracts were washed with water and brine, dried over N?SO?, filtered, and concentrated. The crude product was purified by EtOAc EtOAc EtOAc (EtOAc) Step 6: [3-Bromo-5-(3-fluorobenzyl)-4-indolyl]cyclopropylamino decanoic acid tert-butyl ester from the 3-bromo group obtained from the previous step - 5-[(3-Fluorophenyl)(hydroxy)indolyl]-4-hydrazino}}cyclopropylaminocarbamic acid tert-butyl ester (1 equivalent) in dioxane (〇1M) in solution Add Dess-Martin periodinane (lo equivalent) with sodium bicarbonate (丨2 when 1). After the mixture was allowed to stand at room temperature for 1 hour, the reaction mixture was diluted with ether and washed successively with a saturated aqueous solution of Na.sub.2.sub.3, in aqueous NaOH, water and brine. The organic extract was dried with EtOAc (EtOAc)EtOAc. Step 7: Amine 92 in cH2C12 (o.im) from [3_bromo- 5-(3-fluorophenylindenyl)-4-hydrazinobenzyl]cyclopropylamino decanoic acid Within the tri-butyl ester (1 equivalent), Ηα (4.0 M in dioxane, 2 〇 equivalent) was added. The resulting solution was stirred at room temperature for 2 hours. Then, the reaction was quenched with a 1N aqueous NaH solution and extracted with ether. Next, the combined organic extracts were further washed with water and brine, dried over NazSO4, and filtered. The filtrate was concentrated in vacuo to give the title compound <RTI ID=0.0> The aromatic ring structural units in Table 2 were synthesized as follows. Table 2 Compound structure Compound structure Arrocyclic ring 1 Br Aromatic ring 3 1 143482-1 -158- 201111364 Compound structure aromatic ring 2 Me^N^OBn MeV Br Compound structure aromatic ring 4 Ν^ΟΒη (J Τ Br aromatic ring 1 4- Bromo-2-(decyloxy)pyridine aromatic ring 1 is based on Fraley, Μ· E. et al. C/zem/jtry

Leiiers 2002,〗2, 3537-3542所述之程序製成。 芳環2 ® 4-溴基-2,3-二甲基-6-[(苯基曱基)氧基Μ啶 使根據由 McElroy, W. Τ ; DeShong, R Ogam’c Leiiers 2003,5, 4779-4782所述程序製成之4-溴基-5,6-二曱基-2(1H)-吡啶酮(1 當量)懸浮於苯(0.13M)中。然後,於其中添加碳酸銀(0.6當 量)與溴化苄(1.2當量),接著將此懸浮液在45°C下,於黑暗 中加熱3天。使反應懸浮液冷卻至室溫,以苯稀釋,並經過 矽藻土床過濾。將濾液以飽和NaHC03水溶液洗滌,以Na2S04 0 脫水乾燥,過濾,及使濾液在真空中濃縮。經由管柱層析 之純化(Si02,己烷—10:1 (v/v)己烷:EtOAc),獲得標題化合 物,為無色油。 芳環3 4-碘基-3-{[(甲氧基)甲基]氧基}吡啶 步驟1 : 2-{[(曱氧基)曱基]氧基}吡啶 使3-吡啶醇(1當量)溶於DMF : THF之2:1 (v/v)混合物(0.9M) 中。然後,於其中,在-15°C下添加第三-丁醇鉀(1.1當量), 並將所形成之懸浮液於-15°C下攪拌25分鐘,接著逐滴添加 143482-1 -159- 201111364 氣基甲基甲基醚(u當量),歷經15分鐘。然後,使混合物 溫熱至室溫,歷經1小時,且將其在室溫下再攪拌2小時。 接著,使反應混合物於真空中濃縮,i將所形成之殘留物 於EtOAc與水之間作分液處理。分離水層,且以逆萃 取。然後,將合併之有機萃液以水與鹽水洗滌,以Na2s〇4 脫水乾燥,經過短Si〇2填充柱過濾,及使濾液在真空中濃 縮’而得標題化合物,為無色油。 步驟2:芳環3 在-78°C下’於得自前一步驟之2_丨[(曱氧基)曱基]氧基}吡啶 (1當量)在醚(0.16M)中之溶液内,逐滴添加第三丁基鋰 (1.7M,在戊烷中,U當量),歷經3〇分鐘期間。將其在% °C下攪拌15分鐘,然後逐滴添加碘(〇 5M,在醚中,i 2當 里),歷經30分鐘期間。接著,將反應混合物於_78。〇下攪拌 1小時,然後以水使反應淬滅。分離水層,並以醚逆萃取。 將合併之有機萃液以10% NaHS〇3水溶液、水及鹽水相繼洗 滌,以NasSO4脫水乾燥,及過濾。濾液在真空中之濃縮, 獲得米黃色粉末。如此獲得之粗產物經由管柱層析之純化 (Si〇2,9:1 (v/v)己烷:Et〇Ac_^Et〇Ac) ’獲得標題化合物,為 白色固體。 芳環4 2-(苄氧基)-4-溴基吡啶 於4-溴基-2-氟基吡啶(1當量)、芊醇(12當量)及二苯并_18_ 冠-6醚(〇.〇5當量)在甲苯(〇·4Μ)十之溶液内,添加氫氧化鉀(2 當量)。然後,連接Dean_Stark裝置,並將反應懸浮液於回流 143482-1 •160- 201111364 下加熱3小時。於冷卻至室溫後,將反應混合物以己烷稀釋, 接著經過矽藻土墊過濾。濾液在真空中之濃縮,獲得黃色 油。如此獲得之粗產物經由管柱層析之純化(&amp;〇2,97:3 (v/v) 己烧.Et2 Ο),獲得標題化合物,為無色油。 羧酸1 叛酸結構單位(羧酸i ; (3S,4S)-r-曱基-2·-酮基_3,4,5,6,Γ,2,-六 氫-2Η-[4,4’]聯吡啶基-ΐ,3_二羧酸μ第三_丁酯)係按下述合成 而得。The procedure described in Leiiers 2002, 〗 2, 3537-3542. Aromatic Ring 2 ® 4-Bromo-2,3-dimethyl-6-[(phenylindenyl)oxyacridine is based on by McElroy, W. Τ; DeShong, R Ogam'c Leiiers 2003, 5, The 4-bromo-5,6-dimercapto-2(1H)-pyridone (1 eq.) prepared as described in 4779-4782 was suspended in benzene (0.13 M). Then, silver carbonate (0.6 equivalents) and benzyl bromide (1.2 equivalents) were added thereto, and the suspension was heated at 45 ° C for 3 days in the dark. The reaction suspension was cooled to room temperature, diluted with benzene and filtered over a pad of Celite. The filtrate was washed with aq. aq. EtOAc (aq.). The title compound was obtained as a colorless oil. Aromatic ring 3 4-iodo-3-{[(methoxy)methyl]oxy}pyridine Step 1: 2-{[(indolyl)indenyl]oxy}pyridine gives 3-pyridinol (1 Equivalent) is dissolved in a 2:1 (v/v) mixture of DMF:THF (0.9 M). Then, potassium tributoxide (1.1 equivalent) was added thereto at -15 ° C, and the resulting suspension was stirred at -15 ° C for 25 minutes, followed by dropwise addition of 143482-1 -159- 201111364 Gas-based methyl methyl ether (u equivalent) over 15 minutes. Then, the mixture was allowed to warm to room temperature over 1 hour, and it was stirred at room temperature for further 2 hours. Next, the reaction mixture was concentrated in vacuo to give a crystallite crystal crystal crystal crystal crystals The aqueous layer was separated and taken up in reverse. The combined organic extracts were washed with water and brine, dried over Na2ssssssssssssssssssssssssss Step 2: The aromatic ring 3 is at -78 ° C in a solution of 2_丨[(decyloxy)indolyl]oxy}pyridine (1 equivalent) in the previous step in ether (0.16 M). Ternary butyllithium (1.7 M in pentane, U equivalent) was added dropwise over a period of 3 min. It was stirred at % ° C for 15 minutes, then iodine (〇 5M in ether, i 2 ) was added dropwise over a period of 30 minutes. Next, the reaction mixture was at -78. The mixture was stirred for 1 hour, and then quenched with water. The aqueous layer was separated and back extracted with ether. The combined organic extracts were washed successively with 10% aq. NaH.sub.3, water and brine, dried over NasSO4 and filtered. The filtrate was concentrated in vacuo to give a beige powder. The crude product thus obtained was purified by EtOAc EtOAcjjjjjjjj Aromatic ring 4 2-(benzyloxy)-4-bromopyridine in 4-bromo-2-fluoropyridine (1 equivalent), decyl alcohol (12 equivalents) and dibenzo- 18_ crown-6 ether (〇 〇5 equivalents) Potassium hydroxide (2 equivalents) was added to a solution of toluene (〇·4Μ). Then, the Dean_Stark apparatus was connected, and the reaction suspension was heated under reflux for 14 hours at 143482-1 • 160-201111364. After cooling to room temperature, the reaction mixture was diluted with hexanes and filtered thru a pad. The filtrate was concentrated in vacuo to give a yellow oil. The crude product thus obtained was purified by column chromatography ( &amp; </ RTI> </ RTI> </ RTI> </ RTI> </ RTI> <RTIgt; Carboxylic acid 1 tickic acid structural unit (carboxylic acid i; (3S, 4S)-r-mercapto-2·-keto_3,4,5,6,Γ,2,-hexahydro-2Η-[4, 4']bipyridyl-indole, 3-dicarboxylic acid μ-t-butyl ester) was synthesized as follows.

TFA 步驟1 : 4-溴基-2-甲氧基ρ比咬 將4-肩基-2-氣峨D定、甲醇鈉(16當量)及甲苯$ j份體積) 加熱至95 C,歷經40小時。添加甲苯(61份體積)與水(3份體 積)並將下層水相切除。將有機物質以水(ι·5份體積)洗滌, 然後使揮發性物質蒸發’而得標題化合物’為油狀物。hrms (ES,M+H)計算值 187·9711 實测值 ΐ87 97ΐι。 ν驟2 . 2 -甲氧基_5,6_二氫_2η [4 4,]聯吡啶基-υ•二羧酸3乙酯 三氟曱基酯 143482-1 -161 - 201111364 將醋酸鉀(2.0當量)、雙(品吶可基)二硼(1〇5當量)及市購 可得之Pd(Cl)2dppf.二氣甲烷複合物(0.02當量)在2_曱基THF (6.5份體積)與N,N-二曱基乙醯胺(1份體積)中混合。添加2_ 曱基THF(3.4份體積)中之4-溴基-2-曱氧基吡啶,並將混合物 加熱至85°C,歷經4小時,然後冷卻至25t。添加已溶於水 (4.9份體積)中之碳酸氫鉀(3.〇當量),接著為三氟曱烷磺酸 3-(乙氧羰基)-1-(2’2,2-三氟乙醯基)_ι,2,5,6-四氫吡啶_4_基酯(1 〇2 當量)。二氟甲烷磺酸3-(乙氧羰基)小(2,2,2-三氟乙醯基) 四氫吡啶-4-基酯可使用關於獲得其中在氮上之三氟乙醯乙 醯胺基團為Boc基團之類似化合物之已知方法,利用市購可 得之/3酮酯(下方1)獲得。TFA Step 1: 4-Bromo-2-methoxy ρ ratio bite 4-sodium-2-carboindole D, sodium methoxide (16 equivalents) and toluene (j part volume) heated to 95 C, after 40 hour. Toluene (61 parts by volume) and water (3 parts by volume) were added and the lower aqueous phase was removed. The organic material was washed with water (1·5 parts by volume), and then the volatile material was evaporated to give the title compound as an oil. Hrms (ES, M+H) calculated 187·9711 measured value ΐ87 97ΐι.骤2. 2 -Methoxy_5,6-dihydro-2η [4 4,]bipyridyl-indole dicarboxylic acid 3 ethyl ester trifluorodecyl ester 143482-1 -161 - 201111364 Potassium acetate (2.0 equivalents), bis(quinolyl)diboron (1〇5 equivalent) and commercially available Pd(Cl)2dppf. digas methane complex (0.02 equivalents) in 2_mercapto THF (6.5 parts) The volume is mixed with N,N-dimercaptoacetamide (1 part by volume). 4-Bromo-2-indolylpyridine in 2_ mercapto THF (3.4 parts by volume) was added, and the mixture was heated to 85 ° C for 4 hours and then cooled to 25t. Add potassium bicarbonate (3. 〇 equivalent) dissolved in water (4.9 parts by volume), followed by 3-(ethoxycarbonyl)-1-(2'2,2-trifluoroethyl trifluoromethanesulfonate醯,), 2,5,6-tetrahydropyridine _4_yl ester (1 〇 2 equivalent). 3-(ethoxycarbonyl)succinyl (2,2,2-trifluoroethyl)tetrahydropyridin-4-yl difluoromethanesulfonate can be used to obtain trifluoroacetamidine which is present on nitrogen A known method in which a group is a similar compound of a Boc group is obtained using a commercially available /3 ketoester (bottom 1).

rNccrNcc

ο 0B 添加另外之Pd(Cl)2dPPf.二氣甲烷複合物(〇 〇〇5當量),並將 此批料加熱至85t,歷經2小時’然後冷卻至20t,且使其 沉降。將下層水相切除,並將有機物質以水洗務,接著通 過砂膠充填柱。使有機溶液濃縮至~116份體積,然後添加 市購可付之HBF4.〇Et2(l.l當量)。使此批料冷卻至2(rc ,熟 成小時,接著藉由蒸餾移除另外4份體積溶劑,並使漿液 卩至1 C。過濾所形成之漿液,且將固體以醋酸異丙酯 '先滌而知軚題化合物,為灰白色固體。1 H NMR (4〇〇 MHz, 細㈣6) 5 12·2 (br S,1H),817 (cU = 5.2 Hz,1H),6.90 (d,J = 4.8 Hi H), 6.81-6.79 (m, 1H), 4.43-4.35 (m, 2H), 3.97-3.83 (m, 5H), 3.82-3.75 143482-1 •162- 201111364 (m,2H),2.62-2.55 (m,2H),0.92-0.83 (m,3H)。HRMS (ES,M+H)計算 值 359.1219.實測值 359.1237。 步驟 3: (3R,4S)-2,-曱氧基-3,4,5,6-四氫-2H-[4,4,]聯吡啶基-1,3-二緩 酸3-乙酯1-三氟曱基酯 將2’-曱氧基-5,6-二氫-2H-[4,4']聯吡啶基-l,3-二羧酸3-乙酯1- 三氟曱基酯在2-曱基THF (6.4份體積)與二氣曱烷(1.5份體 積)中配成漿液’並添加HBF4 .OEt2 (〇_1當量)。觸媒溶液係經 鲁 由使市購可得之雙(2-曱烯丙基)(COD))Ru(II) (0.01當量)與市 構可得之(R)-1-[(S)-二-2-呋喃基膦基]二環戊二烯鐵基]乙基二 -第三-丁基膦(0.0125當量)溶於二氣曱烷(0J2份體積)中而製 成’並添加至前述漿液中。然後,將漿液加熱至5crc,且 以氫加壓至8巴。於熟成2小時後,使此批料冷卻至2〇°c。 添加NaHCOs (1.5當量)之水溶液,並使液層沉降。流出下層 水相’且拋棄。將有機層以10重量% NaCl溶液洗滌,並將 下層水相切除,及拋棄。關於產物,使溶液在真空中蒸餾 # 至〜2份體積’接著添加DMF (2份體積),並將所形成之溶液 用於下一步驟。HRMS (ES,M+H)計算值361.1375·實測值 361.1367。 步驟 4. (3R’4S)-r-甲基-2’-酮基-3,4,5,6/,2:六氫-2H-[4,4,]聯吡啶基 -1,3-二羧酸3-乙酯1-三氟甲基酯 於DMF/2-MeTHF中作成溶液之(3R,4S)4,_甲基_2,酮基 -3,4,5,6,1',2’-六氫_2«:-[4’4']聯吡啶基_1,3_二羧酸3_乙醋1_三氟甲 基酯之經攪拌溶液内,添加碘化三曱基硫鑌(15當量)、氫 氧化鎂(1.5當量)及水(1.〇當量)。將漿液加熱至l〇〇t,歷經 Ϊ 43482-1 -163- 201111364 5小時,然後冷卻至環境溫度。添加二氣曱烷(3份體積)與 醋酸異丙酯(5份體積)’接著為4M HC1 (2.5當量)。然後,分 離液相’並將下層水溶液以二氣曱烷(1·89份體積)萃取,且 合併有機物質。將有機物質以25重量% LiC1溶液洗滌。關 於產物’使有機層在真空中蒸餾至〜5份體積,並使產物結 晶。關於產物,蒸餾係持續至〜2.5份體積,然後添加甲基_ 第三丁基醚(1份體積),及使漿液冷卻至_3t:,熟成2小時, 接著過濾。將固體以曱基-第三丁基醚洗滌,而得產物,為 6.13 (m, 2H), 4.59-4.55 ((m, 0.6H), 4.47-4.40 (m, 0.4H), 4.08-3.95 (m, 1H), 3.92-3.82 (m, 2H), 3.69-3.53 (m, 0.4H), 3.45-3.25 (m, 4.6H), 3.12-2.95 (m, 1H), 2.34-2.18 (m, 1H),1.85-1.75 (m, 1H),1.03-0.96 (m, 3H)。HRMS (ES, M+H)計算值 361.1375.實測值 361.1392。 步驟 5: (3S,4S)-1·-甲基-2’-酮基-3,4,5,6,Γ,2,-六氫-2H-[4,4]聯吡啶基 -1,3-二羧酸1-第三-丁酯 於(3R,4S)-1’-曱基-2’-酮基-3,4,5,6,1_,2,-六氫-2H-[4,4]聯吡啶基 -1,3-二緩酸3-乙酯1-三氟曱基酯在乙醇(4.1份體積)中之經檀 拌溶液内,添加乙醇鈉(1.20當量)。使混合物熟成3〇分鐘, 然後添加水(1.20當量)。於1小時熟成後,添加b〇c酐(1.20當 量),並使溶液熟成1小時。添加氫氧化鈉(2M,5.00當量), 且將溶液加熱至70°C,歷經1小時。使混合物冷卻至3〇°C, 並使溶液濃縮至份體積,以致使大部份乙醇被移除。將 溶液以MTBE (2.5份體積)洗滌。分離水層,然後以濃HC1酸 化,而得漿液。接著,添加2-曱基四氫吱喃(6份體積),且 143482-1 -164- 201111364 :-勿卜夬逮地授拌’然後將液層分離。移除水層,並收 集有拽物吳。接著,將水層再裝填至萃取器,且以MeTHF (2 伤體積)逆萃取。然後,將有機離份再裝填至萃取器,以50% 氣化鈉/奋液洗滌。收集有機層,及在真空中濃縮,而得泥 狀淡黃色固體。將固體在MTBE (6份體積)中配成漿液,並 於室溫下攪拌18小時。將漿液過濾至MTBE中,並以其洗滌, 而得私題化合物,為灰白色固體。! H NMR (5〇〇 MHz,CHa3 ): δ 7.30-7.26 (m, 1H), 6.74 (s, 1H), 6.25 (dd, J = 6.96, 2.00 Hz, 1H), 4.44 (s, 1H), 4.30 (s, 1H), 3.52 (s, 3H), 3.09-2.73 (m, 3H), 2.59 (s, 1H), 1.77 (d, J = 13.10 Hz, 1H),1.61 (d,J = 12.58 Hz, 1H),1.48 (s, 9H)。HRMS (ES, M+H)計算值 337· 1763.實測值 337.1768。 實例1 反式-N-環丙基-N-[(2,3-二氣苯基)曱基]-4-(1-甲基_2_酮基-1,2-二 氫-4-p比唆基)-3-六氫p比。定後酿胺ο 0B Additional Pd(Cl) 2dPPf. digas methane complex (〇 5 equivalents) was added and the batch was heated to 85 t for 2 hours' then cooled to 20 t and allowed to settle. The lower aqueous phase is cut off and the organic material is washed with water, followed by filling the column with sand. The organic solution was concentrated to ~116 parts by volume, and then commercially available HBF4.〇Et2 (1.1 equivalent) was added. The batch was allowed to cool to 2 (rc, cooked for an hour, then an additional 4 parts by volume of solvent was removed by distillation and the slurry was taken to 1 C. The resulting slurry was filtered and the solid was isopropyl acetate. The compound is known as an off-white solid. 1 H NMR (4 〇〇 MHz, fine (4) 6) 5 12·2 (br S, 1H), 817 (cU = 5.2 Hz, 1H), 6.90 (d, J = 4.8) Hi H), 6.81-6.79 (m, 1H), 4.43-4.35 (m, 2H), 3.97-3.83 (m, 5H), 3.82-3.75 143482-1 •162- 201111364 (m,2H), 2.62-2.55 (m, 2H), 0.92-0.83 (m, 3H). HRMS (ES, M+H) calc. 359.1212. Found 359.1237. Step 3: (3R,4S)-2,-methoxy-3,4 ,5,6-tetrahydro-2H-[4,4,]bipyridyl-1,3-di-acid 3-ethyl 1-trifluorodecyl ester 2'-decyloxy-5,6- Dihydro-2H-[4,4']bipyridyl-l,3-dicarboxylic acid 3-ethyl ester 1-trifluorodecyl ester in 2-mercapto THF (6.4 parts by volume) with dioxane ( 1.5 parts by volume) is formulated into a slurry' and HBF4.OEt2 (〇_1 equivalent) is added. The catalyst solution is commercially available bis(2-decylallyl) (COD) Ru(II) (0.01 equivalent) and commercially available (R)-1-[(S)-di-2-furan Phosphino] dicyclopentadienyl iron-yl] -ethyl two - third - butylphosphine (0.0125 eq.) Was dissolved in dioxane gas Yue (0J2 parts by volume) prepared as in 'and added to the slurry. The slurry was then heated to 5 crc and pressurized to 8 bar with hydrogen. After 2 hours of ripening, the batch was cooled to 2 °C. An aqueous solution of NaHCOs (1.5 eq.) was added and the layers were allowed to settle. Flow out of the lower aqueous phase' and discard. The organic layer was washed with a 10% by weight NaCl solution, and the lower aqueous phase was excised and discarded. With respect to the product, the solution was distilled in a vacuum of # to ~2 parts by volume. Then DMF (2 parts by volume) was added, and the resulting solution was used in the next step. HRMS (ES, M+H) calculated 361.1375. Found 361.1367. Step 4. (3R'4S)-r-Methyl-2'-keto-3,4,5,6/,2: hexahydro-2H-[4,4,]bipyridyl-1,3- (3R,4S)4,_methyl-2,keto-3,4,5,6,1' as a solution of 3-ethyl ester of dicarboxylic acid 1-trifluoromethyl ester in DMF/2-MeTHF , 2'-hexahydro-2«:-[4'4']bipyridyl-1,3-dicarboxylic acid 3-ethyl acetate 1-trifluoromethyl ester in a stirred solution, adding triazine iodide Pyrithione (15 equivalents), magnesium hydroxide (1.5 equivalents) and water (1. 〇 equivalent). The slurry was heated to l〇〇t and passed through Ϊ 43482-1 -163- 201111364 for 5 hours and then cooled to ambient temperature. Dioxane (3 parts by volume) and isopropyl acetate (5 parts by volume) were added followed by 4M HCl (2.5 equivalents). Then, the liquid phase was separated and the lower aqueous solution was extracted with dioxane (1·89 parts by volume), and the organic substances were combined. The organic material was washed with a 25% by weight LiCl solution. With respect to the product 'the organic layer was distilled in vacuo to ~5 parts by volume and the product was crystallized. With respect to the product, the distillation was continued to ~2.5 parts by volume, then methyl-tert-butyl ether (1 part by volume) was added, and the slurry was cooled to _3t:, matured for 2 hours, and then filtered. The solid was washed with decyl-tert-butyl ether to give the product as 6.13 (m, 2H), 4.59-4.55 ((m, 0.6H), 4.47-4.40 (m, 0.4H), 4.08-3.95 ( m, 1H), 3.92-3.82 (m, 2H), 3.69-3.53 (m, 0.4H), 3.45-3.25 (m, 4.6H), 3.12-2.95 (m, 1H), 2.34-2.18 (m, 1H ), 1.85-1.75 (m, 1H), 1.03-0.96 (m, 3H). HRMS (ES, M+H) calculated 361.1375. Found 361.1392. Step 5: (3S,4S)-1·-Methyl -2'-keto-3,4,5,6,anthracene,2,-hexahydro-2H-[4,4]bipyridyl-1,3-dicarboxylic acid 1-tris-butyl ester 3R,4S)-1'-mercapto-2'-keto-3,4,5,6,1_,2,-hexahydro-2H-[4,4]bipyridyl-1,3-? Acid 3-ethyl ester 1-trifluorodecyl ester In ethanol (4.1 parts by volume), sodium ethoxide (1.20 equivalents) was added via a sandalwood solution. The mixture was aged for 3 minutes, then water (1.20 equivalents) was added. After 1 hour of aging, b〇c anhydride (1.20 equivalents) was added and the solution was allowed to mature for 1 hour. Sodium hydroxide (2M, 5.00 equivalents) was added and the solution was heated to 70 ° C for 1 hour to cool the mixture. Up to 3 ° C, and concentrate the solution to the volume so that most of the ethanol The solution was washed with MTBE (2.5 parts by volume). The aqueous layer was separated and then acidified with concentrated HCl to give a slurry. Next, 2-mercaptotetrahydrofuran (6 parts by volume) was added, and 143482-1 - 164- 201111364 : - Do not pick up the mixture and then separate the liquid layer. Remove the water layer and collect the material Wu. Then, refill the water layer to the extractor and use MeTHF (2 wound volume) Reverse extraction. The organic fraction was then refilled into an extractor and washed with 50% sodium sulphate/spike. The organic layer was collected and concentrated in vacuo to give a pale yellow solid. The mixture was slurried and stirred at room temperature for 18 hours. The slurry was filtered and washed with EtOAc to give the title compound as an off-white solid. H NMR (5 〇〇MHz, CHa3) : δ 7.30-7.26 (m, 1H), 6.74 (s, 1H), 6.25 (dd, J = 6.96, 2.00 Hz, 1H), 4.44 (s, 1H), 4.30 (s, 1H), 3.52 (s, 3H), 3.09-2.73 (m, 3H), 2.59 (s, 1H), 1.77 (d, J = 13.10 Hz, 1H), 1.61 (d, J = 12.58 Hz, 1H), 1.48 (s, 9H). HRMS (ES, M+H) calc. 337· 1763. Found 337.1768. Example 1 trans-N-cyclopropyl-N-[(2,3-diphenyl)indenyl]-4-(1-methyl-2-keto-1,2-dihydro-4- p is more than decyl)-3-hexahydrop. Fixed amine

MeMe

步驟1 : 4-(4,4,5,5-四曱基-1,3,2- 一氧棚伍圜-2-基)-5,6-二氮 -1,3(2ΗΗ:σ定二叛酸^1,1-二曱基乙基)3-乙酯 於4-{[(三氟曱基)績醯基]氧基卜5,6_二氫-1,3(2H)-吡啶二羧酸 1-(1,1-二甲基乙基)3_乙醋(1當量)與七4,4',4,,5,5,^·-八甲基-2,2,-雙-1,3,2-二氧棚伍圜(1.1當量)之二氧陸圜溶液中’添 加醋酸鉀(3當量)。將此懸浮液抽氣’並以A逆充填。最後’ 以一快速部份添加[丨,1'—雙(二笨基膦基)二環戊二烯鐵]二氯 143482-1 -165- 201111364 鈀(II) (0.03當量)’且將反應懸浮液在8〇〇c下加熱14小時。然 後,藉由添加乙醚與飽*NH4C1水溶液使反應淬滅。分離水 層,並以醚逆萃取。將合併之有機萃液以水與鹽水進一步 洗滌,以Na2S〇4脫水乾燥,過濾,及使濾液在真空中濃縮。 如此獲得之粗產物經由管柱層析之純化(Si〇2,95:5— 8〇:2〇 (v/v)曱苯:Et0Ac) ’獲得標題化合物,為金黃色油。 步驟 2. 2 (甲氧基)_5,6-二虱-4,4’-聯 p比 σ定 _ι,3(2Η)-二叛酸 1_(1,1_二 甲基乙基)3-乙酉旨 於得自前一步驟之4_(4,4,5,5-四曱基_丨,3,2_二氧硼伍圜_2_ 基)-5,6-二氫-1,3(2H)_吡啶二羧酸•二曱基乙基)3乙酯當 量)與芳環1 (1當量)之n-Pr0H溶液(015_中,添加碳酸鈉 (2M水溶液,3當量)。將此懸浮液抽氣,並以^逆充填。 最後,以一快速部份添加[丨芥雙(二苯基膦基)二環戊二烯鐵] 二氣鈀(II) (0.03當量),並將反應懸浮液在8〇t下加熱“小 時。然後,藉由添加乙醚與飽和Ni^Ci水溶液使反應淬滅。 分離水層,且以醚逆萃取。將合併之有機萃液以水與鹽水 進-步洗蘇,以Na2S〇4脫水乾燥’過;慮,及錢液在真空 中濃縮。如此獲得之粗產物經由管柱層析之純化(si〇2, 95:5 (v/v)己烧:EtOAc— EtOAc),獲得標題化合物,為白色固體。 步驟3 ··順式伟(甲氧基)冰峨α定基R3j氮心定二缓酸 1-(1,1-一 T基乙基)3-乙酉旨 於得自前-步驟之2:(甲氧基)_5,6_二氫·44Ι•聯 二缓酸l-(u-二甲基乙基)3-乙醋(1當量)之Me〇H溶液(〇 iM) 中’添加賴屑(3.3當量)1此懸浮液抽氣,並以Ν2逆充 143482-1 -166- 201111364 填。最後’使反應混合物在室溫下音振3.5小時,於此段期 間内鎂鏃屑消失。然後,藉由添加乙鍵與飽和NH4 Cl水溶液 使反應淬滅。分離水層,且以醚逆萃取。將合併之有機萃 液以水與鹽水進一步洗滌,以Naa SO4脫水乾燥,過渡,及 使濾液在真空中濃縮。如此獲得之粗產物經由管柱層析之 純化(Si02 ’ 90:10 (v/v)己烧:EtOAc— EtOAc) ’獲得標題化八 物,為無色油。 魯 步驟4 :反式斗[2-(甲氧基)斗吡啶基]-1,3-六氫吡啶二竣酸 1-(1,1-二曱基乙基)3_乙酯 於得自前一步驟之順式-4-[2-(甲氧基)-4-吡啶基]_],3_六氫 p比啶二羧酸1-(1,1-二曱基乙基)3-乙酯(1當量)之乙醇溶液 (〇,1Μ)中,添加剛製成之乙醇鈉(1.1當量)。將所形成之黃橘 色溶液在55°C下加熱12小時。然後,於真空中移除揮發性 物質’並使殘留物於乙醚與飽和NH4C1水溶液之間作分液處 理。分離水層’且以醚逆萃取。將合併之有機萃液以水與 籲 鹽水進一步洗務,以Na〗SO*脫水乾燥,過濾,及使濾液在 真空中濃縮。如此獲得之粗產物經由管柱層析之純化(si〇2, 90:10 (v/v)己烷:EtOAc— EtOAc),獲得標題化合物,為無色 油0 步驟5:反式_4_(1-甲基-2-酮基-1,2-二氫-4-吡啶基)-1,3-六氫吡啶 二羧酸HU-二曱基乙基)3-乙酯 於得自前一步驟之反式-4-[2-(甲氧基)-4-吡啶基]-1,3-六氫 叶匕°疋一缓酸1-(1,1-一甲基乙基)3-乙醋(1當量)與峨化鈉(3當 量)之乙腈懸浮液(0.1M)中,添加純碘甲烷(3當量)。然後, 143482-1 167. 201111364 將反應容器密封,並在45°C下加熱3天。接著,於真空中移 除揮發性物質’且使殘留物於EtOAc與飽和NH4 C1水溶液之 間作分液處理。分離水層,並以EtOAc逆萃取。將合併之有 機萃液以IN NaOH水溶液、水及鹽水進一步洗滌,以Na2 s〇4 脫水乾燥’過濾’及使濾液在真空中濃縮。如此獲得之粗 產物經由管柱層析之純化(Si〇2,80:20 (v/v)己烷:Et0Ac—Step 1: 4-(4,4,5,5-tetradecyl-1,3,2-oxo-indole-2-yl)-5,6-diaza-1,3 (2ΗΗ: σ定2,1,1-dimercaptoethyl)3-ethyl ester in 4-{[(trifluoromethyl)methyl]oxybu 5,6-dihydro-1,3(2H)- 1-(1,1-dimethylethyl) 3 -ethyl pyridine (1 equivalent) and 7 4,4',4,5,5,^--octamethyl-2,2, - Addition of potassium acetate (3 equivalents) in a solution of bis-1,3,2-dioxane (1.1 equivalents) in dioxane. The suspension was evacuated' and backfilled with A. Finally, add [丨,1'-bis(diphenylphosphino)dicyclopentadienyl]dichloride 143482-1 -165- 201111364 palladium(II) (0.03 equivalent)' in a quick portion and react The suspension was heated at 8 ° C for 14 hours. The reaction was then quenched by the addition of diethyl ether and saturated aqueous NH4CI. The aqueous layer was separated and back extracted with ether. The combined organic extracts were further washed with water and brine, dried over Na 2 EtOAc, filtered, and evaporated. The crude product thus obtained was purified by column chromatography (Si.sub.2, 95:5-8:2 (v/v) benzene: EtOAc (EtOAc)). Step 2. 2 (Methoxy)_5,6-dioxin-4,4'-linked p ratio σ定_ι,3(2Η)-ditrologous acid 1_(1,1-dimethylethyl)3 - 酉 酉 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 2H)-Pyridinedicarboxylic acid (dimercaptoethyl)3 ethyl ester equivalent) and an aromatic ring 1 (1 equivalent) of n-Pr0H solution (015_, added sodium carbonate (2M aqueous solution, 3 equivalents). The suspension is evacuated and filled with reversed. Finally, a portion of [Iridium bis(diphenylphosphino)dicyclopentadienyl]di-palladium(II) (0.03 equivalent) is added in a quick portion and The reaction suspension was heated to "hours" at 8 Torr. The reaction was then quenched by the addition of diethyl ether and a saturated aqueous solution of EtOAc. The aqueous layer was separated and extracted with ether. The combined organic extracts were taken with water and brine. - Step Washing, dehydrated and dried with Na2S〇4; and, and the liquid solution is concentrated in vacuo. The crude product thus obtained is purified by column chromatography (si〇2, 95:5 (v/v) The title compound was obtained as a white solid. Step 3 ··············· Base R3j Nitrogen-densine di-acid 1-(1,1-mono-T-ethyl)3-ethylidene is derived from the pre-step 2: (methoxy)_5,6-dihydro·44Ι• Acid l-(u-dimethylethyl) 3-ethyl vinegar (1 equivalent) in Me〇H solution (〇iM) 'Adding swarf (3.3 eq.) 1 This suspension is pumped and refilled with Ν2 143482-1 -166- 201111364 Fill in. Finally 'The reaction mixture was sonicated at room temperature for 3.5 hours, during which time the magnesium swarf disappeared. Then, the reaction was quenched by adding an ethyl bond with saturated aqueous NH4Cl. The aqueous layer was separated and extracted with ether. The combined organic extracts were further washed with water and brine, dried over Na Na. Purification (Si02 '90:10 (v/v) hexanes: EtOAc - EtOAc) </ </ RTI> </ RTI> </ RTI> </ RTI> </ RTI> </ RTI> </ RTI> 1-(1,1-Dimercaptoethyl) 3 -ethyl 1,3-hexahydropyridine dicarboxylate in cis-4-[2-(methoxy)-4-pyridine obtained from the previous step Base]_],3_hexahydrop-pyridyldicarboxylic acid 1-(1,1-didecyl A solution of 3-ethyl ester (1 equivalent) in ethanol (〇, 1 Μ) was added with freshly prepared sodium ethoxide (1.1 eq.). The resulting yellow orange solution was heated at 55 ° C for 12 hours. The volatiles were removed in vacuo and the residue was partitioned between diethyl ether and saturated aqueous NH.sub.4Cl. The combined organic extracts were further washed with water and brine, dried over Na.sub.SO*, filtered, and concentrated. The crude product thus obtained was purified by column chromatography (EtOAc EtOAc (EtOAc:EtOAc) -Methyl-2-keto-1,2-dihydro-4-pyridyl)-1,3-hexahydropyridinedicarboxylic acid HU-dimercaptoethyl)3-ethyl ester obtained from the previous step Trans-4-[2-(methoxy)-4-pyridyl]-1,3-hexahydroazepine------ 1-(1,1-monomethylethyl) 3-ethylacetate Pure iodomethane (3 equivalents) was added to a suspension of acetonitrile (0.1 M) with sodium hydride (3 eq.). Then, 143482-1 167. 201111364 The reaction vessel was sealed and heated at 45 ° C for 3 days. Next, the volatiles were removed in vacuo and the residue was partitioned between EtOAc and saturated aqueous NH4CI. The aqueous layer was separated and extracted with EtOAc. The combined organic extracts were further washed with aqueous 1 N NaOH, water and brine, dried &lt;RTI ID=0.0&gt;&gt; The crude product thus obtained was purified by column chromatography (Si〇2, 80:20 (v/v) hexane: Et0Ac-

EtOAc— 95:5 (v/v) CH2C12 :在 MeOH 中之 2.0M NH3),獲得標題 化合物,為無色油。 步驟6:反式-1-{[(ι,ΐ-二曱基乙基)氧基]羰基} 4 (1甲基_2酮基 -1,2-二氫-4-p比咬基)-3-六氫p比。定緩酸 於得自前一步驟之反式冰(1-曱基_2_酮基_u·二氫斗吡啶 基)-1,3-六氫吡啶二羧酸L二甲基乙基)3乙酯(1當量)之 3:2 (Wv) THF: MeOH溶液(〇.07M)中,添加氫氧化鋰(1M水溶液, 3.1當量)。將所形成之混濁溶液在室溫下激烈攪拌18小 時。然後,於真空中移除揮發性物質,並使殘留物於Et〇Ac 與10% HC1水溶液之間作分液處理。分離水層,且以Et〇Ac 逆萃取。將合併之有機萃液以水與鹽水進一步洗滌,以 Naz S〇4脫水乾燥,及過濾。濾液在真空中之濃縮,獲得標 題化合物,為白色固體。 步驟7 .反式-3-({環丙基[(2 3·二氣苯基)曱基]胺基}羰基)4 (1_ 曱基-2-酮基-1,2-二氫_4_吡啶基)小六氫吡啶羧酸以-二曱基乙酯 於付自剛一步驟之反式二甲基乙基)氧基]羰基}-4-(1-曱基-2-酮基二氫斗吡啶基)3_六氫吡啶羧酸(1當量)、 Humg氏驗(3當量)及胺1(1當量)之DMF (〇 lM)溶液中,分次 143482-1 201111364 添加六氟磷酸〇_(7_氮苯并三唑小基)_n,n,N',N'_四甲基錁(1.2 當量)。將所形成之反應溶液在室溫下攪拌48小時。將目前 帶紅色溶液以EtOAc稀釋,並以1〇% HC1水溶液、IN NaOH水 溶液及鹽水相繼洗滌。然後,使有機萃液以Na2S04脫水乾 燥’過濾’及使濾液在真空中濃縮,而得黃色油。如此獲 得之粗產物經由急驟式層析之純化(si〇2,7:3 (v/v)己烷:EtOAc-95:5 (v/v) EtOAc (EtOAc) Step 6: trans-1-{[((, ΐ-didecylethyl)oxy)carbonyl} 4 (1 methyl-2-keto-1,2-dihydro-4-p ratio) -3-hexahydrop ratio. The acid is neutralized in the trans step (1-mercapto-2-keto-u-dihydropyridinyl)-1,3-hexahydropyridinedicarboxylic acid L-dimethylethyl) from the previous step. Ethyl acetate (1 eq.) 3:2 (Wv) THF: MeOH solution (.07M), lithium hydroxide (1M aqueous solution, 3.1 eq.). The resulting cloudy solution was vigorously stirred at room temperature for 18 hours. The volatiles were then removed in vacuo and the residue was partitioned between Et EtOAc and 10% EtOAc. The aqueous layer was separated and back-extracted with Et 〇Ac. The combined organic extracts were further washed with water and brine, dried over Naz.sub.4, and filtered. The filtrate was concentrated in vacuo to give title compound as a white solid. Step 7. trans-3-({cyclopropyl[(2 3 ·diphenyl)indolyl]amino}carbonyl)4 (1 - decyl-2-keto-1,2-dihydro-4 _Pyridinyl) small hexahydropyridinecarboxylic acid with -didecylethyl ester in trans-dimethylethyl)oxy]carbonyl}-4-(1-mercapto-2-oneyl) Hydrogen pyridine pyridyl) 3_hexahydropyridinecarboxylic acid (1 equivalent), Humm's test (3 equivalents) and amine 1 (1 equivalent) in DMF (〇lM) solution, fraction 143482-1 201111364 Add hexafluorophosphate 〇_(7-nitrobenzotriazole small group)_n,n,N',N'_tetramethylguanidine (1.2 equivalent). The resulting reaction solution was stirred at room temperature for 48 hours. The current reddish solution was diluted with EtOAc and washed successively with 1% aqueous HCl solution, 1N aqueous NaOH solution and brine. Then, the organic extract was dehydrated to dryness &lt;RTI ID=0.0&gt;&gt; The crude product thus obtained was purified by flash chromatography (si 〇 2, 7:3 (v/v) hexane:

EtOAc— EtOAc— 95:5 (v/v) CH2C12 :在 MeOH 中之 2.0M NH3),獲 ^ 得標題化合物,為白色泡床物。 步驟8 :反式-N-環丙基-N-[(2,3-二氣苯基)甲基]-4-(1-曱基-2-酮 基-1,2-二氫-4-p比咬基)-3-六氫p比π定緩醯胺 於得自前一步驟之反式-3-({環丙基[(2,3-二氯苯基)甲基]胺 基陳基)-4-(1-曱基-2-酮基-l,2-二氫-4-吡啶基)-1-六氫吡啶羧 酸1,1-二曱基乙酯(1當量)之CH2C12溶液(0.05M)中,添加HC1 (4.0M —氧陸圜溶液’ 30當量)。將所形成之溶液在室溫下 攪拌3小時。於真空中移除揮發性物質之後,將所形成之殘 φ 留物直接地裝填至以94:6 (v/v) CH^Cl2 :在MeOH中之2.0M NH3 填充之Si〇2官柱上。以相同溶劑系統之溶離,獲得標題化 合物’為白色泡沫物。MS (ESI+,M+H) : 434。 實例2 反式-N-[{5-氣基-2-[3-(甲氧基)丙基]_4_吡啶基}曱基]_N•環丙基 -4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺 143482-1 -169- 201111364EtOAc - EtOAc - 95:5 (V/V) Step 8: trans-N-cyclopropyl-N-[(2,3-diphenyl)methyl]-4-(1-indol-2-yl-1,2-dihydro-4 -p ratio -3-hexahydrop to π cis hydrazide in trans-3-({cyclopropyl[(2,3-dichlorophenyl)methyl]amino) from the previous step Chen Ji) 1,1-Didecylethyl 4-(1-nonyl-2-keto-l,2-dihydro-4-pyridyl)-1-hexahydropyridinecarboxylate (1 equivalent) In the CH2C12 solution (0.05 M), HCl (4.0 M - oxygen guanidine solution '30 equivalents) was added. The resulting solution was stirred at room temperature for 3 hours. After removing the volatiles in a vacuum, the resulting residue was directly loaded onto a 94:6 (v/v) CH^Cl2: 2.0 M NH3 filled Si 〇 2 column in MeOH. . The title compound was obtained as a white foam by dissolving in the same solvent system. MS (ESI+, M+H): 434. Example 2 trans-N-[{5-Gasyl-2-[3-(methoxy)propyl]_4_pyridyl}indenyl]-N•cyclopropyl-4-(1-methyl-2 -keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide 143482-1 -169- 201111364

根據實例1中所述之程序製成,但替代地使用胺2作為起 始物質°獲得標題化合物,為白色泡沫物。MS (ESI+, M+H): 473。 實例3 反式-N-({2-氣基·5_[3_(曱氧基)丙基]苯基}曱基)_N_環丙基冰(1- _ 甲基-2-酮基-1,2-二氫-4-吡啶基)各六氫吡啶羧醯胺It was made according to the procedure described in Example 1, but instead of using amine 2 as the starting material, the title compound was obtained as a white foam. MS (ESI+, M+H): 473. Example 3 trans-N-({2-carbyl·5_[3_(decyloxy)propyl]phenyl}indenyl)_N_cyclopropyl ice (1- _methyl-2-keto-1 , 2-dihydro-4-pyridyl) each hexahydropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用胺3作為起 始物質。獲得標題化合物,為白色泡沫物。MS (ESI+,M+H): 472 ° 實例4 反式-N-({2-氣基-5-[2-(曱氧基)乙基]苯基}甲基)-N-環丙基-4-(ι_ 曱基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺It was made according to the procedure described in Example 1, but instead using amine 3 as the starting material. The title compound was obtained as a white foam. MS (ESI+, M+H): 472 ° Example 4 trans-N-({2-carbyl-5-[2-(decyloxy)ethyl]phenyl}methyl)-N-cyclopropyl -4-(ι_ decyl-2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用胺4作為起 •170· 143482-1 201111364 始物質。獲得標題化合物,為白色泡沫物。MS (ESI+,M+H): 458。 實例5 反式-N-環丙基-N-({2,3-二氣-5-[3-(甲氧基)丙基]苯基}曱基)-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺It was made according to the procedure described in Example 1, but instead of using amine 4 as the starting material of ?170·143482-1 201111364. The title compound was obtained as a white foam. MS (ESI+, M+H): 458. Example 5 trans-N-cyclopropyl-N-({2,3-dioxa-5-[3-(methoxy)propyl]phenyl}indolyl)-4-(1-indenyl- 2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide

MeMe

根據實例1中所述之程序製成,但替代地使用胺5作為起 始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H): 508。1H NMR (CDC13) δ (ppm) : 0.65-0.68 (m,2H),0.89-0.94 (m,2H), 1-60-1.90 (m, 6H), 2.49-2.63 (m, 3H), 2.76-2.90 (m, 2H), 2.95-3.04 (m, 1H), 3.19-3.24 (m, 1H), 3.27-3.38 (m, 6H), 3.48-3.55 (m, 4H), 4.49 (d, J = 15.6 Hz, 1H), 4.56 (d, J = 15.6 Hz, 1H), 6.05-6.09 (m, 1H), 6.46 (s, 1H), 6.70 (s’ 1H),7‘13 (d,J = 6.9 Hz,1H),7.19 (s, 1H)。人類腎素 IC50(緩 衝劑):0.3 nM。人類腎素ic50(血聚):1.3 nM。 實例6 反式-N-環丙基_N_({2,3-二氣-5-[2-(甲氧基)乙基]苯基}曱 基)-4-(1-甲基_2_酮基-l,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺It was made according to the procedure described in Example 1, but instead of using amine 5 as the starting material. The title compound was obtained as a white foam. </ RTI> <RTIgt; 2.49-2.63 (m, 3H), 2.76-2.90 (m, 2H), 2.95-3.04 (m, 1H), 3.19-3.24 (m, 1H), 3.27-3.38 (m, 6H), 3.48-3.55 (m , 4H), 4.49 (d, J = 15.6 Hz, 1H), 4.56 (d, J = 15.6 Hz, 1H), 6.05-6.09 (m, 1H), 6.46 (s, 1H), 6.70 (s' 1H) , 7'13 (d, J = 6.9 Hz, 1H), 7.19 (s, 1H). Human renin IC50 (buffer): 0.3 nM. Human renin ic50 (blood aggregation): 1.3 nM. Example 6 trans-N-cyclopropyl_N_({2,3-dioxa-5-[2-(methoxy)ethyl]phenyl}indolyl)-4-(1-methyl-2- -keto-l,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用胺6作為起 143482-1 -171 - 201111364 始物質。獲得標題化合物,為無色油。MS (ESI+,M+H): 492。 實例7 反式-N-環丙基_N_(丨2_甲基·5_[3 (曱氧基)丙基]苯基}曱基 曱基-2-酮基-ΐ,2-二氫_4_吡啶基)冬六氫吡啶羧醯胺It was made according to the procedure described in Example 1, but instead of using amine 6 as the starting material from 143482-1 -171 - 201111364. The title compound was obtained as a colorless oil. MS (ESI+, M+H): 492. Example 7 trans-N-cyclopropyl_N_(丨2_methyl·5_[3(decyloxy)propyl]phenyl}indolyl-2-yl-yl-indole, 2-dihydro_ 4_pyridyl) winter hexahydropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用胺7作為起 始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, Μ+Η): 452。 實例8 反式-Ν-環丙基_Ν_({2_甲基_5-[2-(甲氧基)乙基;|苯基}甲基) 甲基-2-酮基-l,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺It was made according to the procedure described in Example 1, but instead of using amine 7 as the starting material. The title compound was obtained as a white foam. MS (ESI+, Μ+Η): 452. Example 8 trans-Ν-cyclopropyl_Ν_({2_methyl_5-[2-(methoxy)ethyl;|phenyl}methyl)methyl-2-keto-l,2 -dihydro-4-pyridyl)-3-hexahydropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用胺8作為起 始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, Μ+Η): 438。 實例9 反式-N-環丙基-N-({2,3-二氟-5-[3-(甲氧基)丙基]苯基}甲基)_ 4_(1-曱基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺 143482-1 • 172- 201111364It was made according to the procedure described in Example 1, but instead using amine 8 as the starting material. The title compound was obtained as a white foam. MS (ESI+, Μ+Η): 438. Example 9 trans-N-cyclopropyl-N-({2,3-difluoro-5-[3-(methoxy)propyl]phenyl}methyl)_ 4_(1-indolyl-2 -keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide 143482-1 • 172- 201111364

根據實例1中所述之程序製成,但替代地使用胺9作為起 始物貝獲传仏通化合物’為白色泡末物。MS (ESI+, M+H): 474。 實例10It was prepared according to the procedure described in Example 1, but instead using amine 9 as the starting material, the compound was white foam. MS (ESI+, M+H): 474. Example 10

反式-N-環丙基_4-(1_甲基_2-酮基-l,2-二氫-4-吡啶基)-N-({3-(曱 氧基)-5-[3-(甲氧基)丙基]苯基丨甲基)各六氫吡啶羧醯胺trans-N-cyclopropyl_4-(1-methyl-2-keto-l,2-dihydro-4-pyridyl)-N-({3-(decyloxy)-5-[ 3-(methoxy)propyl]phenylindolemethyl)hexahydropyridine carboxamide

MeMe

根據會例1中所述之程序製成,但替代地使用胺10作為 起始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 468。 實例11 反式-N-環丙基-4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)-N-({3-{[2-(甲氧基)乙基]氧基}-5-[3-(曱氧基)丙基]苯基)甲基)-3-六氫吡 啶羧醯胺 V8It was prepared according to the procedure described in Example 1, but using amine 10 as a starting material instead. The title compound was obtained as a white foam. MS (ESI+, M+H): 468. Example 11 trans-N-cyclopropyl-4-(1-methyl-2-keto-1,2-dihydro-4-pyridyl)-N-({3-{[2-(methoxy) Ethyl]oxy}-5-[3-(decyloxy)propyl]phenyl)methyl)-3-hexahydropyridine carboxamide V8

143482-1 -173 201111364 根據實例1中所述之程序製成,但替代地使用胺11作為起 始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H): 512。 實例12 反式-N-環丙基-4-(1-乙基_2_酮基4,2-二氫-4-吡啶基)-N-({3-{[2-(曱氧基)乙基]氧基}-5-[3-(甲氧基)丙基]苯基}甲基)-3-六氫p比 啶羧醯胺143482-1 -173 201111364 was prepared according to the procedure described in Example 1, but using amine 11 as the starting material instead. The title compound was obtained as a white foam. MS (ESI+, M+H): 512. Example 12 trans-N-cyclopropyl-4-(1-ethyl-2-keto 4,2-dihydro-4-pyridyl)-N-({3-{[2-(oximeoxy) Ethyl]oxy}-5-[3-(methoxy)propyl]phenyl}methyl)-3-hexahydrop-pyridinium carboxamide

步驟1: 5,6-二氫-4,4,-聯吡啶-1,3(2H)-二羧酸1-(1,1-二甲基乙基)3_ 乙酯 於4 {[(一氟甲基)¾酿基]氧基}-5,6-二氫-l,3(2H)-p比。定二缓酸 1_(1’丨_一甲基乙基)3-乙醋(1當量)與4-ρ比。定基二經基石朋院(1 1 當量)之1:1 (ν/ν)乙醇:曱苯溶液(018M)中,添加碳酸鈉(2Μ 水溶液,2.6當量)。將此懸浮液抽氣,並以Ν〗逆充填。最 後,以一快速部份添加肆(三苯膦)鈀⑼(〇 〇4當量),且將反 應懸浮液在8(TC下加熱18小時。然後,以飽和Nh4C1水溶液Step 1: 5,6-Dihydro-4,4,-bipyridine-1,3(2H)-dicarboxylic acid 1-(1,1-dimethylethyl)3_ethyl ester in 4 {[(1 Fluoromethyl) 3⁄4 aryl]oxy}-5,6-dihydro-l,3(2H)-p ratio. The acid is 1 - (1' 丨 - monomethyl ethyl) 3-ethyl vinegar (1 equivalent) and the ratio of 4-ρ. Sodium carbonate (2 水溶液 aqueous solution, 2.6 eq.) was added to a solution of 1:1 (ν/ν) ethanol: benzene solution (018 M) in a base stone base (1 1 eq.). The suspension was evacuated and backfilled with Ν. Finally, ruthenium (triphenylphosphine)palladium (9) (〇4 equivalent) was added in a quick portion, and the reaction suspension was heated at 8 (TC for 18 hours. Then, a saturated Nh4C1 aqueous solution was used.

80:20 (v/v)己烧:EtOAc— EtOAc), 色油。 143482-1 -174- 201111364 步驟2 ’·順式-4-(4-卩比η定某3 _x_ g ,、 吞J,乂、虱吡啶二羧酸1-(1,1-二曱基乙 基)3-乙酯 於得自前一步驟之5,6-二 氫-4,4’-聯吡啶-i,3(2H&gt;二羧酸80:20 (v/v) hexane: EtOAc - EtOAc. 143482-1 -174- 201111364 Step 2 '· cis-4-(4-卩 ratio η 定3 _x_ g , , 吞 J, 乂, 虱 pyridine dicarboxylic acid 1-(1,1-didecyl B 3-ethyl ester in 5,6-dihydro-4,4'-bipyridine-i,3 (2H&gt; dicarboxylic acid from the previous step

HU 一甲基乙基)3·乙酷(1當量)之Me〇H溶液①_中添加 鎮镟屑(3當量)。將此懸浮液抽氣,並以N2逆充填。最後, 使反應混合物在室溫下音振2小時,於此段期間内鎮鐵屑消 失。然後,藉由添加Et0Ac與1NNa〇H水溶液使反應淬滅。 分離水層’ JiiXEtOAe逆萃取。將合併之有機萃液以水與鹽 水進-步洗蘇,以Na2s〇4脫水錢m纽在真空 中之濃縮’獲得標題化合物,為金黃色油。 步驟3 :反式斗(4-吡啶基H,3_六氫吡啶二_ -二曱基乙 基)3-乙酯 於得自前一步驟之順式-4-(4-吡啶基H,3_六氫吡啶二羧酸 ι-(ι,ι-二甲基乙基)3·乙醋(1當量)之乙醇溶液(〇 4m)中添加 剛製成之乙醇鈉(u當量)。將所形成之黃橘色溶液在6〇t 下加熱12小時。然後,於真空中移除揮發性物質,並使殘 留物於EtOAc與飽和溶液之間作分液處理。分離水 層,且以EtOAc逆萃取。將合併之有機萃液以水與鹽水進一 步洗滌,以NazSO4脫水乾燥,以活性炭處理,過濾,及使 濾液在真空中濃縮。如此獲得之粗產物經由管桎層析之純 化(Si〇2,80:20 (v/v)己烷:Et0Ac_&gt; Et0Ac),獲得標題化合物, 為淡黃色油。 步驟4 :反式-4-(1-氧化-4-吡啶基)-1,3-六氫吡啶_ 、〜疋—羧酸-二 甲基乙基)3-乙酯 143482·】 -175- 201111364An antimony crumb (3 equivalents) was added to the Me〇H solution 1_ of HU monomethylethyl) 3 · ethyl (1 equivalent). The suspension was evacuated and backfilled with N2. Finally, the reaction mixture was sonicated at room temperature for 2 hours during which time the iron filings disappeared. The reaction was then quenched by the addition of Et0Ac and 1NN aq. Separate the water layer ' JiiXEtOAe back extraction. The combined organic extracts were washed with water and brine, and the title compound was obtained from EtOAc. Step 3: trans-bucket (4-pyridyl H,3-hexahydropyridine bis-didecylethyl) 3-ethyl ester in cis-4-(4-pyridyl H,3 from the previous step Add sodium ethoxide (u equivalent) freshly prepared to a solution of hexahydropyridine dicarboxylic acid ι-(ι,ι-dimethylethyl) 3 · vinegar (1 eq.) in ethanol (〇4m). The resulting yellow-orange solution was heated at 6 Torr for 12 hours. Then the volatiles were removed in vacuo and the residue was partitioned between EtOAc and sat. The combined organic extracts are further washed with water and brine, dried over NazSO4, treated with activated carbon, filtered, and concentrated in vacuo. The crude product thus obtained is purified by column chromatography (Si〇2) , 80:20 (v/v) hexane: Et0Ac_&gt; Et0Ac) to give the title compound as pale yellow oil. Step 4: trans-4-(1-oxo-4-pyridyl)-1,3-hexa Hydropyridine _, ~ hydrazine-carboxylic acid-dimethylethyl) 3-ethyl ester 143482 ·] -175- 201111364

於得自前一步驟之反式-4-(4-p比咬基)-1,3-六氣p比〇定-鼓西交 HU-二曱基乙基)3-乙酯(1當量)之二氣曱烷溶液(0.1M)中, 添加3-氣基過氧苯曱酸(1當量)。將所形成之無色溶液在室 溫下攪拌13小時。然後,以飽和NaHS03水溶液與1N Na〇H 水溶液使反應淬滅。分離水層,並以EtO Ac逆萃取。將合併 之有機萃液以水與鹽水進一步洗滌,以Na2S04脫水乾燥, 及過濾。濾液在真空中之濃縮’獲得標題化合物,為白色 固體。 步驟5:反式-4-(1-乙基-2-酮基-1,2-二氫-4-吡啶基)_ι,3_六氫?比咬 二羧酸1-(1,1-二甲基乙基)3-乙酯 於得自前一步驟之反式-4-(1-氧化斗吡啶基^义六氫峨咬 二羧酸1-(1,1-二甲基乙基)3-乙酯(1當量)之曱苯溶液(〇 〇6m) 中,添加三乙胺(3當量)。其中將反應容器浸沒在冰水浴中, 逐滴添加純三氟醋酸酐(3當量),歷經5分鐘期間。使所形 成之黃色溶液慢慢地溫熱至室溫,然後將其在室溫下攪拌 18小時。藉由添加Et0Ac與飽和NH4C1水溶液使反應淬滅。 分離水層,並以Et0Ac逆萃取。將合併之有機萃液以水與鹽 水進一步洗滌,以NhSO4脫水乾燥,過濾,及使濾液在真 空中濃縮。使如此獲得之膠黏橘色油立即溶於乙醇(〇im) 中。然後,於其中,在〇°C下,添加氩氧化鈉(2M水溶液,3 當量)與硫酸二乙醋(4當量)。使所形成之橘色溶液慢慢地 溫熱至室S ’接著,將其在室溫下攪拌42小時。於真空中 移除揮發性㈣,並使殘留物於£與水之間作分液處 理。分離水層’且以職e逆萃取。將合併之有機萃液以水 143482-1 -176- 201111364 與鹽水進一步洗滌,以Na2S〇4脫水乾燥,過濾,及使濾液 在真空中濃縮。如此獲得之粗產物經由管柱層析之純化 (Si02,95:5 (v/v) CH2 Cl2 ··在 MeOH 中之 2雇 NH3),獲得標題 化合物,為淡黃色泡珠物。 步驟6 :反式-H[(U•二f基乙基)氧基]羰基} 4 (1乙基_2酮基 -1,2-二氫-4-吡啶基)-3-六氫吡啶羧酸 於得自前一步驟之反式斗(1_乙基冬酮基二氫_4_吡啶 基)1,3-八氫!:比咬二叛酸^(丨丨二甲基乙基)3乙酯(1當量)之 3:2 (V/V) THF: MeOH溶液(0·07Μ)中,添加氫氧化鋰(1M水溶液, 3.1當量)。將所形成之混濁溶液在室溫下激烈攪拌18小時。 然後,於真空中移除揮發性物質,並使殘留物於Et〇Ac與1〇% HC1水洛液之間作分液處理。分離水層,且以段〇逆萃取。 將合併之有機萃液以水與鹽水進一步洗滌,以脫水 乾燥,及過濾。濾液在真空中之濃縮,獲得標題化合物, 為白色固體。 步驟7:反式-3-{[環丙基({3][2_(曱氧基)乙基]氧基卜5_丨&gt;(曱氧 基)丙基]苯基}甲基)胺基]幾基}·4_(1_乙基_2_酮基_u二氫冬吡 啶基)-1-六氫吡啶羧酸u-二曱基乙酯 於得自前一步驟之反式_H[(U_二甲基乙基)氧基]羰基}_ 4-(1-乙基-2-酮基二氫斗吡啶基)冬六氫吡啶羧酸(1當量)、 Humg氏鹼(3當量)及胺U (1當量)之DMF溶液中,分次添加 六氟磷酸0-(7-氮笨并三唑小基)_N,N,N,,N,_四甲基錁〇 2當 量)。將所形成之反應溶液在室溫下攪拌48小時。將目前帶 紅色溶液以EtOAc稀釋,並以1〇% Ηα水溶液、m Na〇H水溶 143482-1 -177- 201111364 液及鹽水相繼洗滌。然後,使有機萃液以Na2S〇4脫水乾燥, 過濾,及使濾液在真空中濃縮,而得黃色油。如此獲得之 粗產物經由急驟式層析之純化(Si〇2,7:3 (v/v)己烷:Et〇Ac_Trans-4-(4-p ratio)-1,3-hexa-p-p-rhenidine--------------------------- In the dioxane solution (0.1 M), 3-oxoperoxybenzoic acid (1 equivalent) was added. The resulting colorless solution was stirred at room temperature for 13 hours. The reaction was then quenched with saturated aqueous NaHS03 and 1N aqueous NaH. The aqueous layer was separated and back-extracted with EtO Ac. The combined organic extracts were further washed with water and brine, dried over Na 2 SO 4 and filtered. The filtrate was concentrated in vacuo to give the title compound as a white solid. Step 5: trans-4-(1-ethyl-2-keto-1,2-dihydro-4-pyridyl)_ι,3_hexahydro? 1-(1,1-dimethylethyl)3-ethyl ester of dicarboxylic acid in trans--4-(1-piperidinylpyridinyl hexahydroindole dicarboxylic acid 1 obtained from the previous step To a solution of -(1,1-dimethylethyl)3-ethyl ester (1 equivalent) in benzene (〇〇6m), triethylamine (3 equivalents) was added, and the reaction vessel was immersed in an ice water bath. Pure trifluoroacetic anhydride (3 eq.) was added dropwise over a period of 5 min. The resulting yellow solution was slowly warmed to room temperature and then stirred at room temperature for 18 h. by Et0Ac and sat. The aqueous solution was quenched with aqueous NH4C1. The aqueous layer was separated and extracted with Et0Ac. The combined organic extracts were further washed with water and brine, dried over NhSO4, filtered, and concentrated in vacuo. The sticky orange oil was immediately dissolved in ethanol (〇im), and then, sodium argon (2M aqueous solution, 3 equivalents) and diethyl sulfate (4 equivalents) were added at 〇 ° C. The orange solution was slowly warmed to chamber S'. Then, it was stirred at room temperature for 42 hours. The volatiles were removed in vacuo and the residue was left. Separate between water and water. Separate the water layer' and carry out reverse extraction with the job. The combined organic extracts are further washed with water 143482-1 -176- 201111364 with brine, dehydrated with Na2S〇4, filtered And the filtrate is concentrated in vacuo. The crude product obtained is purified by column chromatography (SiO2, 95:5 (v/v) CH2Cl2. Light yellow vesicles. Step 6: trans-H[(U•dif-ethyl)oxy]carbonyl} 4 (1 ethyl-2-keto-1,2-dihydro-4-pyridyl) -3- Hexahydropyridinecarboxylic acid in the counter-step (1_ethylbutanyldihydro-4-pyridyl)1,3-octahydro! from the previous step!: than biting two oxic acid ^ (丨丨3:2 (V/V) of dimethylethyl)3 ethyl ester (1 equivalent) in THF: MeOH solution (0·07 Torr), lithium hydroxide (1 M aqueous solution, 3.1 eq.) was added. The solution was stirred vigorously for 18 hours at room temperature. Then, the volatiles were removed in vacuo, and the residue was partitioned between Et 〇Ac and 1 〇% HCl. The aqueous layer was separated and Segmental reversal extraction. Combined organic extracts It is further washed with water and brine, dried over water, and filtered, and filtered. The filtrate is concentrated in vacuo to give the title compound as a white solid. Step 7: trans-3-{[cyclopropyl({3][2_(曱Oxy)ethyl]oxybu 5_丨&gt;(decyloxy)propyl]phenyl}methyl)amino]]yl}·4_(1_ethyl_2-keto-u dihydrogen U-dimercaptoethyl ester of winter pyridyl)-1-hexahydropyridinecarboxylate in the trans-_H[(U-dimethylethyl)oxy]carbonyl}_ 4-(1- obtained from the previous step Addition of hexafluorophosphate to the DMF solution of ethyl-2-ketodihydropyridinyl) winter hexahydropyridinecarboxylic acid (1 equivalent), Humg's base (3 equivalents) and amine U (1 equivalent) -(7-aza-benzotriazole small group)_N,N,N,,N,_tetramethylguanidine 2 equivalents). The resulting reaction solution was stirred at room temperature for 48 hours. The current reddish solution was diluted with EtOAc and washed successively with 1% aqueous solution of Ηα, m Na〇H water soluble 143482-1 -177- 201111364 and brine. Then, the organic extract was dried over Na 2 SO 4 , filtered, and the filtrate was concentrated in vacuo to give a yellow oil. The crude product thus obtained is purified by flash chromatography (Si〇2, 7:3 (v/v) hexane: Et 〇Ac_

EtOAc— 95:5 (v/v) CH2C12 :在 MeOH 中之 2.0M NH3),獲得標題 化合物,為白色泡泳物。 步驟8 :反式-N-環丙基-4-(1-乙基酮基-i,2-二氫-4-吡啶基)_ N-({3-{[2-(曱軋基)乙基]氧基}-5-[3-(曱氧基)丙基]苯基丨曱基)_3· 六氫峨。定缓醯胺 於得自前一步驟之反式-3-{[環丙基({3-{[2-(曱氧基)乙基]氧籲 基}-5-[3-(甲氧基)丙基]苯基}曱基)胺基擒基卜4_(1_乙基_2酮 基-1,2-二氫-4-吡啶基)-1-六氫吡啶羧酸丨,;^二曱基乙酯(1當 量)之(¾¾溶液(0.07M)中,添加HC1 (4·0Μ二氧陸園溶液, 30當量)。將所形成之溶液在室溫下攪拌3小時。於真空中 移除揮發性物質之後,將所形成之殘留物直接地裝填至以 93:7 (v/v) CH2C12 :在 MeOH 中之 2.0Μ ΝΗ3 填充之 Si02 管柱上。 以相同溶劑系統之溶離’獲得標題化合物,為白色泡沫物。 MS (ESI+,M+H) : 526。人類腎素IQ〆緩衝劑):200 nM。人類® 腎素 IC50(血漿):460 nM。 實例13 反式-N-環丙基-N-({3-{[2-(甲氧基)乙基]氧基卜5-[3-(曱氧基)丙 基]苯基}曱基)-4-(1,5,6-三曱基-2-酮基-1,2-二氫-4-吡啶基)_3_六 氫吡啶羧醯胺 143482-1 -178- 201111364EtOAc-95:5 (v/v) <RTI ID=0.0></RTI> <RTIgt; </RTI> <RTIgt; Step 8: trans-N-cyclopropyl-4-(1-ethylketo-i,2-dihydro-4-pyridyl)_N-({3-{[2-(曱)) Ethyl]oxy}-5-[3-(decyloxy)propyl]phenylindenyl)_3·hexahydroindole. Cyclohexylamine in trans-3-{[cyclopropyl({3-{[2-(decyloxy)ethyl)oxy)}-5-[3-(methoxy) from the previous step )propyl]phenyl}indolyl)aminoindolyl 4_(1-ethyl-2-keto-1,2-dihydro-4-pyridyl)-1-hexahydropyridinecarboxylate; To the solution of dimercaptoethyl ester (1 eq.) (3⁄4⁄4⁄4 solution (0.07M), add HCl (4.00 dioxin solution, 30 equivalents). The resulting solution was stirred at room temperature for 3 hours. After removing the volatiles, the resulting residue was directly loaded onto a SiO2 column packed with 93:7 (v/v) CH2C12: 2.0 Μ3 in MeOH. Dissolution from the same solvent system' The title compound was obtained as a white foam. MS (ESI+, M+H): 526. Human renin IQ buffer: 200 nM. Human® Renin IC50 (plasma): 460 nM. Example 13 trans-N-cyclopropyl-N-({3-{[2-(methoxy)ethyl]oxybu 5-[3-(decyloxy)propyl]phenyl}fluorenyl )-4-(1,5,6-tridecyl-2-keto-1,2-dihydro-4-pyridyl)_3_hexahydropyridine carboxamide 143482-1 -178- 201111364

步驟1 : 2',3’-二曱基-6,_[(苯基甲基)氧基]_5,6_二氫_4,4,聯吡啶 -1,3(2H)-二缓酸1-(1,1-二曱基乙基)3·乙酯 於4-(4,4,5,5-四甲基_1,3,2_二氧硼伍圜_2·基)_5,6二氫·j,抑印_ 吡啶二羧酸1-U,1-二曱基乙基)3_乙醋(1當量,實例卫步驟工) • 與芳環2(1當量)之3:1(v/v)甲苯:乙醇溶液(〇·〇85Μ)*,添加 碳酸鈉(2Μ水溶液,3當量)。將此懸浮液抽氣,並以化逆 充填。最後,以一快速部份添加队^雙(二苯基膦基)二環戊 二烯鐵]二氣鈀(II) (0.06當量),且將反應懸浮液在8〇&lt;t下加 熱18小時。然後,藉由添加乙醚與飽和ΝΗ4α水溶液使反應 淬滅。分離水層,並以醚逆萃取。將合併之有機萃液以水 與鹽水進一步洗滌,以N^SO4脫水乾燥,過濾,及使濾液 在真空中濃縮。如此獲得之粗產物經由管柱層析之純化 鲁(Si02 ’ 95:5 (v/v)己烧:EtOAc— 70:30 (Wv) EtOAc :己烧),獲得 標題化合物,為無色油。 步驟2 ··順式-4-〖2,3-二曱基_6-[(苯基曱基)氧基]_4_吡啶基}_13_ 六氫p比咬二羧酸1-(1,1-二甲基乙基)3_乙酯 於得自前一步驟之2,,3,-二甲基-6,-[(苯基曱基)氧基]_5,6_二 氫-4,4·-聯峨啶-1,3(2H)-二綾酸ΐ-(ι,ΐ-二甲基乙基)3-乙酯(1當 量)之MeOH溶液(〇·〇9Μ)中’添加鎂鎚屑(3.3當量)。將此懸 浮液抽氣’並以N2逆充填。最後,使反應混合物在室溫下 143482-1 •179- 201111364 音振3小時’於此段期間内鎂镟屑消失。然後,藉由添加乙 醚與飽和NH4 C1水溶液使反應淬滅。分離水層,且以醚逆萃 取。將合併之有機萃液以水與鹽水進一步洗滌,以Na2 S04 脫水乾燥’過濾,及使濾液在真空中濃縮。如此獲得之粗 產物經由管柱層析之純化(Si〇2,95:5 (v/v)己烷:EtOAc— 1:1 (v/v)己烧.EtOAc) ’獲得標題化合物,為淡黃色油。 步驟3 :反式-4-(2,3-二曱基-6-[(苯基甲基)氧基]-4-峨啶基}-1,3-六氫吡啶二羧酸1-(1,1-二甲基乙基)3_乙酯 於得自前一步驟之順式-4-(2,3-二曱基-6-[(苯基曱基)氧基]-4-p比。定基}-1,3-六氫峨啶二羧酸二甲基乙基)3_乙酯(1當 量)之乙醇溶液(0.1Μ)中’添加剛製成之乙醇鈉(1.2當量)。 將所形成之黃橘色溶液在55°C下加熱16小時。然後,於真 空中移除揮發性物質,並使殘留物於Et0Ac與飽和nh4C1水 溶液之間作分液處理。分離水層,且以Et〇Ac逆萃取。將合 併之有機萃液以水與鹽水進一步洗滌,以Na2 s〇4脫水乾燥, 過渡’及使濾液在真空中濃縮。如此獲得之粗產物經由管 柱層析之純化(Si〇2,90:10 (v/v)己烷:EtOAc— 1:1 (Wv)己烷: EtOAc) ’獲得標題化合物’為淡黃色油。 步驟4:反式-4-(6-羥基_2,3-二曱基-4-吡啶基)-1,3-六氫吡啶二羧 酸1-(1,1-二曱基乙基)3_乙酯 於得自前一步驟之反式冰{2,3-二曱基-6-[(苯基曱基)氧基]_ 4-p比咬基}-1,3-六氫吡啶二羧酸二甲基乙基)3•乙酯(1當 量)之乙醇溶液(〇·07Μ)中,添加鈀(1〇% w/w,於碳上,〇3當 篁)。將所形成之懸浮液抽氣,並以氫滌氣。在經充填氫大 143482-1 -180- 201111364 氣之氣瓶下,將反應混合物於室溫下攪拌2小時。然後,以 CH2C12使反應淬滅,經過矽藻土床過濾,並將不溶物以Step 1: 2',3'-Dimercapto-6,_[(phenylmethyl)oxy]_5,6-dihydro-4,4,bipyridin-1,3(2H)-dibasic acid 1-(1,1-Dimercaptoethyl)3·ethyl ester in 4-(4,4,5,5-tetramethyl-1,3,2-dioxaboron-2-yl)_5 ,6 dihydrogen·j, imprinting _ pyridine dicarboxylic acid 1-U,1-didecylethyl) 3 -ethyl vinegar (1 equivalent, example wei step) • 3 with aromatic ring 2 (1 equivalent) : 1 (v/v) Toluene: Ethanol solution (〇·〇85Μ)*, sodium carbonate (2 Μ aqueous solution, 3 equivalents) was added. The suspension was evacuated and refilled. Finally, a group of bis(diphenylphosphino)dicyclopentadienyl]digas palladium (II) (0.06 equivalents) was added in a quick portion, and the reaction suspension was heated at 8 Torr &lt;t 18 hour. Then, the reaction was quenched by the addition of diethyl ether and a saturated aqueous solution of EtOAc. The aqueous layer was separated and back extracted with ether. The combined organic extracts were further washed with water and brine, dried over Naz. The crude product thus obtained was purified by column chromatography eluting elut elut elut elut elut eluting Step 2 ·· cis-4-〖2,3-dimercapto_6-[(phenylindenyl)oxy]_4_pyridyl}_13_ hexahydrop than biting dicarboxylic acid 1-(1,1 -Dimethylethyl)3_ethyl ester from 2,3,-dimethyl-6,-[(phenylindenyl)oxy]_5,6-dihydro-4,4 from the previous step Adding magnesium to hydrazine solution (峨·〇9Μ) in a solution of hydrazine-1,3(2H)-bismuth bismuthate-(I, dimethyl-dimethyl 3-ethyl 3-ethyl ester (1 eq.) Hammer (3.3 equivalents). The suspension was evacuated&apos; and backfilled with N2. Finally, the reaction mixture was allowed to vibrate for 3 hours at room temperature 143482-1 •179-201111364. During this period, the magnesium swarf disappeared. The reaction was then quenched by the addition of diethyl ether and saturated aqueous NH4CI. The aqueous layer was separated and extracted with ether. The combined organic extracts were further washed with water and brine, dried over Na. The crude product thus obtained was purified by column chromatography (EtOAc: EtOAc: EtOAc: 1:1 (v/v) Yellow oil. Step 3: trans-4-(2,3-dimercapto-6-[(phenylmethyl)oxy]-4-indolyl}-1,3-hexahydropyridinedicarboxylic acid 1-( 1,1-Dimethylethyl)3_ethyl ester in cis-4-(2,3-dimercapto-6-[(phenylindenyl)oxy]-4-p from the previous step Adding freshly prepared sodium ethoxide (1.2 equivalents) to an ethanol solution (0.1 Å) of a fixed amount of 1-1,3-hexahydroacridine dicarboxylic acid dimethylethyl) 3 - ethyl ester (1 equivalent) The resulting yellow-orange solution was heated at 55 ° C for 16 hours. Then, the volatiles were removed in vacuo and the residue was partitioned between Et0Ac and saturated aqueous nh 4 C1. And the combined organic extracts were further washed with water and brine, dried over Na 2 s 〇 4, and then allowed to pass, and the filtrate was concentrated in vacuo. The crude product thus obtained was subjected to column chromatography. Purification (Si 〇 2, 90:10 (v/v) hexanes: EtOAc - 1:1 (Wv) hexanes: EtOAc. 1-hydroxy-1,3-dimercapto-4-pyridyl)-1,3-hexahydropyridinedicarboxylic acid 1-(1,1-dimercaptoethyl) 3 -ethyl ester Trans-ice {2,3-dimercapto-6-[(phenylindenyl)oxy]- 4-p-bityl}-1,3-hexahydropyridinedicarboxylic acid dimethyl from the previous step Palladium (1〇% w/w, on carbon, 〇3 as 篁) was added to an ethanol solution (〇·07Μ) of ethyl)3•ethyl ester (1 eq.). The resulting suspension was evacuated and purged with hydrogen. The reaction mixture was stirred at room temperature for 2 hours under a gas cylinder filled with hydrogen 143482-1 -180 - 201111364. Then, the reaction is quenched with CH2C12, filtered through a bed of diatomaceous earth, and the insoluble matter is

EtOAc沖洗。濾液在真空中之濃縮,獲得標題化合物,為白 色固體。 步驟5 :反式-4-(l,5,6-三甲基_2·酮基二氫斗吡啶基H,3-六 氫吡啶二羧酸HU-二曱基乙基)3_乙醋 於得自前一步驟之反式斗(6_羥基_2,3_二曱基斗吡啶基)_ U-六氫吡啶二羧酸1-(U-二甲基乙基)3_乙酯(1當量)與氫化 鈉(於油中之60%分散液,2當量)之DMF懸浮液(〇liM)中, 添加碘甲烷(1.5當量)。然後,將所形成之混合物在室溫下 攪拌18小時。藉由添加EtOAc與飽和NH4C1水溶液使反應淬 滅。分離水相,並以EtOAc逆萃取。將合併之有機萃液以水 與鹽水相繼洗滌,以N^SO4脫水乾燥,過濾,及使濾液在 真空中濃縮。如此獲得之粗產物經由管柱層析之純化(si〇2, 95:5 (V/V) CH2C12 :在MeOH中之2.0M NH3),獲得標題化合物, 為淡黃色泡沫物。 步驟6:反式-H[(U_二曱基乙基)氧基]叛基} 4 (15,6三甲基·2_ 酮基-1,2-二氫-4-P比咬基)-3-六氫it比。定缓酸 於得自前一步驟之反式-4-(l,5,6-三甲基-2-酮基4,2-二氫-4-口比疋基)-1,3-六氫ντ比。疋一叛酸1-(1,1-二曱基乙基)3_乙酷(;[當 量)之3:2 (v/v) THF : MeOH溶液(0.07M)中,添加氫氧化鋰(1M 水溶液,11當量)^將所形成之混濁溶液在室溫下激烈攪 拌18小時。然後,於真空中移除揮發性物質,並使殘留物 於EtOAc,10% HC1水溶液之間作分液處理。分離水層,且 143482-1 -181 - 201111364 以EtOAc逆萃取。將合併之有機萃液以水與鹽水進一步洗 滌,以NasSCXj脫水乾燥,及過濾。濾液在真空中之濃縮, 獲得標題化合物,為白色固體。 步驟7 .反式-3-{[環丙基({3-{[2-(甲氧基)乙基]氧基卜5_[3·(曱氧 基)丙基]笨基}甲基)胺基]欺基卜4_(15,6三曱基·2·酮基_12_二 氩-4-吡啶基)-1-六氫吡啶羧酸u_二曱基乙酯 於得自前一步驟之反式二甲基乙基)氧基]幾基卜 4-(1,5,6-二曱基-2-酮基-l,2-二氫-4-P比。定基)_3_六氫?比定敌酸(1 當量)、Hunig氏驗(3當量)及胺11 (1當量)之dmf (0.1M)溶液 中’分次添加六氟J鱗酸〇-(7-氮苯并三。坐小基)_ν,ν,Ν',Ν'-四曱 基錁(1.2當量)。將所形成之反應溶液在室溫下授拌48小時。 將目前帶紅色溶液以EtOAc稀釋,並以1〇% HC1水溶液、in NaOH水溶液及鹽水相繼洗滌。然後,使有機萃液以Na2S〇4 脫水乾燥’過濾’及使濾液在真空中濃縮,而得黃色油。 如此獲得之粗產物經由急驟式層析之純化(Si〇2,7:3 (v/v)己 烧:EtOAc— EtOAc— 95:5 (v/v) CH2C12 :在 MeOH 中之 2.0M NH3), 獲得標題化合物,為白色固體。 步驟8:反式-N-環丙基-N-({3-{[2-(曱氧基)乙基]氧基(曱氧 基)丙基]苯基}曱基)-4-(1,5,6-三曱基-2-酮基-1,2-二氫-4-吡咬 基)-3-六氫峨咬竣醯胺 於得自前一步驟之反式-3-{[環丙基({3-{[2-(曱氧基)乙基]氧 基}-5-[3-(甲氧基)丙基]苯基}曱基)胺基]叛基}-4-(1,5,6-三甲基 -2-酮基-1,2-二氫-4-吡啶基)-1-六氫吡啶羧酸1,1-二甲基乙酯(1 當量)之CH2C12溶液(0.06M)中,添加HC1(4.0M二氧陸圜溶液, 143482-1 -182- 201111364 30當量)。將所形成之溶液在室溫下攪拌4小時β於真空中 移除揮發性物質之後’將所形成之殘留物直接地裝填至以 94:6 (v/v) CH2C12 :在 MeOH 中之 2.0Μ ΝΗ3 填充之 Si02 管柱上。 以相同溶劑系統之溶離’獲得標題化合物,為白色泡沫物。 MS (ESI+,M+H) : 540。人類腎素 IC5〇(缓衝劑):25 nM。人類 腎素IC5〇(血漿):80 nM。 實例14Rinse with EtOAc. The filtrate was concentrated in vacuo to give the title compound as white crystal. Step 5: trans-4-(l,5,6-trimethyl-2-keto-dihydropyridylpyridyl H,3-hexahydropyridinedicarboxylic acid HU-dimercaptoethyl) 3_ethyl vinegar In the first step of the counter-type (6-hydroxy-2,3-dihydropyridylpyridyl)_U-hexahydropyridinedicarboxylic acid 1-(U-dimethylethyl) 3 ethyl ester ( Methyl iodide (1.5 equivalents) was added to a DMF suspension (〇liM) of sodium hydride (60% dispersion in oil, 2 eq.). Then, the resulting mixture was stirred at room temperature for 18 hours. The reaction was quenched by the addition of EtOAc and saturated aqueous NH4CI. The aqueous phase was separated and extracted with EtOAc. The combined organic extracts were washed successively with water and brine, dried over N?SO?, filtered, and concentrated. The crude product thus obtained was purified by column chromatography eluting elut elut elut elut elut elut elut elut Step 6: trans-H[(U-didecylethyl)oxy]refenyl} 4 (15,6-trimethyl-2-keto-1,2-dihydro-4-P ratio) -3- hexahydro it ratio. The slow acid is obtained from the previous step of trans-4-(l,5,6-trimethyl-2-keto 4,2-dihydro-4-port thiol)-1,3-hexahydro Ντ ratio. Add lithium hydroxide to a solution of 1-(1,1-dimercaptoethyl)3_e (([equivalent) 3:2 (v/v) THF: MeOH (0.07M) 1M aqueous solution, 11 equivalents) The vigorously formed turbid solution was stirred vigorously at room temperature for 18 hours. Then, the volatiles were removed in vacuo and the residue was partitioned between EtOAc and 10% EtOAc. The aqueous layer was separated, and 143482-1 -181 - 201111364 was reversed with EtOAc. The combined organic extracts were further washed with water and brine, dried over NasSCXj and filtered. The filtrate was concentrated in vacuo to give title titled Step 7. trans-3-{[cyclopropyl({3-{[2-(methoxy)ethyl)oxy)5_[3.(decyloxy)propyl]phenyl}methyl) Amino]behide 4_(15,6-tridecyl-2-keto-yl-12-di-aryl-4-pyridyl)-1-hexahydropyridinecarboxylic acid u-didecylethyl ester obtained from the previous step Trans-dimethylethyl)oxy]pyridyl 4-(1,5,6-dimercapto-2-one-l,2-dihydro-4-P ratio. Stationary)_3_6 hydrogen? Add hexafluoro-J sulphate-(7-nitrobenzotriazole) in portions of dmf (0.1 M) solution of dilute acid (1 eq.), Hunig's test (3 eq.), and amine 11 (1 eq.). Sit on the small base) _ν, ν, Ν ', Ν '- four 曱 锞 (1.2 equivalents). The resulting reaction solution was stirred at room temperature for 48 hours. The current reddish solution was diluted with EtOAc and washed successively with 1% aqueous HCl solution, aqueous NaOH solution and brine. Then, the organic extract was dehydrated to dryness &lt;RTI ID=0.0&gt;&gt; The crude product thus obtained was purified by flash chromatography (Si 〇 2, 7:3 (v/v) hexanes: EtOAc - EtOAc - 95:5 (v/v) CH2C12: 2.0M NH3 in MeOH) , the title compound was obtained as a white solid. Step 8: trans-N-cyclopropyl-N-({3-{[2-(decyloxy)ethyl)oxy(decyloxy)propyl]phenyl}indolyl)-4-( 1,5,6-tridecyl-2-keto-1,2-dihydro-4-pyridyl)-3-hexahydroguanidine amide in trans -3- from the previous step [Cyclopropyl ({3-{[2-(decyloxy)ethyl]oxy}-5-[3-(methoxy)propyl]phenyl}indolyl)amino]] 1,1-dimethylethyl 4-(1,5,6-trimethyl-2-keto-1,2-dihydro-4-pyridyl)-1-hexahydropyridinecarboxylate (1 equivalent In the CH2C12 solution (0.06 M), HCl (4.0 M dioxane solution, 143482-1 -182 - 201111364 30 equivalents) was added. The resulting solution was stirred at room temperature for 4 hours. After removing the volatiles in vacuo, the residue formed was directly loaded to 94:6 (v/v) CH2C12: 2.0 in MeOH. ΝΗ3 Filled on the Si02 column. The title compound was obtained as a white foam. MS (ESI+, M+H): 540. Human renin IC5 〇 (buffer): 25 nM. Human renin IC5 〇 (plasma): 80 nM. Example 14

反式-N-環丙基-4-(1-甲基-5-{[(曱氧基)曱基]氧基卜2_酮基n 二氫-4-吡啶基)_N-({3-{[2-(曱氧基)乙基]氧基}曱氧基)丙 基]苯基}甲基)-3-六氫p比咬缓酿胺trans-N-cyclopropyl-4-(1-methyl-5-{[(indolyl)indolyloxy)-2-keto]ndihydro-4-pyridyl)_N-({3 -{[2-(decyloxy)ethyl]oxy}decyloxy)propyl]phenyl}methyl)-3-hexahydrop ratio

步驟1 : 3’-{[(曱氧基)曱基]氧基}_5,6_二氫_4,4,聯吡啶{泊办 二羧酸HU-二甲基乙基)3-乙酯 於 4-(4,4,5,5-四曱基-1,3,2-二氧硼伍圜 _2_基)_5,6_二氫 _U(2H)_ 叶匕°疋一缓酸1-(1,1-一甲基乙基)3_乙酯(丨當量,實例i步驟工) 與芳環3 (1當量)之3:1 (v/v)甲苯:乙醇溶液(〇1M)中,添加碳 酸鈉(2M水溶液,3當量)。將此懸浮液抽氣,並以A逆充 填。最後,以一快速部份添加[1JL雙(二苯基膦基)二環戍二 烯鐵]二氣鈀(II) (0.06當量),並將反應懸浮液在8〇t下加熱 16小時。然後,藉由添加Et0Ac與水使反應淬滅。分離水層, 且以EtOAc逆萃取。將合併之有機萃液以1N Na〇H水溶液、 143482-1 -183- 201111364 減鹽水進-步洗滌,以Na2s〇4脫水乾燥,過濾,及使濾 液在真空中濃縮。如此獲得之粗產物經由管柱層析之純化 (Si〇2,90:10 (νΛΟ 己烷:Et0Ac—Et0Ac),獲得標題化合物, 為淡黃色油。 步驟2 :順式-4-(3-{[(甲氧基)甲基]氧基}_4•吡啶基)13•六氫吡 啶二羧酸HU-二甲基乙基)3-乙酯 於得自前一步驟之3,-{[(甲氧基)甲基]氧基卜56_二氫_44,聯 吡啶-1,3(2H)-二羧酸1-(1,1_二甲基乙基)3_乙酯(1當量)之Me〇H 洛液(0.09M)中,添加鎂鏃屑(3.3當量)。將此懸浮液抽氣, 並以%逆充填。最後,使反應混合物在室溫下音振15小時, 於此段期間内鎂鏃屑消失。然後,藉由添加Et〇Ac與1N Na〇H 水溶液使反應淬滅。分離水層,且以Et〇Ac逆萃取。將合併 之有機萃液以水與鹽水進一步洗滌,以Na2S〇4脫水乾燥, 及過濾。濾液在真空中之濃縮,獲得標題化合物,為淡黃 色油。 步驟3 :反式-4_(3_U(曱氧基)甲基]氧基}斗吡啶基)13•六氫吡 咬二羧酸1-(1,1-二曱基乙基)3_乙酯 於得自前一步驟之順式_4-(3-{[(曱氧基)甲基]氧基卜4_p比啶 基)-1’3-六氫吡啶二羧酸二曱基乙基)3_乙酯(1當量)之 乙醇溶液(0.1M)中,添加剛製成之乙醇鈉(1.2當量)。將所形 成之黃橘色溶液在55°C下加熱16小時。然後,於真空中移 除揮發性物質,並使殘留物於EtOAc與飽和NH4C1水溶液之 間作分液處理。分離水層,且以Et〇 Ac逆萃取。將合併之有 機萃液以水與鹽水進一步洗滌,以]^&amp;25〇4脫水乾燥,過渡, 143482*1 •184· 201111364 及使濾液在真空中濃縮。如此獲得之粗產物經由管柱層析 之純化(Si02,95:5 (Wv)己烷:EtOAc-&gt; 1:1 (v/v)己烷:EtOAc), 獲得標題化合物,為淡黃色油。 步驟4:反式-4-(3-{[(甲氧基)甲基]氧基μΐ_氧化_4_吡啶基)_13 六氫吡啶二羧酸1-(1,1-二甲基乙基)3_乙酯 於得自前一步驟之反式-4-(3-{[(甲氧基)甲基]氧基}斗吡啶 基)-1,3-六氫吡啶二羧酸二甲基乙基)3_乙酯(1當量)之 一氯曱烷溶液(0.1Μ)中,添加3-氯基過氧苯甲酸(1當量)。將 所形成之無色溶液在室溫下攪拌13小時。然後,以飽和 NaHS〇3水溶液水溶液使反應淬滅。分離水層,並 以EtOAc逆萃取。將合併之有機萃液以水與鹽水進一步洗滌 ,以NaaSO4脫水乾燥,及過濾。濾液在真空中之濃縮,獲 得標題化合物,為白色固體。 步驟5:反式-4-(1-甲基-5-{[(曱氧基)甲基]氧基}_2_酮基二氫 斗吡啶基)-1,3-六氫吡啶二羧酸•二曱基乙基)3_乙酯 於得自前一步驟之反式斗(3_{[(曱氧基)甲基]氧基H氧化 斗吡啶基)-1,3-六氫吡啶二羧酸Hu_二甲基乙基)3乙酯(1當 量)之甲苯溶液(0.06M)中,添加三乙胺(3當量)。其中將反 應谷器 &gt;又 &gt;又在冰水浴中,逐滴添加純三氟醋酸酐(3當量), 歷經2分鐘期間。使所形成之黃色溶液慢慢地溫熱至室溫, 然後將其在室溫下攪拌18小時。藉由添加段〇八〇與飽和 水/容液使反應淬滅。分離水層,並以Et〇Ac逆萃取。將合併 之有機萃液以水與鹽水進一步洗滌,以Na2S〇4脫水乾燥, 過濾,及使濾液在真空中濃縮。使如此獲得之膠黏橘色油 143482-1 -185. 201111364 立即溶於甲醇__中。然後,於其甲,在〇。口,添加氮 氧化納⑽水溶液,3當量)與硫酸二曱師當量)。使所形 成之橘色溶液慢慢地溫熱至室溫’然後將其在室溫下攪拌 科時。於真空巾移除揮發性物f,錢殘留物於她c 與飽和NH4C1水溶液之間作分液處理。分離水層,且以Et0Ac 逆萃取。將合併之有機萃液以水與鹽水進—步洗務,以 Na2S〇4脫水乾燥,過渡’及使濾液在真空中濃縮。如此獲 得之粗產物經由管柱層析之純化(Si〇2, 95:5(v/v)cH2ci2 :在Step 1: 3'-{[(曱oxy)indolyl]oxy}_5,6-dihydro-4,4,bipyridyl {Bodio-carboxylic acid HU-dimethylethyl) 3-ethyl ester 4-(4,4,5,5-tetradecyl-1,3,2-dioxaborin-2-yl)_5,6-dihydro-U(2H)_叶匕°疋缓1-(1,1-Methylethyl) 3 -ethyl acid (equivalent, example i step) and aromatic ring 3 (1 equivalent) of 3:1 (v/v) toluene: ethanol solution (〇 In 1M), sodium carbonate (2M aqueous solution, 3 equivalents) was added. The suspension was evacuated and backfilled with A. Finally, [1 JL of bis(diphenylphosphino)bicyclononanediene]digaspalladium(II) (0.06 equivalent) was added in a quick portion, and the reaction suspension was heated at 8 °t for 16 hours. The reaction was then quenched by the addition of Et0Ac and water. The aqueous layer was separated and extracted with EtOAc. The combined organic extracts were washed with aq. 1N NaH aqueous solution, &lt;RTI ID=0.0&gt;&gt;&&&&&&&&&&&&&&& The crude product thus obtained was purified by column chromatography (EtOAc: EtOAc: EtOAc: EtOAc (EtOAc) {[(Methoxy)methyl]oxy}_4•pyridyl)13•hexahydropyridinedicarboxylic acid HU-dimethylethyl)3-ethyl ester obtained from the previous step 3, -{[( Methoxy)methyl]oxybu 56_dihydro-44, bipyridyl-1,3(2H)-dicarboxylic acid 1-(1,1-dimethylethyl) 3 ethyl ester (1 equivalent Magium swarf (3.3 eq.) was added to Me〇H Lok (0.09 M). The suspension was evacuated and filled in %. Finally, the reaction mixture was sonicated at room temperature for 15 hours during which time the magnesium swarf disappeared. Then, the reaction was quenched by the addition of Et 〇Ac and 1N Na〇H aqueous solution. The aqueous layer was separated and back-extracted with Et 〇Ac. The combined organic extracts were further washed with water and brine, dried over Na 2 EtOAc, and filtered. The filtrate was concentrated in vacuo to give the title compound as pale yellow oil. Step 3: trans-4_(3_U(decyloxy)methyl]oxy}piperidinyl)13•hexahydropyridyldicarboxylic acid 1-(1,1-dimercaptoethyl)3_ethyl ester Cis- 4-(3-{[(indolyl)methyl]oxyb 4_p-pyridyl)-1'3-hexahydropyridinedicarboxylic acid dimercaptoethyl)3 from the previous step To the ethanol solution (0.1 M) of ethyl ester (1 equivalent), freshly prepared sodium ethoxide (1.2 equivalents) was added. The resulting yellow orange solution was heated at 55 ° C for 16 hours. The volatiles were then removed in vacuo and the residue was partitioned between EtOAc and sat. The aqueous layer was separated and back-extracted with Et. The combined organic extracts were further washed with water and brine, dehydrated to dryness, transition, 143482*1 • 184 · 201111364 and the filtrate was concentrated in vacuo. The crude product thus obtained was purified by EtOAc EtOAc EtOAc (EtOAc:EtOAc . Step 4: trans-4-(3-{[(methoxy)methyl]oxypyrrole_oxidation_4_pyridyl)_13 Hexahydropyridinedicarboxylic acid 1-(1,1-dimethylethyl Base 3_ethyl ester in trans-4-(3-{[(methoxy)methyl]oxy}piperidinyl)-1,3-hexahydropyridine dicarboxylic acid dimethyl obtained from the previous step 3-Chloroperoxybenzoic acid (1 equivalent) was added to a solution of chlorodecane (0.1 Torr) in one of ethyl ethyl) 3-ethyl ester (1 eq.). The resulting colorless solution was stirred at room temperature for 13 hours. Then, the reaction was quenched with saturated aqueous NaHS 3 aqueous solution. The aqueous layer was separated and extracted with EtOAc. The combined organic extracts were further washed with water and brine, dried over Na.sub.2SO4, and filtered. The filtrate was concentrated in vacuo to give the title compound as white crystal. Step 5: trans-4-(1-methyl-5-{[(indolyl)methyl]oxy}_2-one dihydropyridinyl)-1,3-hexahydropyridinedicarboxylic acid • Dimercaptoethyl) 3_ethyl ester in the counter-step (3_{[(曱oxy)methyl]oxy H oxidized pyridyl)-1,3-hexahydropyridine dicarboxylate from the previous step Triethylamine (3 equivalents) was added to a toluene solution (0.06 M) of EtOAc. Among them, the reaction barr &gt; and &gt; was again added dropwise in a ice water bath to pure trifluoroacetic anhydride (3 equivalents) over a period of 2 minutes. The resulting yellow solution was slowly warmed to room temperature and then stirred at room temperature for 18 hours. The reaction was quenched by the addition of hydrazine and saturated water/liquid. The aqueous layer was separated and back-extracted with Et 〇Ac. The combined organic extracts were further washed with water and brine, dried over Na 2 EtOAc, filtered, and evaporated. The thus obtained adhesive orange oil 143482-1 -185. 201111364 Immediately dissolved in methanol __. Then, in its A, in the hustle and bustle. Mouth, adding sodium (10) aqueous solution of nitrogen oxide, 3 equivalents) and diterpene sulfate equivalent). The resulting orange solution was slowly warmed to room temperature and then it was stirred at room temperature. The volatile matter f was removed from the vacuum towel, and the residue of the residue was subjected to liquid separation between her c and a saturated aqueous NH4Cl solution. The aqueous layer was separated and back-extracted with Et0Ac. The combined organic extracts were washed with water and brine, dried over Na.sub.2.sub.4, and then evaporated and evaporated. The crude product thus obtained was purified by column chromatography (Si〇2, 95:5 (v/v) cH2ci2: at

MeOH中之2.〇MNH3)’獲得標題化合物,為淡紫色泡泳物。 步驟6 :反式·W[(U_: f基乙基)氧基擒基}邻▼基_5仙甲 氧基)甲基]氧基卜2-酮基-i,2_二氫领。定基)3六氩峨咬敌酸 於得自前一步驟之反式邻-曱基_5_{[(曱氧基)曱基]氧 基}-2-酮基-1,2-二氫-4-吡啶基H,3_六氫吡啶二羧酸Hu_二甲 基乙基)3-乙醋(1當量)之3:2 (v/v)避:Me〇H溶液(〇 〇娜中, 添加氫氧化鋰(ΙΜ水溶液,3當量)。將所形成之混濁溶液 在室溫下激烈㈣24小時。然後,於真空中移除揮發性物 質,並使殘留物於EtOAc與l〇%HCl水溶液之間作分液處理。 分離水層,且以EtOAc逆萃取。將合併之有機萃液以水與鹽 水進一步洗滌,以N^SO4脫水乾燥,及過濾。濾液在真空 中之濃縮’獲得標題化合物,為粉紅色固體。 步驟7:反式-3-{[環丙基({3_{[2_(甲氧基)乙基]氧基卜5 [3 (甲氧 基)丙基]本基}甲基)胺基]炭基卜4-(1-甲基_5_{[(甲氧基)甲基]氧 基}-2-酮基-1,2-二氫-4-P比咬基)_ι_六氫p比啶叛酸〗,丨_二甲基乙酯 於得自前一步驟之反二甲基乙基)氧基]羰基卜4_ 143482-1 -186· 201111364 (1-甲基-5-{[(甲氧基)曱基]氧基}_2_酮基-二氫_4_吡啶基)_3_ 六氫吡啶羧酸(1當量)、Hunig氏鹼(3當量)及胺11 (1當量)之 DMF (0.1M)溶液中’分次添加六氟磷酸0·(7_氮苯并三唑小 基)-Ν,Ν,Ν·,Ν·-四曱基錁(1.2當量)。將所形成之反應溶液在室 溫下攪拌48小時。將目前帶紅色溶液以Et〇Ac稀釋,並以1〇% HC1水溶液、IN NaOH水溶液及鹽水相繼洗滌。然後,使有 機萃液以Na2S〇4脫水乾燥,過濾,及使濾液在真空中濃縮, 而得紫色油。如此獲得之粗產物經由急驟式層析之純化 (Si02,96:4 (v/v) CH2C12 :在MeOH 中之 2.0M NH3),獲得標題 化合物’為略帶粉紅色泡沫物。 步驟8 :反式-N-環丙基-4-(1-曱基-5-{[(甲氧基)甲基]氧基卜2__ 基-1,2-二氫-4-吡啶基)-N-({3-{[2-(曱氧基)乙基]氧基}-5-[3-(曱氧 基)丙基]苯基}甲基)-3-六氫峨。定叛醯胺 於得自前一步驟之反式-3-{[環丙基({3-{[2-(甲氧基)乙基]氧 基}-5-[3-(曱氧基)丙基]苯基}曱基)胺基]羰基卜4_(1_甲基_5_丨[(甲 乳基)甲基]氧基}-2-酮基-1,2-二氫-4-p比咬基)-1-六氫p比咬叛酸 U-二曱基乙酯(1當量)之CI^Cl2溶液(0.02M)中,添加溴化鋅 (11)(10當量)。使所形成之懸浮液音振15分鐘,並在室溫下 攪拌13小時。藉由添加EtOAc與IN NaOH水溶液使反應淬滅, 然後音振15分鐘《分離水相,且以EtOAc逆萃取。將合併之 有機萃液以水與鹽水進一步洗滌,以Na2S04脫水乾燥,過 濾,及使濾液在真空中濃縮。如此獲得之粗產物經由急驟 式層析之純化(Si〇2 ’ 90:10 (v/v) CH2C12 :在 MeOH 中之 2.0M NH3) ’獲得標題化合物’為無色油。MS (ESI+,M+H) : 572。 143482-1 -187- 201111364 實例15 反式-N-環丙基-N-{[2,3-二氯-5-(3-氰基丙基)苯基]甲基Η-d-甲 基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺2. The title compound was obtained as a lavender soak in MeOH. Step 6: trans-W[(U_: f-ethyl)oxyindenyl}-o--------------------- Fixation of 3 hexamethylene argon to the di-ortho-indolyl_5_{[(decyloxy)indolyl]oxy}-2-keto-1,2-dihydro-4 - Pyridyl H,3-hexahydropyridinedicarboxylic acid Hu-dimethylethyl) 3-ethyl vinegar (1 equivalent) of 3:2 (v/v) Avoid: Me〇H solution (〇〇娜中, Lithium hydroxide (aqueous solution of hydrazine, 3 eq.) was added. The resulting turbid solution was vigorously quenched (tetra) for 24 hours at room temperature. The volatiles were then removed in vacuo and the residue was taken from EtOAc and EtOAc. The aqueous layer was separated and the title compound was obtained from EtOAc EtOAc. Is a pink solid. Step 7: trans-3-{[cyclopropyl({3_{[2-(methoxy)ethyl]oxy) 5 [3 (methoxy)propyl]benz} Amino]carbonyl] 4-(1-methyl-5-{[(methoxy)methyl]oxy}-2-one-1,2-dihydro-4-P ratio) _ι_ hexahydrop-pyridyl acid, 丨 dimethyl dimethyl ester from the previous step of the anti-dimethylethyl oxy] carbonyl b 4 _ 143482-1 -186· 201111364 (1-Methyl-5-{[(methoxy)indenyl]oxy}_2-keto-dihydro-4-pyridyl)_3_ hexahydropyridinecarboxylic acid (1 Equivalent), Hunig's base (3 equivalents) and amine 11 (1 equivalent) in DMF (0.1M) solution 'sequential addition of hexafluorophosphate 0·(7-azabenzotriazole small group)-Ν, Ν, Ν·,Ν·-four 曱 锞 (1.2 equivalents). The resulting reaction solution was stirred at room temperature for 48 hours. The current reddish solution was diluted with Et〇Ac and washed successively with 1% HCl aqueous solution, 1 N aqueous NaOH solution and brine. Then, the organic extract was dehydrated and dried over Na 2 SO 4 , filtered, and the filtrate was concentrated in vacuo to give a purple oil. The crude product thus obtained was purified by flash chromatography (EtOAc, EtOAc: EtOAc (EtOAc) Step 8: trans-N-cyclopropyl-4-(1-indolyl-5-{[(methoxy)methyl]oxybu 2__yl-1,2-dihydro-4-pyridyl) -N-({3-{[2-(decyloxy)ethyl)oxy}-5-[3-(decyloxy)propyl]phenyl}methyl)-3-hexahydroindole. Derivatization of trans-amine -3-{[cyclopropyl({3-{[2-(methoxy)ethyl)oxy}-5-[3-(decyloxy))) Propyl]phenyl}indolyl)amino]carbonyl-4-(1_methyl_5_丨[(methyllacyl)methyl]oxy}-2-keto-1,2-dihydro-4 -p octyl bromide (1) was added to a CI^Cl2 solution (0.02 M) of U-dimercaptoethyl ester (1 equivalent), and zinc bromide (11) (10 equivalents) was added. The resulting suspension was sonicated for 15 minutes and stirred at room temperature for 13 hours. The reaction was quenched by the addition of EtOAc and aqueous EtOAc EtOAc. The combined organic extracts were further washed with water and brine, dried over Na 2 EtOAc, filtered, and evaporated. The crude product thus obtained was purified by flash chromatography (yield: </ RTI> </ RTI> </ RTI> </ RTI> </ RTI> </ RTI> </ RTI> </ RTI> <RTIgt; MS (ESI+, M+H): 572. 143482-1 -187- 201111364 Example 15 trans-N-cyclopropyl-N-{[2,3-dichloro-5-(3-cyanopropyl)phenyl]methylindole-d-methyl -2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺12及如在實例14步驟8中之溴化鋅(Π)-促進之BOC-籲 去除保護。獲得標題化合物,為淡綠色泡沫物。MS (ESI+, M+H) : 502。 實例16 反式-N-{[5-(3-氰基丙基)-2,3-二氟苯基]甲基}-N-環丙基-4-(1-甲 基-2-酮基-1,2-二氫-4-吡啶基)·3-六氫吡啶羧醯胺The procedure described in Example 1 was followed, but instead the amine 12 as the starting material and the zinc bromide-promoted BOC-extraction protection as in Example 8 Step 8 were used. The title compound was obtained as a pale green foam. MS (ESI+, M+H): 502. Example 16 trans-N-{[5-(3-Cyanopropyl)-2,3-difluorophenyl]methyl}-N-cyclopropyl-4-(1-methyl-2-one Base-1,2-dihydro-4-pyridyl)·3-hexahydropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺13及如在實例14步驟8中之溴化鋅(II)-促進之BOC- 去除保護。獲得標題化合物,為淡綠色泡沫物。MS (ESI+, M+H) : 469。 實例17 反式-N-環丙基-N-{[2,3-二氣-5-(4-羥丁基)苯基]曱基甲基 -2-酮基-1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺 143482-1 -188 · 201111364The procedure described in Example 1 was followed, but instead the amine 13 as the starting material and the zinc (II) bromide-promoted BOC- removal protection as in Example 8 Step 8. The title compound was obtained as a pale green foam. MS (ESI+, M+H): 469. Example 17 trans-N-cyclopropyl-N-{[2,3-dioxa-5-(4-hydroxybutyl)phenyl]nonylmethyl-2-keto-1,2-dihydro -4-pyridyl)_3_hexahydropyridine carboxamide 143482-1 -188 · 201111364

MeMe

步驟1 :反式-3-{[環丙基({2,3-二氯-5-[4-(甲氧基)-4-酮基丁基] 苯基}甲基)胺基機基)-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)-1-六氫吡啶羧酸1,1-二甲基乙醋 於反式-1-{[(1,1-二甲基乙基)氧基]羰基甲基-2-酮基 φ -1,2-二氫冰吡啶基)-3-六氫吡啶羧酸(1當量,實例1步驟6)、Step 1: trans-3-{[cyclopropyl({2,3-dichloro-5-[4-(methoxy)-4- ketobutyl]phenyl}methyl)amino) -4-(1-mercapto-2-keto-1,2-dihydro-4-pyridyl)-1-hexahydropyridinecarboxylic acid 1,1-dimethylethyl acetonate in trans-1- {[(1,1-Dimethylethyl)oxy]carbonylmethyl-2-keto) φ-1,2-dihydropyridinyl)-3-hexahydropyridinecarboxylic acid (1 equivalent, Example 1 Step 6),

Hunig氏鹼(3當量)及胺14(1當量)之DMF (0.1M)溶液中,分次 添加六氟磷酸0-(7-氮苯并三唑-1-基)_ν,Ν,Ν',Ν'-四曱基錁(1.2 當量)。將所形成之反應溶液在室溫下攪拌48小時。將目前 黃色溶液以EtOAc稀釋,並以1〇% HC1水溶液、IN NaOH水溶 液及鹽水相繼洗滌。然後,使有機萃液以Na2s〇4脫水乾燥, 過遽,及使渡液在真空中濃縮’而得帶紅橘色油。如此獲 得之粗產物經由急驟式層析之純化(Si〇2,7:3 (v/v)己烷: β EtOAc— EtOAc— 95:5 (v/v) CH2C12 :在 MeOH 中之 2.0M NH3),獲 传標題化合物’為淡黃色泡泳物。 步驟2 :反式-3-[(環丙基{[2,3-二氯-5-(4-羥丁基)苯基]曱基}胺 基]幾基}-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)小六氫吡唆緩 酸1,1-二甲基乙酯 於得自前一步驟之反式-3-{[環丙基({2,3-二氯-5-[4-(曱氧 基)-4-酮基丁基]苯基}甲基)胺基]羰基卜4_(1_曱基_2_酮基u二 氫-4-p比咬基)-1-六氫吡&quot;定叛酸二曱基乙酯(丨當量)之 143482-1 -189- 201111364 溶液(0.08M)中,以一快速部份添加硼氫化鋰⑺當量)。於3Hunig's base (3 equivalents) and amine 14 (1 equivalent) in DMF (0.1M) solution, adding hexafluorophosphate 0-(7-azabenzotriazol-1-yl)_ν, Ν, Ν' , Ν '- four 曱 锞 (1.2 equivalent). The resulting reaction solution was stirred at room temperature for 48 hours. The current yellow solution was diluted with EtOAc and washed sequentially with 1% aqueous HCl solution, aqueous 1 N NaOH and brine. Then, the organic extract was dehydrated and dried over Na 2 s 4 , dried, and concentrated to give a red-brown oil. The crude product thus obtained was purified by flash chromatography (Si 〇 2, 7:3 (v/v) hexane: EtOAc EtOAc - EtOAc - 95:5 (v/v) CH2C12: 2.0M NH3 in MeOH ), the title compound was passed as a light yellow bubble. Step 2: trans-3-[(cyclopropyl{[2,3-dichloro-5-(4-hydroxybutyl)phenyl]decyl}amino]]yl}-4-(1-indole) 1,2-dihydro-4-pyridyl) hexahydropyridinium acid 1-diethyl phthalate in trans--3-{[cyclopropyl] from the previous step (2,3-Dichloro-5-[4-(decyloxy)-4- ketobutyl]phenyl}methyl)amino)carbonyl] 4_(1_fluorenyl-2-keto) u dihydro-4-p ratio bite base)-1-hexahydropyridyl &quot; deuterated acid dimercaptoethyl ester (丨 equivalent) of 143482-1 -189- 201111364 solution (0.08M), to a fast department Lithium borohydride (7) equivalents were added in portions. At 3

濾液在真空中之濃縮,獲得標題化合物,為白色泡沫物。The filtrate was concentrated in vacuo to give the title compound as white powder.

4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺 於得自前一步驟之反式_3_[(環丙基{[23_二氣_5·(4羥丁基) 苯基]甲基}胺基)羰基]-4-(1-曱基_2-酮基-1,2-二氫-4-吡啶基)-1_ _ 八氫吡啶羧酸1,1-二甲基乙酯(1當量)之CH2C12溶液(〇 〇5Μ) 中,添加HC1 (4.0Μ二氧陸圜溶液,3〇當量)。將所形成之溶 液在室溫下攪拌3小時。於真空中移除揮發性物質之後,將 所形成之殘留物直接地裝填至以93:7 (v/v) CH2ci2 :在MeOH 中之2.0M NH3填充之Si〇2管柱上。以相同溶劑系統之溶離, 獲得標題化合物,為白色泡沫物。MS (ESI+,M+H) : 508。 實例18 反式環丙基_4-(1_甲基_2_酮基-以二氫_4_吡啶基 (甲氧基)丙基Η-尊基丨甲基)各六氫吡啶羧醯胺4-(1-Methyl-2-keto-1,2-dihydro-4-pyridyl)_3_hexahydropyridine carboxamide in trans _3_[(cyclopropyl{[] from the previous step 23_二气_5·(4hydroxybutyl)phenyl]methyl}amino)carbonyl]-4-(1-indolyl-2-keto-1,2-dihydro-4-pyridyl) -1_ _ 1,2-dimethylethyl octahydropyridinecarboxylate (1 equivalent) in a CH2C12 solution (〇〇5Μ) was added with HCl (4.0 Μ dioxane solution, 3 〇 equivalent). The resulting solution was stirred at room temperature for 3 hours. After removal of the volatiles in vacuo, the resulting residue was loaded directly onto a &lt;RTI ID=0.0&gt;&gt;&gt;&gt; The title compound was obtained as a white foam. MS (ESI+, M+H): 508. Example 18 Transcyclopropyl_4-(1-methyl-2-keto--dihydro-4-pyridyl(methoxy)propyl-anthracene-methyl)dihydropyridinecarboxylate amine

根據實例1中所述之程序製成,但替代地使用胺15作為 起始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, 143482-1 -190· 201111364 M+Na)· 510 ° NMR (CDC13) δ (ppm); 0.72-0.78 (br m, 1H), 0.82-0.96 (br m, 3H), 1.59-1.66 (m, 1H), 1.74-1.84 (br s, 2H), 1.91-1.97 (m, 2H), 2.22-2.28 (br m, 1H), 2.74-2.87 (m, 4H), 3.03 (dt, J = l〇.4, 5 2 Hz 1H) 3.14-3.21 (m, 2H),3.36 (s,3H),3.37 (s,3H), 3.42 (t,J = 7.4 Hz, 2H), 3.43-3.47 (m, 1H), 4.83 (d, J = 14 Hz, 1H), 5.02 (d, J = 14 Hz, 1H), 5.94 (d, J = 6.9 Hz, 1H), 6.34 (s, 1H), 6.78 (d, J = 6.9 Hz, 1H), 7.16 (s, 1H), 7.33-7.46 (m, 2H), 7.55 (s, 1H), 7.77 (d, J = 7.2 Hz, 1H), 7.94 (d, J = 7.2 Hz, 1H)。人類腎素IC5〇(緩衝劑):〇.4nM。人類腎素IC5〇(血 漿):1.8 nM。 實例19 反式-(2-{3,4-二氣-5-[(環丙基{[4-(1-甲基-2-酮基-1,2-二氫-4-吡啶 基)-3-六氫吡啶基]戴基}胺基)曱基]笨基}乙基)胺基曱酸曱酯It was made according to the procedure described in Example 1, but instead using amine 15 as the starting material. The title compound was obtained as a white foam. MS (ESI+, 143482-1 -190· 201111364 M+Na)· 510 ° NMR (CDC13) δ (ppm); 0.72-0.78 (br m, 1H), 0.82-0.96 (br m, 3H), 1.59-1.66 (m, 1H), 1.74-1.84 (br s, 2H), 1.91-1.97 (m, 2H), 2.22-2.28 (br m, 1H), 2.74-2.87 (m, 4H), 3.03 (dt, J = L〇.4, 5 2 Hz 1H) 3.14-3.21 (m, 2H), 3.36 (s, 3H), 3.37 (s, 3H), 3.42 (t, J = 7.4 Hz, 2H), 3.43-3.47 (m , 1H), 4.83 (d, J = 14 Hz, 1H), 5.02 (d, J = 14 Hz, 1H), 5.94 (d, J = 6.9 Hz, 1H), 6.34 (s, 1H), 6.78 (d , J = 6.9 Hz, 1H), 7.16 (s, 1H), 7.33-7.46 (m, 2H), 7.55 (s, 1H), 7.77 (d, J = 7.2 Hz, 1H), 7.94 (d, J = 7.2 Hz, 1H). Human renin IC5 缓冲 (buffer): 〇. 4nM. Human renin IC5 (blood): 1.8 nM. Example 19 trans-(2-{3,4-dioxa-5-[(cyclopropyl{[4-(1-methyl-2-keto-1,2-dihydro-4-pyridyl)) -3-hexahydropyridyl]-yl}amino) fluorenyl] phenyl} ethyl) amide decyl decanoate

根據實例1中所述之程序製成,但替代地使用胺16作為 起始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 535。 實例20 反式-N-環丙基曱基_2•酮基-1,2-二氫-4-吡啶基)-N-(8-〇奎淋 基甲基)-3-六氫吡啶羧醢胺 143482-1 • 191- 201111364It was made according to the procedure described in Example 1, but instead using amine 16 as the starting material. The title compound was obtained as a white foam. MS (ESI+, M+H): 535. Example 20 trans-N-cyclopropylindenyl-2- keto-1,2-dihydro-4-pyridyl)-N-(8-fluorenylmethyl)-3-hexahydropyridinecarboxylate Guanamine 143482-1 • 191- 201111364

根據實例1中所述之程序製成,但替代地使用胺p作為 起始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 417 〇 實例21 反式-N-環丙基-N-(8-異喳啉基甲基)-4-(1-甲基-2-酮基-1,2-二氫 -Otb咬基)-3-六氫p比咬叛醯胺It was made according to the procedure described in Example 1, but instead using amine p as the starting material. The title compound was obtained as a white foam. MS (ESI+, M+H): 417 </RTI> </RTI> <RTI ID=0.0>############################################################## 2-dihydro-Otb dimethyl)-3-hexahydrop ratio

MeMe

根據實例1中所述之程序製成,但替代地使用胺18作為 起始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 417。 實例22 反式-N-環丙基-N-(5-異喳啉基甲基)-4-(1-曱基-2-酮基-l,2-二氫 -4-ρ比°定基)-3-六氮p比°定缓酿胺It was made according to the procedure described in Example 1, but instead using amine 18 as the starting material. The title compound was obtained as a white foam. MS (ESI+, M+H): 417. Example 22 trans-N-cyclopropyl-N-(5-isoindolylmethyl)-4-(1-indolyl-2-keto-l,2-dihydro-4-ρ ratio )-3-hexanitrogen p ratio

根據實例1中所述之程序製成,但替代地使用胺19作為 起始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, 143482-1 • 192- 201111364 M+H) : 417。 實例23 反式-N-環丙基_4·(ι_曱基_2_酮基-1,2-二氫-4-吡啶基)_n_(5-喹啉 基曱基)-3-六氫吡啶羧醯胺It was made according to the procedure described in Example 1, but instead using amine 19 as the starting material. The title compound was obtained as a white foam. MS (ESI+, 143482-1 • 192-201111364 M+H): 417. Example 23 trans-N-cyclopropyl_4·(ι_indolyl-2-keto-1,2-dihydro-4-pyridyl)_n_(5-quinolinylfluorenyl)-3-hexa Hydropyridine carboxamide

MeMe

根據實例1中所述之程序製成’但替代地使用胺20作為 起始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 417。 實例24 反式-N-環丙基_N-(1-異喳啉基曱基)-4-(1-甲基-2-酮基-i,2-二氫 -4-p比咬基)-3-六氫?比。定叛醢胺It was made according to the procedure described in Example 1 but using amine 20 as a starting material instead. The title compound was obtained as a white foam. MS (ESI+, M+H): 417. Example 24 trans-N-cyclopropyl-N-(1-isoindolyl fluorenyl)-4-(1-methyl-2-keto-i,2-dihydro-4-p ratio )-3-hexahydro? ratio. Detamine

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根據實例1中所述之程序製成,但替代地使用胺21作為 起始物質。獲得標題化合物,為白色泡床物。MS (ESI+, M+H) : 417。 實例25 反式-N-環丙基-4-(1-甲基-2-酮基-1,2-二氫-4-ρ比。定基)_n_({2_[3_ (曱氧基)丙基]-4-喹淋基}曱基)_3_六氫吡啶羧醯胺 143482-1 -193- 201111364It was made according to the procedure described in Example 1, but instead using amine 21 as the starting material. The title compound was obtained as a white blister. MS (ESI+, M+H): 417. Example 25 trans-N-cyclopropyl-4-(1-methyl-2-keto-1,2-dihydro-4-ρ ratio. Stationary)_n_({2_[3_(decyloxy)propane ]]-4-quinolyl}hydrazino)_3_hexahydropyridine carboxamide 143482-1 -193- 201111364

根據實例1中所述之程序製成,但替代地使用胺22作為 起始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H): 489。4 NMR (CD3OD) 5(ppm): 0.83-0.88 (m,1H),0.89-0.97 (m, 1H), 1.00-1.08 (m, 2H), 1.69 (qd, J = 12.8, 4.1 Hz, 1H), 1.82 (d, J = 13.3 Hz, 1H), 2.02 (p, J = 7.0 Hz, 2H), 2.67-2.71 (m, 1H), 2.72-2.81 (m, # 2H), 2.93 (m, 2H), 3.04 (dt, J = 12.8, 4.1 Hz, 1H), 3.18 (d, J = 13.0 Hz, 1H), 3.32-3.38 (m, 3H), 3.40-3.47 (m, 5H), 3.72 (m, 2H), 4.78 (d, J = 7.5 Hz, 1H), 5.18 (d, J = 7.5 Hz, 1H), 6.27 (d, J = 6.9 Hz, 1H), 6.42 (s, 1H), 6.99 (s, 1H), 7.39 (d, J = 6.9 Hz, 1H), 7.51 (t, J = 7.6 Hz, 1H), 7.74 (t, J = 7.7 Hz,1H),7.99 (t, J = 7.3 Hz,2H)。人類腎素 IC50(緩衝劑):L4 nM。人類腎素IC5〇(血漿):3 〇 nM。 實例26 反式-N-環丙基_4·(1_曱基么酮基_12_二氫冰吡啶基籲 (甲氧基)丙基]-8-喹啉基}甲基)·3_六氫吡啶羧醯胺It was made according to the procedure described in Example 1, but instead using amine 22 as the starting material. The title compound was obtained as a white foam. MS (ESI+, M+H): 489. 4 NMR (CD3OD) 5 (ppm): 0.83-0.88 (m, 1H), 0.89-0.97 (m, 1H), 1.00-1.08 (m, 2H), 1.69 ( Qd, J = 12.8, 4.1 Hz, 1H), 1.82 (d, J = 13.3 Hz, 1H), 2.02 (p, J = 7.0 Hz, 2H), 2.67-2.71 (m, 1H), 2.72-2.81 (m , # 2H), 2.93 (m, 2H), 3.04 (dt, J = 12.8, 4.1 Hz, 1H), 3.18 (d, J = 13.0 Hz, 1H), 3.32-3.38 (m, 3H), 3.40-3.47 (m, 5H), 3.72 (m, 2H), 4.78 (d, J = 7.5 Hz, 1H), 5.18 (d, J = 7.5 Hz, 1H), 6.27 (d, J = 6.9 Hz, 1H), 6.42 (s, 1H), 6.99 (s, 1H), 7.39 (d, J = 6.9 Hz, 1H), 7.51 (t, J = 7.6 Hz, 1H), 7.74 (t, J = 7.7 Hz, 1H), 7.99 (t, J = 7.3 Hz, 2H). Human renin IC50 (buffer): L4 nM. Human renin IC5 〇 (plasma): 3 〇 nM. Example 26 trans-N-cyclopropyl_4·(1_fluorenyl ketone ketone 12-dihydropyridinyl (methoxy)propyl]-8-quinolinyl}methyl)·3 _ hexahydropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用胺23作為 起始物質。獲得標題化合物,為白色泡泳物。MS (ESI+, M+H) : 489。 143482-1 •194- 201111364 實例27 反式-N-[(5-、;臭基-2,3-二氣苯基)曱基]_N_環丙基_4_(1_曱基_2_酮 基-1,2-二氫-4-P比啶基)_3_六氫吡啶羧醯胺Prepared according to the procedure described in Example 1, but instead using amine 23 as the starting material. The title compound was obtained as a white soak. MS (ESI+, M+H): 489. 143482-1 •194- 201111364 Example 27 trans-N-[(5-,; odoryl-2,3-diphenyl)indenyl]_N_cyclopropyl_4_(1_mercapto_2_ Keto-1,2-dihydro-4-Ppyridyl)_3_hexahydropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用N_[(5_溴基 # _2,3_二氯苯基)曱基]環丙胺(胺5步驟2)作為胺起始物質。獲 得標題化合物,為白色泡沫物。MS (ESI+,M+H) : 512。 實例28 反式-N-({3-氣基-5-[3-(甲氧基)丙基]苯基)曱基}_N_環丙基 甲基-2-酮基-1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺 MePrepared according to the procedure described in Example 1, but instead using N_[(5-bromo #2,3-dichlorophenyl)indolyl]cyclopropylamine (amine 5 step 2) as the amine starting material. The title compound was obtained as a white foam. MS (ESI+, M+H): 512. Example 28 trans-N-({3-carbyl-5-[3-(methoxy)propyl]phenyl)indolyl}_N-cyclopropylmethyl-2-keto-1,2- Dihydro-4-pyridyl)_3_hexahydropyridine Carboxamide Me

根據實例1中所述之程序製成,但替代地使用胺24起始 物質。獲得標題化合物,為淡黃色泡沫物。MS (ESI+,M+H): 472。 實例29 反式-N-環丙基-4-(1-曱基-2-酮基_i,2_二氫-4-吡啶基)-Ν-({1-[3- (甲氧基)丙基HH-啕哚-3-基}曱基)_3_六氫吡啶羧醢胺 143482-1 ,195· 201111364It was made according to the procedure described in Example 1, but instead the amine 24 starting material was used. The title compound was obtained as a pale yellow foam. MS (ESI+, M+H): 472. Example 29 trans-N-cyclopropyl-4-(1-indol-2-oneyl-i,2-dihydro-4-pyridyl)-indole-({1-[3-(methoxy) )propylHH-indol-3-yl}indenyl)_3_hexahydropyridine carboxamide 143482-1,195· 201111364

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺25及如在實例14步驟8中之溴化鋅(Π)-促進之B〇c_ 去除保護。獲得標題化合物’為白色泡沫物^ MS (ESI+, M+H) : 477。 實例30 反式-N-環丙基-N-{[2,3-二氣-5-(2-氰基乙基)苯基]曱基}_4_(1_甲 基-2-酮基-1,2-二氫-4-P比啶基)-3-六氫吡啶羧醯胺The procedure described in Example 1 was followed, but instead the amine 25 as the starting material and the zinc bromide-promoted B〇c_ removal protection as in Example 8 Step 8 were used. The title compound was obtained as a white foam m. MS (ESI+, M+H): 477. Example 30 trans-N-cyclopropyl-N-{[2,3-dioxa-5-(2-cyanoethyl)phenyl]indolyl}_4_(1_methyl-2-keto- 1,2-dihydro-4-Ppyridyl)-3-hexahydropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺26及如在實例14步驟8中之溴化鋅(11)_促進之B〇c_ 去除保護。獲得標題化合物,為白色泡珠物。Ms (ESI+, M+H). 487。人類腎素1C5 〇 (緩衝劑):8·4 nM。人類腎素汇5 〇 (血 漿):17 nM。 實例31 反式-(2-{3’4-二氣_5-[(環丙基{[4-(1-曱基-2-酮基-i,2-二氫_4-p比咬 基)-3-六氫'»比咬基]幾基}胺基)甲基]苯基丨乙基)胺基甲酸乙酯 143482-1 -196· 201111364The procedure described in Example 1 was followed, but instead the amine 26 as the starting material and the zinc bromide (11)-promoted B〇c_ removal protection as in Example 8 Step 8. The title compound was obtained as a white blister. Ms (ESI+, M+H). 487. Human renin 1C5 〇 (buffer): 8.4 nM. Human renin sink 5 血 (blood): 17 nM. Example 31 trans-(2-{3'4-digas_5-[(cyclopropyl{[4-(1-mercapto-2-one)-i,2-dihydro_4-p ratio bite Ethyl)-3-hexahydro'»bitergic]amino}amino)methyl]phenylhydrazineethyl)urethane 143482-1 -196· 201111364

MeMe

物 起始物質。獲得標題化合 549 為白色固體。MS (ESI+,M+H): 實例32 反式卿漠基·5-[3-(曱氧基)丙基]苯基}甲基)-N-環丙基-4仆 曱基2酮1,2-一氫_4:比唆基)冬六氫被咬叛醢胺Starting material. The title compound 549 was obtained as a white solid. MS (ESI+, M+H): Example 32 trans-invitrogen 5-[3-(decyloxy)propyl]phenyl}methyl)-N-cyclopropyl-4-mercapto 2 ketone 1 , 2-monohydrogen _4: thiol) winter hexahydrogen bite retinoin

MeMe

CC 步驟1 .反式-3-{[[3-溴基-5-(3-甲氧基丙基)宇基](環丙基)胺基] 羰基丨·4_(1_甲基_2_酮基_u_二氫咻啶斗基)小六氫吡啶羧酸第 三-丁酯 於反式-1-{[(1,1-二甲基乙基)氧基]羰基卜4 (1曱基_2酮基 -1,2-二氫-4-吡啶基)-3-六氫吡啶羧酸(1當量,實例i步驟6)、 Hunig氏鹼(3當量)及胺28(1當量)之DMF (〇 1M)溶液中,分次 添加六氟磷酸0-(7-氮苯并三唑_1_基)_N,N,N,,N,_ra曱基錁(12 當量)。將所形成之反應溶液在室溫下攪拌48小時》將目前 黃色溶液以EtOAc稀釋,並以1〇% HC1水溶液、IN NaOH水溶 液及鹽水相繼洗滌。然後,使有機萃液以Na2S〇4脫水乾燥, 143482,1 -197- 201111364 過濾,及使濾液在真空中濃縮,而得帶紅橘色油。如此獲 得之粗產物經由急驟式層析之純化(Si〇2,土95 (v/vj 在MeOH中之2.OMNH3 : CH^2) ’獲得標題化合物,為黃色 步驟2 :反式-N-({3-溴基-5-[3-(甲氧基)丙基]苯基}甲基)界環丙 基-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺 於得自前一步驟之反式-3-{[[3-溴基-5-(3-甲氧基丙基)爷基] (環丙基)胺基]幾基}-4-(1-甲基-2-酮基-i,2_二氫吡啶斗基)小六 氫吡啶羧酸第三-丁酯(1當量)之(¾¾溶液(0·05Μ)中,添加鲁 HC1(4.0M二氧陸圜溶液,30當量)^將所形成之溶液在室溫 下攪拌1.5小時。於真空中移除揮發性物質之後,將所形成 之殘留物直接地裝填至以93:7 (v/v) CH2C12 :在MeOH中之2.0Μ NH3填充之Si〇2管柱上。以相同溶劑系統之溶離,獲得標題 化合物,為白色泡泳物。MS (ESI+,M+H) : 516。 實例33 反式-N-環丙基-4-(1-曱基-2-酮基-1,2-二氫-4-p比。定基)-N-({5-[3-(甲氧基)丙基]-3-聯苯基}甲基)-3-六氫吡啶羧醯胺CC Step 1. trans-3-{[[3-Bromo-5-(3-methoxypropyl)ylidene](cyclopropyl)amino]carbonylcarbonyl·4_(1_methyl_2 _keto-_u_dihydroindolyl) small hexahydropyridinecarboxylic acid tert-butyl ester in trans-1-{[(1,1-dimethylethyl)oxy]carbonyl b 4 ( 1 mercapto-2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridinecarboxylic acid (1 equivalent, Example i Step 6), Hunig's base (3 equivalents) and amine 28 (1) In an equivalent amount of DMF (〇1M) solution, 0-(7-azabenzotriazol-1-yl)-N,N,N,,N,-ra-indole (12 equivalents) of hexafluorophosphate was added in portions. The resulting reaction solution was stirred at room temperature for 48 hours. The current yellow solution was diluted with EtOAc and washed sequentially with 1% aqueous HCl solution, aqueous NaOH solution and brine. Then, the organic extract was dehydrated and dried over Na 2 S 〇 4, filtered, 143482, 1-197-201111364, and the filtrate was concentrated in vacuo to give a red orange oil. The crude product thus obtained was purified by flash chromatography (Si.sub.2, EtOAc (m/vj. ({3-Bromo-5-[3-(methoxy)propyl]phenyl}methyl)-b-cyclopropyl-4-(1-mercapto-2-one-1,2-dihydro 4-pyridyl)_3_hexahydropyridine carboxamide in trans-3-{[[3-bromo-5-(3-methoxypropyl)-yl] (cyclopropyl) from the previous step Amino]amino]-4-(1-methyl-2-keto-i,2-dihydropyridyl) tris-butylpyridine carboxylic acid tri-butyl ester (1 equivalent) (3⁄43⁄4 In the solution (0·05Μ), Lu HC1 (4.0M dioxane solution, 30 equivalents) was added, and the resulting solution was stirred at room temperature for 1.5 hours. After removing volatile substances in a vacuum, it was formed. The residue was directly loaded onto a column of a mixture of the following solvent: MS (ESI+, M+H): 516. Example 33: &lt;RTI ID=0.0&gt;&gt; -N-({5-[3-(methoxy)propane) ] -3-biphenylyl} methyl) -3-piperidine-2carboxamide

步驟1 :反式-3-[(環丙基{[5-(3-甲氧基丙基)聯苯-3-基]曱基}胺 基)羰基]-4-(1-曱基-2-酮基-U-二氫吡啶-4-基)六氫吡啶-1-羧酸 第三-丁酯 143482-1 •198- 201111364 將反式-3-{[[3-溴基-5-(3-曱氧基丙基)芊基](環丙基)胺基]羰 基}-4-(1-曱基-2-酮基-1,2-二氫p比。定-4-基)-1-六氫p比咬級酸第三 -丁酯(1.0當量’實例32步驟1)、苯基二羥基硼烷(1.2當量) 及碳酸鈉(4_0當量)在DMF (0.1M)中之溶液重複抽氣,並以氮 逆充填。然後,添加Pd(dppf)Cl2(0.13當量),並將燒瓶抽氣, 且以氮再一次回填。將反應混合物加熱至9CTC,歷經16小 時’及在100-110 C下30分鐘。使反應混合物冷卻至室溫, 鲁 並自水以EtOAc萃取。使合併之有機萃液以Na2S〇4脫水乾 燥,過濾,及使濾液在真空中濃縮。如此獲得之粗產物經 由急驟式層析之純化(Si〇2,EtOAc~^· 5:95 (v/v)在MeOH中之 2.0M NHS . CH2 〇2) ’獲得標題化合物,為淡褐色油β 步驟2 :反式-Ν-環丙基-4-(1-甲基-2-酮基-1,2-二氫-4-&lt;:比咬 基)-Ν-({5-[3-(曱氧基)丙基]-3-聯苯基}曱基)_3-六氫ρ比咬緩醯胺 於得自前一步驟之反式-3-[(環丙基{[5-(3-曱氧基丙基)聯苯 -3-基]曱基}胺基)数基]-4-(1-甲基-2-酮基-1,2-二氫吡咬_4_基)六 φ 氫?比咬-1·羧酸第三-丁酯(1當量)之CKCl2溶液(〇.05Μ)中,添 加HC1(4.0M二氧陸圜溶液,30當量)。將所形成之溶液在室 溫下攪拌45分鐘。於真空中移除揮發性物質之後,將所形 成之殘留物直接地裝填至以93:7 (v/v) CI^Cl2 :在MeOH中之 2.0M NH3填充之Si〇2管柱上。以相同溶劑系統之溶離,獲得 標題化合物,為白色泡沫物。MS (ESI+,M+H) : 510人類腎 素IC5〇(緩衝劑):15nM。人類腎素1(:5〇(血漿):81nM。 實例34 反式-N-環丙基-4-(1-甲基-2-酮基-i,2_二氫_4-吡啶基(曱 143482-1 - 199- 201111364Step 1: trans-3-[(cyclopropyl{[5-(3-methoxypropyl)biphenyl-3-yl]indolyl)amino)carbonyl]-4-(1-indenyl- 2-keto-U-dihydropyridin-4-yl)hexahydropyridine-1-carboxylic acid tert-butyl ester 143482-1 •198- 201111364 trans-3-{[[3-bromo-5 -(3-methoxypropyl)indenyl](cyclopropyl)amino]carbonyl}-4-(1-mercapto-2-one-1,2-dihydrop ratio. Base)-1-hexahydrop to bite-acid acid tert-butyl ester (1.0 equivalents 'Example 32 Step 1), phenyl dihydroxyborane (1.2 equivalents) and sodium carbonate (4_0 equivalents) in DMF (0.1M) The solution in the solution was repeatedly evacuated and counter-filled with nitrogen. Then, Pd(dppf)Cl2 (0.13 equivalent) was added, and the flask was evacuated and backfilled again with nitrogen. The reaction mixture was heated to 9 CTC for 16 hours' and at 100-110 C for 30 minutes. The reaction mixture was cooled to rt then EtOAc (EtOAc) The combined organic extracts were dried with Na2SO4, filtered and filtered. The crude product thus obtained was purified by flash chromatography (EtOAc EtOAc EtOAc (EtOAc) β Step 2: trans-Ν-cyclopropyl-4-(1-methyl-2-keto-1,2-dihydro-4-&lt;: than bite)-Ν-({5-[ 3-(decyloxy)propyl]-3-biphenyl}indenyl)_3-hexahydro-p-butanyl hydrazide is obtained from the previous step -3-[(cyclopropyl{[5- (3-methoxypropyl)biphenyl-3-yl]fluorenyl}amino)numberyl]-4-(1-methyl-2-keto-1,2-dihydropyridyl_4_ Base) six φ hydrogen? HCl (4.0 M dioxane solution, 30 equivalents) was added to a CKCl2 solution (〇.05Μ) of a bite-1·carboxylic acid tert-butyl ester (1 equivalent). The resulting solution was stirred at room temperature for 45 minutes. After removal of the volatiles in vacuo, the resulting residue was loaded directly onto a &lt;RTI ID=0.0&gt;&gt;&gt;&gt; The title compound was obtained as a white foam. MS (ESI+, M+H): 510 human renin IC5 (buffer): 15 nM. Human renin 1 (: 5 〇 (plasma): 81 nM. Example 34 trans-N-cyclopropyl-4-(1-methyl-2-keto-i,2-dihydro-4-pyridyl (曱143482-1 - 199- 201111364

氧基)丙基]-5-(3-p比咬基)苯基]甲基}-3-六氫p比。定敌醯胺 根據實例33中所述之程序製成,但在步驟i中,替代地 使用p比β定-3-二經基删烧作為起始物質。獲得標題化合物, 為白色固體。MS (ESI+,Μ+Η) : 515。 實例35 反式-N-環丙基-N-[(2,3-二氯-5-{[2-(甲氧基)乙基]胺基丨苯基)曱 基]-4-(1-曱基-2-酮基-1,2-二氫-4-p比咬基)-3-六氫峨咬叛醯胺Oxy)propyl]-5-(3-p ratio dimethyl)phenyl]methyl}-3-hexahydrop ratio. The entamamine was prepared according to the procedure described in Example 33, but in the step i, p was used as the starting material instead of the ? The title compound was obtained as a white solid. MS (ESI+, Μ+Η): 515. Example 35 trans-N-cyclopropyl-N-[(2,3-dichloro-5-{[2-(methoxy)ethyl]aminoindolylphenyl)indolyl]-4-(1) -mercapto-2-keto-1,2-dihydro-4-p ratio thiol)-3-hexahydropurine ruthenium

步驟1 :反式-3-({環丙基[(2,3-二氯-5-{[2-(曱氧基)乙基]胺基}苯 基)曱基]胺基}幾基)-4-(1-甲基-2-酮基-1,2-二氫-4-p比咬基)-1-六鲁 氫吡啶羧酸1,1-二曱基乙酯 將剛純化之碳酸鉋(1.4當量)、醋酸鈀(π) (〇.〇2當量)及外 消旋-BINAP (〇.〇3當量)合併於無水甲苯(〇 〇8M)中。將容器重 複抽氣’並以氮逆充填。最後’添加反式_3_{[[(5_演基_2,3-二 氣苯基)曱基](環丙基)胺基]羰基卜4-(1_曱基_2_酮基-1,2-二氫-4-吡啶基)-1-六氫吡啶羧酸1,1-二曱基乙酯(丨〇當量,實例27)與 2-甲氧基乙胺(1.2當量),且將所形成之混合物於10〇°c下加 熱20小時。使目前黑色懸浮液冷卻至室溫,以Et〇Ac與飽和 143482-1 -200- 201111364 NH4C1水溶液稀釋。然後,分離有機層,以水與鹽水進一步 洗滌,以Na2S〇4脫水乾燥,過濾,及使濾液在真空中濃縮。 如此獲得之粗產物經由管柱層析之純化(Si〇2,96:4 CH2(^ : 在MeOH中之2.0MNH3),獲得標題化合物,為黃色油。 步驟2 :反式-N-環丙基-N-[(2,3-二氯-5-{[2-(甲氧基)乙基]胺基} 苯基)甲基]-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧 醯胺 於得自前一步驟之反式-3-({環丙基[(2,3-二氯-5-{[2-(甲氧 基)乙基]胺基}苯基)甲基]胺基}幾基)-4-(1-曱基-2-酮基_ι,2-二 氫-4-吡啶基)-1-六氫吡啶羧酸二曱基乙酯(1當量)之 CH2 (¾溶液(0.09M)中,添加HC1 (4.0M二氧陸園溶液,30當 量)。將所形成之溶液在室溫下攪拌4小時。於真空中移除 揮發性物質之後’將所形成之殘留物直接地裝填至以95:5 (v/v) CH2C12 :在MeOH中之2.0M NH3填充之Si02管柱上。以相 同溶劑系統之溶離,獲得所要之化合物,但仍然被不純物 污染。使用製備型HPLC-MS之進一步純化(C-18逆相管柱, 15 毫升 / 分鐘,95:5 (v/v) H20: CH3CN~^ 5:95 (v/v) H20: CH3CN), 獲得標題化合物,為白色固體。MS (ESI+,M+H) : 508 » 實例36 反式-N-環丙基-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)-N-[(3-{[2-(曱氧基)乙基]胺基Η-莕基)甲基]-3-六氫吡啶羧醯胺 143482-1 -201 · 201111364Step 1: trans-3-({cyclopropyl[(2,3-dichloro-5-{[2-(decyloxy)ethyl)amino}phenyl)indolyl]amino}yl -4-(1-methyl-2-keto-1,2-dihydro-4-p ratio), 1,1-didecylethyl ester of 1-hexahydrohydropyridinecarboxylate will be purified Carbonate planer (1.4 equivalents), palladium acetate (π) (〇.〇2 equivalent) and racemic-BINAP (〇.〇3 equivalent) were combined in anhydrous toluene (〇〇8M). The vessel was repeatedly evacuated&apos; and backfilled with nitrogen. Finally 'adding trans_3_{[[(5_基基_2,3-diphenyl)indolyl](cyclopropyl)amino]carbonyl-4- 4-(indolyl-2-yl) 1,1-didecylethyl ester of -1,2-dihydro-4-pyridyl)-1-hexahydropyridinecarboxylate (丨〇 equivalent, Example 27) and 2-methoxyethylamine (1.2 equivalents) The resulting mixture was heated at 10 ° C for 20 hours. The current black suspension was allowed to cool to room temperature and diluted with Et 〇Ac and saturated 143482-1 -200-201111364 NH4C1 aqueous solution. Then, the organic layer was separated, washed further with water and brine, dried over Na 2 EtOAc, filtered, and concentrated. The crude product thus obtained was purified by column chromatography (EtOAc: EtOAc: EtOAc (EtOAc) --N-[(2,3-dichloro-5-{[2-(methoxy)ethyl]amino}phenyl)methyl]-4-(1-indol-2-yl-- 1,2-Dihydro-4-pyridyl)-3-hexahydropyridine carboxamide in trans-3-({cyclopropyl[(2,3-dichloro-5-{[]) 2-(Methoxy)ethyl]amino}phenyl)methyl]amino}yl)-4-(1-indol-2-ylyl-ι,2-dihydro-4-pyridyl In the CH2 (3⁄4 solution (0.09M) of 1-hexahydropyridinecarboxylate (1 eq.), HCl (4.0 M dioxane solution, 30 eq.) was added. The resulting solution was Stir at room temperature for 4 hours. After removing the volatiles in vacuo, the residue formed was directly loaded into a SiO2 column filled with 95:5 (v/v) CH2C12: 2.0 M NH3 in MeOH. The desired compound was obtained by dissolving in the same solvent system, but was still contaminated with impurities. Further purification by preparative HPLC-MS (C-18 reverse phase column, 15 ml/min, 95:5 (v/) v) H20: CH3CN~^ 5:95 (v/v) H20: CH3CN), ield of the title compound as a white solid. MS (ESI+, M+H): 508 » Example 36 trans-N-cyclopropyl- 4-(1-Mercapto-2-keto-1,2-dihydro-4-pyridyl)-N-[(3-{[2-(decyloxy)ethyl]aminopurine-fluorenyl) )methyl]-3-hexahydropyridine carboxamide 143482-1 -201 · 201111364

、〇Me 根據實例1中所述之轾皮 径序I成’但替代地使用胺29作為 起始物質。獲得標題化人铷电二反 。物’為白色固體。MS (ESI+,m+h): 489。腎素IC5 〇 (緩衝劑):$ U 53 ηΜ。人類腎素IC50(血漿):2.4〇Me According to the suede path sequence I described in Example 1, but instead of using amine 29 as a starting material. Obtained the title of the person, the second person. The object 'is a white solid. MS (ESI+, m+h): 489. Renin IC5 〇 (buffer): $ U 53 ηΜ. Human renin IC50 (plasma): 2.4

nM 反式-N-{ [6-(2-氰基乙 -2-嗣基-1,2-二氮-4-口比 實例37 基)-8-4啉基]甲基}_N_環丙基冰(1•曱 。定基)-3-六氫吡啶羧醯胺 基nM trans-N-{[6-(2-cyanoethyl-2-indolyl-1,2-diaza-4-port ratio 37-group)-8-4 phenyl]methyl}_N_ ring Propyl ice (1•曱. 定)-3-hexahydropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺30及如在實例14步驟8中之溴化鋅(II)-促進之BOC-去除保護。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 470。 實例38 反式-N-環丙基-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)-N-({3-[2-(甲氧基)乙基]小莕基}曱基)-3-六氫吡啶羧醯胺 143482-1 •202- 201111364The procedure described in Example 1 was followed, but instead the amine 30 as the starting material and the zinc (II) bromide-promoted BOC-removal protection as in Example 8 Step 8. The title compound was obtained as a white foam. MS (ESI+, M+H): 470. Example 38 trans-N-cyclopropyl-4-(1-indol-2-one-1,2-dihydro-4-pyridyl)-N-({3-[2-(methoxy) Ethyl] hydrazino} decyl)-3-hexahydropyridine carboxamide 143482-1 • 202- 201111364

根據實例1中所述之程序製成,但替代地使用胺31作為 起始物質。獲得標題化合物,為白色固體。MS (ESI+, M+H): 474 〇 實例39 φ 反式-N-({3-[2-(乙醯胺基)乙基]小萘基}甲基)-N-環丙基-4-(1-甲 基-2-_基-1,2-二氫-4-p比咬基)-3-六氫p比咬叛醢胺It was made according to the procedure described in Example 1, but instead using amine 31 as the starting material. The title compound was obtained as a white solid. MS (ESI+, M+H): 474 〇 Example 39 φ trans-N-({3-[2-(ethylamino)ethyl]]-naphthalenyl}methyl)-N-cyclopropyl-4 -(1-Methyl-2-yl-1,2-dihydro-4-p ratio octyl)-3-hexahydrop ratio

根據實例1中所述之程序製成,但替代地使用胺32作為 起始物質。獲得標題化合物,為白色固體。MS (ESI+,M+H): 501。 實例40 反式-N-[(2-溴苯基)曱基]-N-環丙基-4-(1-甲基-2-酮基-1,2-二氫 -4-吡°定基)-3-六氫吡。定羧醯胺It was made according to the procedure described in Example 1, but instead using amine 32 as the starting material. The title compound was obtained as a white solid. MS (ESI+, M+H): 501. Example 40 trans-N-[(2-bromophenyl)indolyl]-N-cyclopropyl-4-(1-methyl-2-keto-1,2-dihydro-4-pyridyl) )-3-hexahydropyrrole. Carboxylamidine

根據實例1中所述之程序製成,但替代地使用胺33作為 143482-1 •203· 201111364 起始物質。獲得標題化合物,為白色固體。MS (ESI+,M+H): 444 〇 實例41 反式'N-環丙基-4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)-Ν-({1-[2-(曱氧基)乙基HH-啕哚-3-基}曱基)-3-六氫吡啶羧醯胺Prepared according to the procedure described in Example 1, but instead using amine 33 as the starting material for 143482-1 • 203 201111364. The title compound was obtained as a white solid. MS (ESI+, M+H): 444 〇 Example 41 trans <N-cyclopropyl-4-(1-methyl-2-keto-1,2-dihydro-4-pyridyl)-indole- ({1-[2-(decyloxy)ethylHH-indol-3-yl}indolyl)-3-hexahydropyridinecarboxamide

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺34及如在實例14步驟8中之溴化鋅(II)-促進之BOC-去除保護。獲得標題化合物,為白色泡洙物。MS (ESI+, M+Na) : 485。 實例42 反式-N-環丙基-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)-Ν-{[1-(2,2,2-三氟乙基)·1Η_叫丨嗓-3_基]曱基}_3-六氫吡咬羧醯胺The procedure described in Example 1 was followed, but instead the amine 34 as the starting material and the zinc (II) bromide-promoted BOC-removal protection as in Example 8 Step 8. The title compound was obtained as a white foam. MS (ESI+, M+Na): 485. Example 42 trans-N-cyclopropyl-4-(1-indol-2-one-1,2-dihydro-4-pyridyl)-indole-{[1-(2,2,2- Trifluoroethyl)·1Η_丨嗓丨嗓-3_yl]fluorenyl}_3-hexahydropyridylcarboxamide

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺35及如在實例14步驟8中之溴化鋅(Π)-促進之BOC-去除保護。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 487。 實例43 143482-1 -204- 201111364 反式-N-環丙基_4_(ι_甲基-2-嗣基-1,2-二鼠-4-p比。定基 (4,4,4-三氟丁基)丨哚_3_基;j曱基卜3-六氫吡啶羧醯胺The procedure described in Example 1 was followed, but instead the amine 35 as the starting material and the zinc bromide-promoted BOC-removal protection as in Example 8 Step 8. The title compound was obtained as a white foam. MS (ESI+, M+H): 487. Example 43 143482-1 -204- 201111364 trans-N-cyclopropyl_4_(ι_methyl-2-mercapto-1,2-dimur-4-p ratio. Stationary (4,4,4- Trifluorobutyl)indole_3_yl;j曱kib 3-hexahydropyridinecarboxamide

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺36及如在實例14步驟8中之溴化鋅(Π)-促進之B0C_ 去除保護。獲得標題化合物,為白色泡泳物。MS (ESI+, M+H) : 515。 實例44 反式-N-[(l-丁基-1H-蚓哚-3-基)曱基]-N-環丙基-4-(1-曱基_2-酮 基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺The procedure described in Example 1 was followed, but instead the amine 36 as the starting material and the zinc bromide-promoted BOC_ removal protection as in Example 8 Step 8 were used. The title compound was obtained as a white soak. MS (ESI+, M+H): 515. Example 44 trans-N-[(l-butyl-1H-indol-3-yl)indolyl]-N-cyclopropyl-4-(1-indolyl-2-keto-1,2- Dihydro-4-pyridyl)-3-hexahydropyridine carboxamide

MeMe

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺37及如在實例14步驟8中之溴化辞(Π)-促進之BOC-去除保護。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 461。 實例45 反式-N-環丙基-Ν-({1-[3-(乙氧基)丙基HH-⑼哚-3-基}曱基)_ 4-(1-曱基-2-嗣基-1,2-二氣-4-p比咬基)-3-六氮p比咬叛酿胺 143482-1 -205- 201111364The procedure described in Example 1 was followed, but instead the amine 37 as the starting material and the brominated (C)-promoted BOC-removal protection as in Example 8 Step 8. The title compound was obtained as a white foam. MS (ESI+, M+H): 461. Example 45 trans-N-cyclopropyl-indole-({1-[3-(ethoxy)propylHH-(9)indol-3-yl}indenyl)-4-(1-indolyl-2-) Mercapto-1,2-digas-4-p ratio bite base)-3-hexanitrogen p than bite-resistant amine 143482-1 -205- 201111364

MeMe

根據實例1中所述之程序製成’但替代地使用作為起始 物質之胺38及如在實例14步驟8中之溴化鋅(π)-促進之boc- 去除保護。獲得標題化合物,為白色泡沐物。MS (ESI+, M+H) : 491。 實例46 反式-N-環丙基-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)-Ν-({1-[3,3,3-二亂-2-(二氟^曱基)丙基]丨嗓-3基}曱基)-3-六氫p比咬 羧醯胺The amine 38 as the starting material and the zinc bromide (π)-promoted boc-removal protection as in the step 8 of Example 14 were prepared as follows according to the procedure described in Example 1. The title compound was obtained as a white foam. MS (ESI+, M+H): 491. Example 46 trans-N-cyclopropyl-4-(1-indol-2-one-1,2-dihydro-4-pyridyl)-indole-({1-[3,3,3- 2-dis-2-(difluoro(fluorenyl)propyl]indol-3-yl}mercapto)-3-hexahydrop

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺39及如在實例14步驟8中之溴化鋅(II)-促進之BOC-去除保護。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 569。 實例47 反式-Ν-({1-[3-(乙醯胺基)丙基HH-啕哚-3-基}甲基)-N-環丙基 -4-(1-曱基-2-酮基-1,2-二氫-4-p比β定基)-3-六氫叶I: °定叛醯胺 143482-1 -206- 201111364The procedure described in Example 1 was followed, but instead the amine 39 as the starting material and the zinc (II) bromide-promoted BOC-removal protection as in Example 8 Step 8. The title compound was obtained as a white foam. MS (ESI+, M+H): 569. Example 47 trans-Ν-({1-[3-(ethylamino)propyl)HH-indol-3-yl}methyl)-N-cyclopropyl-4-(1-indolyl-2 -keto-1,2-dihydro-4-p ratio β-fixed)-3-hexahydrogen I: ° 醯 醯 醯 143482-1 -206- 201111364

根據實例1中所述之程序製成’但替代地使用作為起始 物質之胺40及如在實例14步驟8中之溴化鋅(π)-促進之BOC-According to the procedure described in Example 1, 'but the amine 40 as the starting material and the zinc bromide (π)-promoted BOC as in the step 8 of Example 14 were used instead.

去除保護。獲得標題化合物,為白色泡沫物。MS (ESI+, Μ+Ϊ1) : 504。 實例48 反式-N-環丙基-4-(ι_甲基_2_酮基二氫斗吡啶基)N ({1[3_ (丙醯基胺基)丙基]·1Η-啕哚-3-基}甲基)各六氫吡啶羧醯胺Remove protection. The title compound was obtained as a white foam. MS (ESI+, Μ+Ϊ1): 504. Example 48 trans-N-cyclopropyl-4-(ι-methyl_2-ketodihydropyridinyl)N ({1[3_(propyl decylamino)propyl)·1Η-啕哚-3-yl}methyl)hexahydropyridine carboxamide

MeMe

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺41及如在實例14步驟8中之溴化鋅(11)_促進之b〇c_ 去除保護。獲得標題化合物,為白色泡沫物。MS (esi+, M+H) : 518。 實例49 反式-NAHM乙醢胺基)乙基]_1H_+朵各基}甲基)_N環丙基 斗(1-甲基-2-酮基-1,2-二氫斗吡啶基)各六氫吡啶羧醯胺 143482-1 •207· 201111364The procedure described in Example 1 was followed, but instead the amine 41 as the starting material and the bromide (11)-promoted b〇c_ removal protection as in step 8 of Example 14 were used. The title compound was obtained as a white foam. MS (esi+, M+H): 518. Example 49 trans-NAHM acetamino)ethyl]_1H_+poly}methyl)-N-cyclopropyl (1-methyl-2-keto-1,2-dihydropyridinyl) Hexahydropyridine carboxamide 143482-1 •207· 201111364

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺42及如在實例14步驟8中之溴化鋅(Π)-促進之B〇c_ 去除保s蒦。獲得標題化合物’為白色泡沐物。MS (ESI+ M+H) : 490。 實例50 反式-N-環丙基-4-(1-曱基-2-_基-i,2-二氫_4-P比。定基)-Ν-({ΐ·[2~ (丙醢基胺基)乙基]-1H-引哚-3-基}甲基)_3-六氫吡啶羧醯The procedure described in Example 1 was followed, but instead the amine 42 as the starting material and the zinc bromide-promoted B〇c_ removed in step 8 of Example 14 were used. The title compound was obtained as a white foam. MS (ESI+ M+H): 490. Example 50 trans-N-cyclopropyl-4-(1-indolyl-2-yl-i,2-dihydro_4-P ratio. Stationary)-Ν-({ΐ·[2~ (C Mercaptoamino)ethyl]-1H-indol-3-yl}methyl)_3-hexahydropyridinecarboxylate

胺 根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺43及如在實例14步驟8中之溴化鋅(II)-促進之boc-去除保s蒦。獲得標題化合物’為白色泡沐物。ms (ESI+, M+H) : 504 〇 實例51 反式-N-環丙基-4-(1-甲基_2_酮基-1,2-二氫-4-吡啶基)-N-{ [1-(2-丙 烯-1-基)-1Η-&lt;Ί朵-3-基]甲基}·3_六氫?比咬叛醢胺 143482-1 -208- 201111364The amine was prepared according to the procedure described in Example 1, but instead using amine 43 as the starting material and zinc (II)-promoted boc-removal as in Example 8. The title compound was obtained as a white foam. Ms (ESI+, M+H): 504 〇 Example 51 trans-N-cyclopropyl-4-(1-methyl-2-keto-1,2-dihydro-4-pyridyl)-N- { [1-(2-Prop-1-yl)-1Η-&lt;Ί-3-yl]methyl}·3_hexahydro? Than the bite of ruthenium 143482-1 -208- 201111364

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺44及如在實例14步驟8中之溴化鋅(II)-促進之BOC-去除保護。獲得標題化合物,為白色泡沫物^ MS (ESI+, M+H) : 445。 實例52 反式-N-環丙基_4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)_Ν-{[1-(苯 基甲基1)-1H-吲哚-3-基]甲基}-3-六氫吡啶羧醯胺The procedure described in Example 1 was followed, but instead the amine 44 as the starting material and the zinc (II) bromide-promoted BOC-removal protection as in Example 8 Step 8. The title compound was obtained as a white foam ( MS (ESI+, M+H): 445. Example 52 trans-N-cyclopropyl_4-(1-methyl-2-keto-1,2-dihydro-4-pyridyl)-indole-{[1-(phenylmethyl 1)- 1H-indol-3-yl]methyl}-3-hexahydropyridine carboxamide

MeMe

根據實例1中所述之程序製成,但替代地使用作為起始 # 物質之胺45及如在實例14步驟8中之溴化辞(II)-促進之BOC- 去除保δ蒦。獲得標題化合物,為白色泡泳物。ms (esi+, M+H) : 495。 實例53 反式-N-環丙基-4-(1-甲基_2_酮基],2_二氫_4_吡啶基)_Ν-{[ι_(2_吡 咬基甲基)-1Η-Ί丨哚-3-基]甲基卜3_六氫吡啶羧醯胺 143482-1 -209- 201111364It was made according to the procedure described in Example 1, but instead using the amine 45 as the starting material and the brominated (II)-promoted BOC- removing δ in the step 8 of Example 14. The title compound was obtained as a white soak. Ms (esi+, M+H): 495. Example 53 trans-N-cyclopropyl-4-(1-methyl-2-keto), 2-dihydro-4-pyridyl)_Ν-{[ι_(2_pyridylmethyl)- 1Η-Ί丨哚-3-yl]methyl b 3_hexahydropyridine carboxamide 143482-1 -209- 201111364

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺46及如在實例14步驟8中之溴化鋅(II)-促進之b〇c_ 去除保護。獲得標題化合物,為白色泡沐物^ MS (ESI+, M+H) : 496。 實例54 反式-N-環丙基-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)-N-{比 咬基甲基)-1Η-吲哚-3-基]甲基}-3-六氫吡啶羧醯胺The procedure described in Example 1 was followed, but instead the amine 46 as the starting material and the zinc(II) bromide-promoted b〇c_ removal protection as in Example 8 Step 8. The title compound was obtained as a white foam (MS+, M+H): 496. Example 54 trans-N-cyclopropyl-4-(1-indol-2-one-1,2-dihydro-4-pyridyl)-N-{bitenylmethyl)-1Η-吲Indole-3-yl]methyl}-3-hexahydropyridine carboxamide

MeMe

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺47及如在實例14步驟8中之溴化鋅(II)-促進之boc- 去除保護。獲得標題化合物,為白色泡珠物。MS (ESI+, M+H) : 496。 實例55 反式-N-環丙基-4-(1-曱基_2-酮基-1,2-二氫-4-吡啶基)-N-{ [1-(4-峨 啶基曱基)-1Η-吲哚-3-基]甲基卜3_六氫吡啶羧醯胺 143482-1 -210- 201111364The procedure described in Example 1 was followed, but instead the amine 47 as the starting material and the zinc (II)-promoted boc-removal protection as in Example 8 Step 8. The title compound was obtained as a white blister. MS (ESI+, M+H): 496. Example 55 trans-N-cyclopropyl-4-(1-indolyl-2-keto-1,2-dihydro-4-pyridyl)-N-{ [1-(4-acridinyl) Base)-1Η-吲哚-3-yl]methyl b 3_hexahydropyridine carboxamide 143482-1 -210- 201111364

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺48及如在實例14步驟8中之溴化鋅⑼促進之B〇c_ 去除保護。獲得標題化合物,為白色泡沫物。Ms (Esi+, M+H) : 496。The procedure described in Example 1 was followed, but instead the amine 48 as the starting material and the B〇c_ removal protection as promoted by zinc bromide (9) in Step 8 of Example 14 were used. The title compound was obtained as a white foam. Ms (Esi+, M+H): 496.

實例56 反式-N-環丙基-Ν-({Η(4·氟苯基)甲基]_m吲哚_3基}甲 基)-4-(1-甲基-2-酮基-l,2-二氫_4-吡啶基)_3_六氫吡啶羧醯胺Example 56 trans-N-cyclopropyl-indole-({Η(4.fluorophenyl)methyl]_m吲哚_3yl}methyl)-4-(1-methyl-2-keto- l,2-Dihydro-4-pyridyl)_3_hexahydropyridine carboxamide

MeMe

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺49及如在實例14步驟8中之漠化鋅(II)-促進之B0C_ 去除保護。獲得標題化合物’為白色泡珠物。MS (ESI+, M+H) : 513。 實例57 反式-Ν-({1-[(4-氣苯基)曱基]-1H-吲哚各基}甲基)-N-環丙基 -4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺 143482-1 •211- 201111364The procedure described in Example 1 was followed, but instead the amine 49 as the starting material and the zinc (II)-promoted BOC_ removal protection as in the step 8 of Example 14 were used. The title compound was obtained as a white blister. MS (ESI+, M+H): 513. Example 57 trans-Ν-({1-[(4-Phenylphenyl)indolyl]-1H-indoleyl}methyl)-N-cyclopropyl-4-(1-methyl-2- Ketopropyl-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide 143482-1 •211- 201111364

MeMe

Cl 根據實例l中所述之程序製成,但替代地使用作為起始 物質之胺50及如在實例14步驟8中之溴化鋅(π)_促進之B〇c_ 去除保護。獲得標題化合物’為白色泡沫物。MS (ESI+,M+H): 529。 實例58 反式-N-環丙基-Ν-({1-[(3-氟苯基)甲基HH-吲哚-3-基}曱基)-4-(1-曱基-2-酮基-1,2-二氫-4-1»比α定基)-3-六氫p比。定叛酿胺Cl was prepared according to the procedure described in Example 1, but instead using amine 50 as the starting material and B〇c_ removal protection as in zinc bromide (π)_promoted in step 8 of Example 14. The title compound was obtained as a white foam. MS (ESI+, M+H): 529. Example 58 trans-N-cyclopropyl-indole-({1-[(3-fluorophenyl)methylHH-indol-3-yl}indolyl)-4-(1-indolyl-2- The ratio of keto-1,2-dihydro-4-1» to α-based)-3-hexahydrop. Detached amine

MeMe

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺51及如在實例14步驟8中之溴化鋅(11)_促進之BOC-去除保護。獲得標題化合物,為白色泡珠物^ MS (ESI+, M+H) : 513。 實例59 反式-Ν-({1-[(3-氯苯基)曱基]-1Η-Θ丨嗓-3-基}曱基)-N-環丙基 -4-(1-曱基-2-酮基-1,2-二氫_4_峨啶基)_3_六氫哺咬羧酿胺 143482-1 •212- 201111364The procedure described in Example 1 was followed, but instead the amine 51 as the starting material and the zinc bromide (11)-promoted BOC-removal protection as in Example 8 Step 8. The title compound was obtained as a white bead material &lt;EMI&gt; MS (ESI+, M+H): 513. Example 59 trans-Ν-({1-[(3-chlorophenyl)indolyl]-1Η-indol-3-yl}indenyl)-N-cyclopropyl-4-(1-indenyl) -2-keto-1,2-dihydro_4_acridinyl)_3_hexahydronized carboxylic amine 143482-1 •212- 201111364

根據實例1中所述之程序製成’但替代地使用作為起始 物質之胺52及如在實例14步驟8中之溴化鋅(II)-促進之boc-去除保護。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 529。 實例60 反式-Ν-({1-[(3-氰基苯基)甲基]-1H-吲哚-3-基}甲基)-N-環丙基 -4-(1-曱基-2-酮基-1,2-二氫-4-p比β定基)-3-六氳ρ比咬缓醯胺The amine 52 as the starting material and the zinc (II) bromide-promoted boc-removal protection as in the step 8 of Example 14 were prepared as follows according to the procedure described in Example 1. The title compound was obtained as a white foam. MS (ESI+, M+H): 529. Example 60 trans-Ν-({1-[(3-cyanophenyl)methyl]-1H-indol-3-yl}methyl)-N-cyclopropyl-4-(1-indenyl) -2-keto-1,2-dihydro-4-p ratio β-fixed)-3-hexafluoropyrene

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺53及如在實例14步驟8中之溴化鋅(Π)-促進之B0C_ 去除保護。獲得標題化合物,為白色泡洙物。MS (ESI+, M+H) : 520。 實例61 反式-N-環丙基-4-(ι_曱基_2_酮基_i,2二氫·4吡啶基)N ({1[(3_ 曱基苯基)曱基]_1H-吲哚-3-基}甲基)-3-六氫吡啶羧醯胺 143482-1 •213· 201111364The procedure described in Example 1 was followed, but instead the amine 53 as the starting material and the zinc bromide-promoted BOC_ removal protection as in Example 8 Step 8 were used. The title compound was obtained as a white foam. MS (ESI+, M+H): 520. Example 61 trans-N-cyclopropyl-4-(ι_indolyl-2-keto-i,2dihydro-4-pyridyl)N ({1[(3-nonylphenyl)indolyl]_1H -吲哚-3-yl}methyl)-3-hexahydropyridine carboxamide 143482-1 •213· 201111364

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺54及如在實例μ步称8中之溴化鋅(π)-促進之BOC- 去除保護。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 509。 實例62 反式-N-壤丙基-N-({5-氟基-l-[3-(甲氧基)丙基]_1Η_啕哚各基}曱 基)-4-(1-甲基-2-酮基-ΐ,2-二氫_4-吡啶基)_3_六氫毗啶羧醯胺The procedure described in Example 1 was followed, but instead the amine 54 as the starting material and the zinc bromide (π)-promoted BOC- removal protection as in Example μstep 8 were used. The title compound was obtained as a white foam. MS (ESI+, M+H): 509. Example 62 trans-N-platinyl-N-({5-fluoro-l-[3-(methoxy)propyl]_1Η-啕哚-yl}}yl)-4-(1-A Keto-2-keto-oxime, 2-dihydro-4-pyridyl)_3_hexahydropyridinium carboxamide

MeMe

Cr: rCr: r

OMe 根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺55及如在實例14步驟8中之溴化鋅(11)促進之B〇c_ 去除保護。獲得標題化合物,為白色泡沫物。ms(esi+ m+h): 495 » 實例63 反式-N-{[6-漠基-H苯基f基HH_十朵各基]甲基} N環丙基 -4-(1-甲基-2-酮基-1,2-二氫斗吡啶基)_3六氫吡啶羧醯胺 143482-1 •214 ‘ 201111364OMe was prepared according to the procedure described in Example 1, but instead using amine 55 as the starting material and B〇c_ removal protection as promoted by zinc bromide (11) in Step 8 of Example 14. The title compound was obtained as a white foam. Ms(esi+ m+h): 495 » Example 63 trans-N-{[6-Molyl-H-phenyl-f-based HH_decadetyl]methyl}N-cyclopropyl-4-(1-A Benz-2-keto-1,2-dihydropyridinyl)_3 hexahydropyridine carboxamide 143482-1 •214 ' 201111364

根據實例1中所述之程序製成,但替代地㈣作為起始 物質之胺56及如在實例14步驟8中之溴化鋅,足進之齡 去除保護。獲得標題化合物,為白色泡沐物。⑽卿+, M+H) : 573。It was prepared according to the procedure described in Example 1, but instead (4) the amine 56 as the starting material and the zinc bromide as in step 8 of Example 14, the age-removal protection. The title compound was obtained as a white foam. (10) Qing+, M+H): 573.

實例64 反式-N-環丙基-Ν-{[1·[(3_氣苯基)曱基]6 (甲氧基)_則卜朵_3_ 基]甲基Μ-α-甲基相基仏二氣‘比咬基)冬六氫峨錢 醯胺Example 64 trans-N-cyclopropyl-indole-{[1·[(3_-phenylphenyl)indenyl]6(methoxy)_jupo_3_yl]methylindole-α-methyl Phase-based 仏 two gas 'bite base' winter hexahydro hydrazine

根據實例1中所述之程序製成,但替代地使用作為起始 物貝之胺57及如在實例14步驟8中之溴化鋅⑼·促進之 去除保護。獲付標題化合物,為白色泡珠物。MS (ESI+, M+H) · 543 〇 實例65 反式-N•環丙基邻-甲基-2-嗣基-U-二&amp;如比咬基)_N.甲基 小(苯基甲基)-L朵各基]甲基}_3_六氫吡啶羧醢胺 143482-1 -215· 201111364The procedure described in Example 1 was followed, but instead the amine 57 as the starting material and the zinc bromide (9) in step 8 of Example 14 were used for the removal protection. The title compound was obtained as a white blister. MS (ESI+, M+H) · 543 〇 Example 65 trans-N•cyclopropyl o-methyl-2-mercapto-U-di-amp; such as bite base) _N. methyl small (phenyl group) Base)-L-polyyl]methyl}_3_hexahydropyridine carboxamide 143482-1 -215· 201111364

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺58及如在實例14步驟8中之溴化鋅(II)-促進之boc-去除保護。獲得標題化合物,為白色泡沐物。MS (ESI+, M+H) : 509。 實例66 反式-N-{[4-氰基-1-(苯基甲基)-1Η-吲哚-3-基]曱基}-N-環丙基 -4-(1-曱基-2-酬基-1,2-二氮-4-p比咬基)-3-六氮ρ比咬叛酸胺The procedure described in Example 1 was followed, but instead the amine 58 as the starting material and the zinc (II) bromide-promoted boc-removal protection as in Example 8 Step 8. The title compound was obtained as a white foam. MS (ESI+, M+H): 509. Example 66 trans-N-{[4-cyano-1-(phenylmethyl)-1Η-indol-3-yl]indolyl}-N-cyclopropyl-4-(1-indolyl- 2-retinyl-1,2-diaza-4-p ratio thiol)-3-hexanitro-p ratio

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺59及如在實例14步驟8中之溴化鋅(II)-促進之BOC-去除保護。獲得標題化合物’為白色泡沫物。MS (ESI+, M+H) : 520。 實例67 反式-N-環丙基-N-{[4-氟基-1-(苯基甲基)_ih-W哚-3-基]曱 基甲基-2-酮基-U-二氫-4-吡啶基)-3-六氫吡啶羧醢胺 143482-1 -216- 201111364The procedure described in Example 1 was followed, but instead the amine 59 as the starting material and the zinc (II) bromide-promoted BOC-removal protection as in Example 8 Step 8. The title compound was obtained as a white foam. MS (ESI+, M+H): 520. Example 67 trans-N-cyclopropyl-N-{[4-fluoro-1-(phenylmethyl)_ih-W哚-3-yl]nonylmethyl-2-keto-U-di Hydrogen-4-pyridyl)-3-hexahydropyridine carboxamide 143482-1 -216- 201111364

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺60及如在實例14步驟8中之溴化鋅(Π)-促進之BOC-去除保護。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 513。 實例68 反式-N-環丙基-N-({4-氟基-l-[(3-氟苯基)曱基HH-啕哚-3-基]曱 基}-4-(1-曱基-2-_基-1,2-二氫-4-?比。定基)-3-六氫p比咬叛醯胺The procedure described in Example 1 was followed, but instead the amine 60 as the starting material and the zinc bromide-promoted BOC-removal protection as in Example 8 Step 8 were used. The title compound was obtained as a white foam. MS (ESI+, M+H): 513. Example 68 trans-N-cyclopropyl-N-({4-fluoro-l-[(3-fluorophenyl)indolyl HH-indol-3-yl]indenyl}-4-(1- Mercapto-2-yl-1,2-dihydro-4-? ratio. Alkyl)-3-hexahydrop ratio

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺61及如在實例14步驟8中之溴化辞(π)_促進之BOC-去除保護。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H). 531。人類腎素1C5 〇 (緩衝劑):0.06 nM。人類腎素IC5〇 (血 漀):0.6 nM。 實例69 反式-N-%、丙基氟基曱氧基)丙基吲哚各基}曱 基Η-d-甲基-2-酮基-l,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺 143482-1 -217· 201111364The procedure described in Example 1 was followed, but instead the amine 61 as the starting material and the brominated (π)-promoted BOC-removal protection as in Example 8 Step 8. The title compound was obtained as a white foam. MS (ESI+, M+H). 531. Human renin 1C5 〇 (buffer): 0.06 nM. Human renin IC5 血 (blood sputum): 0.6 nM. Example 69 trans-N-%, propylfluoromethoxyoxy) propyl hydrazide} fluorenyl-d-methyl-2-keto-l,2-dihydro-4-pyridyl) _3_hexahydropyridine carboxamide 143482-1 -217· 201111364

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺62及如在實例14步驟8中之溴化鋅(π)-促進之B〇C_ 去除保護。獲得標題化合物,為白色泡床物。MS (ESI+, M+H): 495。4 NMR (CD3OD) (5 (ppm): 0.56-0.71 (m,1H),0.76-0.98 (m, 3H), 1.50-1.70 (m, 2H), 1.90 (m, 2H), 2.52 (m, 1H), 2.60-2.71 (m, 2H), 2.88 (td, J = 11.6, 3.9 Hz, 1H), 3.05 (br d, J = 7.0 Hz, 1H), 3.09-3.19 (m, 3H), 3.23 (s, 3H), 3.27 (s, 3H), 3.43-3.58 (m, 1H), 4.00-4.21 (m, 2H), 4.41 (d, J = 14.8 Hz, 1H), 4.7 (m, 2H), 6.11-6.22 (m, 1H), 6.30 (d, J = 1.8 Hz, 1H), 6.54-6.67 (m, 1H), 6.74 (s, 1H), 6.93-7.04 (m, 1H), 7.10 (d, J = 4.0 Hz,1H)’ 7·16 (d,J = 3.6 Hz, 1H)。人類腎素IC50(緩衝劑):0.3 nM °人類腎素I(:5〇(血漿):〇 9遍。 實例70 反式-Ν-({4-氣基-ΐ_[3-(曱氧基)丙基pm,哚_3_基}甲基環 丙基-4-(1-曱基_2_酮基+2-二氫_4_吡啶基六氫吡啶羧醯胺The procedure described in Example 1 was followed, but instead the amine 62 as the starting material and the zinc bromide (π)-promoted B〇C_ removal protection as in Example 8 Step 8 were used. The title compound was obtained as a white blister. </ RTI> <RTI ID (m, 2H), 2.52 (m, 1H), 2.60-2.71 (m, 2H), 2.88 (td, J = 11.6, 3.9 Hz, 1H), 3.05 (br d, J = 7.0 Hz, 1H), 3.09 -3.19 (m, 3H), 3.23 (s, 3H), 3.27 (s, 3H), 3.43-3.58 (m, 1H), 4.00-4.21 (m, 2H), 4.41 (d, J = 14.8 Hz, 1H ), 4.7 (m, 2H), 6.11-6.22 (m, 1H), 6.30 (d, J = 1.8 Hz, 1H), 6.54-6.67 (m, 1H), 6.74 (s, 1H), 6.93-7.04 ( m, 1H), 7.10 (d, J = 4.0 Hz, 1H)' 7·16 (d, J = 3.6 Hz, 1H). Human renin IC50 (buffer): 0.3 nM ° human renin I (: 5 〇 (Plasma): 〇 9 times. Example 70 trans-Ν-({4-Gayl-ΐ_[3-(oximeoxy)propyl pm, 哚_3_yl}methylcyclopropyl-4- (1-indenyl-2-keto+2-dihydro-4-pyridylhexahydropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺63及如在實例14步驟8中之溴化鋅(II)-促進之B〇C- 1434824 •218· 201111364 去除保遵。獲得標題化合物,為白色泡沫物。]Vis (ESI+, M+H) : 511。 實例71 反式-N-{[4-氣基小(苯基甲基)_1H-吲哚_3_基]曱基} N環丙基 -4-(1-曱基-2-酮基'2-二氫斗吡啶基)_3_六氫吡啶羧醯胺Prepared according to the procedure described in Example 1, but instead using the amine 63 as the starting material and the zinc(II) bromide as promoted in step 8 of Example 14 B〇C-1434824 •218·201111364 Bao Zun. The title compound was obtained as a white foam. ]Vis (ESI+, M+H): 511. Example 71 trans-N-{[4-Alkyl small (phenylmethyl)_1H-indole-3-yl]indenyl}N-cyclopropyl-4-(1-indol-2-oneyl) 2-dihydropyridinyl)_3_hexahydropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺64及如在實例14步驟8中之溴化鋅贝)促進之B〇c_ 去除保濩。獲得標題化合物,為白色泡沫物。MS (esi+, M+H) : 529。 實例72 反式-N-{[4-/臭基小(笨基甲基)_m啕哚_3基]甲基卜n環丙基 -4-(1-甲基-2-嗣基-1,2-二| _4·吡啶基)_3_六氫吡啶羧醯胺The procedure described in Example 1 was followed, but instead the amine 64 as the starting material and the zinc bromide as promoted in step 8 of Example 14 were used to remove the oxime. The title compound was obtained as a white foam. MS (esi+, M+H): 529. Example 72 trans-N-{[4-/ odoryl small (stupylmethyl)_m啕哚_3yl]methyl b-cyclopropyl-4-(1-methyl-2-indolyl-1 ,2-di| _4·pyridyl)_3_hexahydropyridine carboxamide

MeMe

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺65及如在實例14步騍8中之溴化鋅贝)促進之 去除保§蒦。獲得標題化合物,為自色泡;末物。⑽卿+, M+H) : 575。 實例73 143482-1 •219- 201111364It was prepared according to the procedure described in Example 1, but instead using the amine 65 as the starting material and the zinc bromide as in Example 14 step 8 to promote the removal of the hydrazine. The title compound was obtained as a color bubble; (10) Qing+, M+H): 575. Example 73 143482-1 • 219- 201111364

反式_N_({4-溴基-H(3-氟苯基)甲基HH-吲哚-3-基}甲基)-N-環 丙基-4-(1-甲基I酮基-1,2·二氫_4-p比啶基)-3_六氮p比啶羧醢胺 根據實例1中所述之程序製成’但替代地使用作為起始 物質之胺66及如在實例14步驟8中之溴化鋅(Π)-促進之BOC-去除保護。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 591.3。1H NMR (DMSO-d6) : 6 (ppm) 0.60-0.66 (m,1H), 0.89-0.94 (m, 3H), 1.56 (dd, J = 13.3, 10.6 Hz, 1H), 1.67 (d, J = 12.6 Hz, 1H), 2.58 (dt, J = 12.4, 2.2 Hz, 1H), 2.71 (s, 3H), 2.83-2.94 (m, 2H), 3.04 (br d, J = 6.1 Hz, 1H), 3.23 (s, 3H), 3.3 (dd, J = 6.7, 4.0 Hz, 1H), 3.04 (d, J = 12.3 Hz, 1H), 4.87 (q, J = l〇.l Hz, 2H), 5.35 (d, J = 2.6 Hz, 2H), 6.16-6.23 (m, 1H), 6.79 (s, 1H), 6.88 (d, J = 8.3 Hz, 2H), 6.99 (t, J = 7.9trans_N_({4-bromo-H(3-fluorophenyl)methylHH-indol-3-yl}methyl)-N-cyclopropyl-4-(1-methyl-1-keto -1,2·dihydro-4-p-pyridyl)-3_hexanitro-p-pyridylcarboxamide was prepared according to the procedure described in Example 1 but using amine 66 as a starting material instead and as The zinc bromide (Π)-promoted BOC-removal protection in step 8 of Example 14. The title compound was obtained as a white foam. MS (ESI+, M+H): 591.3. 1H NMR (DMSO-d6): 6 (ppm): 0.60-0.66 (m, 1H), 0.89-0.94 (m, 3H), 1.56 (dd, J = 13.3, 10.6 Hz, 1H), 1.67 (d, J = 12.6 Hz, 1H), 2.58 (dt, J = 12.4, 2.2 Hz, 1H), 2.71 (s, 3H), 2.83-2.94 (m, 2H), 3.04 (br d, J = 6.1 Hz, 1H), 3.23 (s, 3H), 3.3 (dd, J = 6.7, 4.0 Hz, 1H), 3.04 (d, J = 12.3 Hz, 1H), 4.87 (q, J = l 〇.l Hz, 2H), 5.35 (d, J = 2.6 Hz, 2H), 6.16-6.23 (m, 1H), 6.79 (s, 1H), 6.88 (d, J = 8.3 Hz, 2H), 6.99 ( t, J = 7.9

Hz, 1H), 7.05-7.12 (m, 1H), 7.20 (d, J = 7.5 Hz, 1H), 7.29-7.40 (m, 2H), 7.54(d,J = 6.9Hz,lH)。人類腎素 IC5〇(緩衝劑):&lt;〇〇6nM。人 類腎素IC50(血漿):〇.5nM。 反式N ({/臭基甲氧基)丙基]•♦朵各基)甲基)_n_環丙 實例74Hz, 1H), 7.05-7.12 (m, 1H), 7.20 (d, J = 7.5 Hz, 1H), 7.29-7.40 (m, 2H), 7.54 (d, J = 6.9 Hz, lH). Human renin IC5 〇 (buffer): &lt; 〇〇 6 nM. Human renin IC50 (plasma): 〇.5nM. Trans N ({/ odorylmethoxy) propyl] ♦ ♦ each group) methyl) _n _ ring C Instance 74

143482-1 201111364143482-1 201111364

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺67及如在實例14步驟8中之溴化鋅(Π)-促進之BOC- 去除保護。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 557。 實例75 反式-N_環丙基1[(4-氟基-1Η-ΘΙ哚-3-基)曱基]-4-(1-曱基-2-酮 基-1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺The procedure described in Example 1 was followed, but instead the amine 67 as the starting material and the zinc bromide-promoted BOC-removal protection as in Example 8 Step 8 were used. The title compound was obtained as a white foam. MS (ESI+, M+H): 557. Example 75 trans-N-cyclopropyl 1[(4-fluoroyl-1Η-indol-3-yl)indolyl]-4-(1-indol-2-ylyl-1,2-dihydro -4-pyridyl)_3_hexahydropyridine carboxamide

MeMe

步驟1 :反式-3-({環丙基[(4_氟基啕哚-3-基)曱基]胺基卜羰 基)-4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)-1-六氫吡咬羧酸1,1-二 甲基乙酯 於反式-1-{[(U-二曱基乙基)氧基]羰基}-4-(1-曱基-2-酮基 -1,2-二氫-4-吡啶基)-3-六氫吡啶羧酸(1當量,實例1步驟6)、 Hunig氏鹼(3當量)及胺68(1當量)之DMF (0.1M)溶液中,分次 添加六氟磷酸0-(7-氮苯并三唑-1-基)-N,N,N,,N'-四曱基錁(1.2 當量)。將所形成之反應溶液在室溫下攪拌48小時。將目前 黃色溶液以EtOAc稀釋,並以10% HC1水溶液、水及鹽水相 繼洗滌。然後,使有機萃液以Na2S04脫水乾燥,過濾,及 143482-1 -221 - 201111364 使濾液在真空中濃縮,而得黑色油。如此獲得之粗產物經 由急驟式層析之純化(Si02,CH2C12 — 90:10 (v/v) CH2C12 :在 MeOH中之2.0M NH3),獲得標題化合物,為白色固體。 步驟2 :反式-N-環丙基-N-[(4-氟基-1H-啕哚-3-基)曱基]-4-(1-曱 基-2-_基-1,2-二氫-4-1»比°定基)-3-六氩p比。定叛醯胺 於得自前一步驟之反式-3-({環丙基[(4-氟基-1H-吲哚-3-基) 曱基]胺基}羰基)-4-(1-甲基-2-酮基-1,2-二氩-4-吡啶基)-1-六氩 吡啶羧酸1,1-二曱基乙酯(1當量)之CH2C12溶液(0.05M)中,添 加溴化鋅(11)(10當量)。使所形成之懸浮液音振15分鐘,並 在室溫下授拌13小時。藉由添加EtOAc與IN NaOH水溶液使 反應淬滅’然後音振15分鐘。分離水相,且以EtOAc逆萃取。 將合併之有機萃液以水與鹽水進一步洗滌,以Na2s〇4脫水 乾燥’過滤’及使渡液在真空中濃縮。如此獲得之粗產物 經由急驟式層析之純化(Si〇2,90:10 (Wv) CH2C12 :在MeOH中 之2.0M NH3) ’獲得標題化合物’為無色油。Ms (ESI+,: 423。1 H NMR (CD3 OD) (5 (ppm) : 〇·79 (m,1H),0.87-0.99 (m,2H), 0.99-1.11 (m, 1H), 1.65-1.75 (m, 1H), 1.78 (m, 1H), 2.53 (m, 1H), 2.72-2.82 (m, 2H), 2.89-3.00 (m, 1H), 3.14-3.26 (m, 2H), 3.34 (s, 3H), 3.51-3.67 (m, 1H), 4.43 (d, J = 14.7 Hz, 1H), 4.96 (d, J = 14.7 Hz, 1H), 6.18 (m, 1H), 6.39 (s, 1H), 6.66 (m, 1H), 6.88 (s, 1H), 6.99-7.06 (m, 1H), 7.14-7.18 (m, 2H)。人類腎素IC5 〇 (緩衝劑):12.7 nM。人類腎素ic5 〇 (血漿): 8.4 nM 0 實例76 反式-N-環丙基-N-{[4-氟基小(3_吡啶基曱基)_m啕哚_3基]甲 143482-1 •222- 201111364 醯胺 基}-4_(l-甲基-2-銅基-l,2-二氫_4-吡啶基)_3_六氫吡啶叛Step 1: trans-3-({cyclopropyl[(4-fluoroindol-3-yl)indolyl]aminobucarbonyl)-4-(1-methyl-2-keto-1, 1,1-Dimethylethyl 2-dihydro-4-pyridyl)-1-hexahydropyridylcarboxylate in trans-1-{[(U-didecylethyl)oxy]carbonyl} 4-(1-mercapto-2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridinecarboxylic acid (1 equivalent, Example 1 Step 6), Hunig's base (3 equivalents) And a solution of amine 68 (1 equivalent) in DMF (0.1 M), adding hexafluorophosphate 0-(7-azabenzotriazol-1-yl)-N,N,N,,N'-four曱 锞 (1.2 equivalents). The resulting reaction solution was stirred at room temperature for 48 hours. The current yellow solution was diluted with EtOAc and washed successively with 10% aqueous HCI, water and brine. Then, the organic extract was dehydrated and dried over Na 2 SO 4 , filtered, and then filtered, and the filtrate was concentrated in vacuo to give a black oil. The crude product thus obtained was purified by flash chromatography eluting elut elut elut elut elut elut Step 2: trans-N-cyclopropyl-N-[(4-fluoro-1H-indol-3-yl)indolyl]-4-(1-indolyl-2-yl-1,2 -Dihydro-4-1» than °) -3-hexafluorop ratio. Derivatization of trans-acetin from the previous step of trans-3-({cyclopropyl[(4-fluoro-1H-indol-3-yl)indolyl]amino}carbonyl)-4-(1- In a solution of 1,2-didecylethyl ester of methyl-2-keto-1,2-di-ar- -4-pyridyl)-1-hexafluoropyridinecarboxylate (1 equivalent) in CH2C12 (0.05 M) Zinc bromide (11) (10 equivalents) was added. The resulting suspension was sonicated for 15 minutes and allowed to mix for 13 hours at room temperature. The reaction was quenched by the addition of EtOAc and aqueous 1N NaOH. The aqueous phase was separated and extracted with EtOAc. The combined organic extracts were further washed with water and brine, dried <RTI ID=0.0># </ RTI> <RTI ID=0.0> The crude product thus obtained was purified by flash chromatography (yield: EtOAc, EtOAc: EtOAc: EtOAc: Ms (ESI+,: 423.1H NMR (CD3 OD) (5 (ppm): 〇·79 (m, 1H), 0.87-0.99 (m, 2H), 0.99-1.11 (m, 1H), 1.65-1.75 (m, 1H), 1.78 (m, 1H), 2.53 (m, 1H), 2.72-2.82 (m, 2H), 2.89-3.00 (m, 1H), 3.14-3.26 (m, 2H), 3.34 (s , 3H), 3.51-3.67 (m, 1H), 4.43 (d, J = 14.7 Hz, 1H), 4.96 (d, J = 14.7 Hz, 1H), 6.18 (m, 1H), 6.39 (s, 1H) , 6.66 (m, 1H), 6.88 (s, 1H), 6.99-7.06 (m, 1H), 7.14-7.18 (m, 2H). Human renin IC5 缓冲 (buffer): 12.7 nM. Human renin ic5 〇 (plasma): 8.4 nM 0 Example 76 trans-N-cyclopropyl-N-{[4-fluoro-small (3_pyridinyl fluorenyl)_m啕哚_3yl] A 143482-1 • 222- 201111364 Amidino}-4_(l-methyl-2-copperyl-l,2-dihydro-4-pyridyl)_3_hexahydropyridine

步驟1 :反式-3-[(環丙基{[4_氟基丄⑶吡啶基曱基)_ih吲哚_3 基]曱基}胺基)羰基]-4-(1-曱基-2-酮基_U_二氫斗吡啶基H六 氫吡啶羧酸1,1-二甲基乙酯Step 1: trans-3-[(cyclopropyl{[4-fluoroylindole(3)pyridinyl)-ih吲哚_3yl]indenyl}amino)carbonyl]-4-(1-indenyl- 2-keto-___dihydropyridinyl H-hexahydropyridinecarboxylic acid 1,1-dimethylethyl ester

在0 C下,於反式-3-({環丙基[(4-氟基-1Η_吲哚_3_基)曱基]胺 基}羰基)-4-(1-甲基-2-酮基-1,2-二氫斗吡啶基)+六氫吡啶羧 酸U-二甲基乙酯(1當量,實例75步驟之DMF (〇 1Μ)溶液 中,相繼地添加KHMDS (在甲苯中之15%w/v溶液,L1當量) 與氣化3-甲基吡啶(1.3當量)。然後,使所形成之溶液慢慢地 溫熱至室溫,歷經16小時。使混合物再冷卻至,接著將 其以EtOAc稀釋,然後以飽和NaHC〇3水溶液小心地使反應淬 滅。分離水層’並以EtOAc逆萃取。將合併之有機萃液以飽 和NaHC〇3水溶液與鹽水進一步洗滌’以Na2 s〇4脫水乾燥, 過渡’及使濾液在真空中濃縮,如此獲得之粗產物經由急 驟式層析之純化(Si02 ’ CH2C12-&gt;90:10 (v/v) CH2C12 :在MeOH 中之2.0M NH3),獲得標題化合物,為白色泡沫物。 步驟2:反式-N-環丙基善{[4-氟基小(3-吡啶基曱基)_1H-吲哚-3- 基]曱基}-4-(1-甲基_2·酮基_丨,二氫斗吡啶基)冬六氫吡啶羧 醯胺 於得自前一步驟之反式_3-[(環丙基{[4-氟基-1-(3-吡啶基曱 143482-1 •223- 201111364 基)-1Η-吲哚-3-基]甲基}胺基)羰基;甲基_2_酮基_12_二氫 -4-吡啶基)-1-六氫吡啶羧酸二曱基乙酯(丨當量)之CH2cl2 溶液(0.05M)中’添加溴化辞(II)(10當量)^使所形成之懸浮 液音振15分鐘,並在室溫下攪拌13小時。藉由添加Et〇Ac 與IN NaOH水溶液使反應淬滅,然後音振15分鐘。分離水相, 且以EtOAc逆萃取。將合併之有機萃液以水與鹽水進一步洗 滌’以Naz SO*脫水乾燥’過濾’及使濾液在真空中濃縮。 如此獲得之粗產物經由急驟式層析之純化(Si〇2,9〇:1〇 (v/v) CH/l2 :在MeOH中之2·〇ΜΝΗ3),獲得標題化合物,為無色籲 油。MS (ESI+, Μ+Η) : 514。 實例77At 0 C, in trans-3-({cyclopropyl[(4-fluoroyl-1Η_吲哚_3_yl)indolyl]amino}carbonyl)-4-(1-methyl-2 -Ketyl-1,2-dihydropyridinyl)+hexahydropyridinecarboxylic acid U-dimethylethyl ester (1 equivalent, in Example 75 step DMF (〇1Μ) solution, sequentially added KHMDS (in toluene) 15% w/v solution, L1 equivalent) and gasified 3-methylpyridine (1.3 equivalents). Then, the formed solution was slowly warmed to room temperature for 16 hours. The mixture was cooled again. The reaction was then quenched with EtOAc EtOAc (EtOAc)EtOAc. Na2 s〇4 is dehydrated and dried, and the filtrate is concentrated in vacuo. The crude product thus obtained is purified by flash chromatography (Si02 'CH2C12-&gt;90:10 (v/v) CH2C12: in MeOH 2.0M NH3), the title compound was obtained as white foam. Step 2: trans-N-cyclopropyl good {[4-fluoro-small (3-pyridinyl)-H-indol-3-yl]曱基}-4-(1-methyl_2.keto-yl) Dihydropyridinyl) winter hexahydropyridine carboxamide in trans-_3-[(cyclopropyl{[4-fluoro-1-(3-pyridyl) 143482-1 •223- obtained from the previous step 201111364 base)-1Η-indol-3-yl]methyl}amino)carbonyl; methyl-2-keto- 12-dihydro-4-pyridyl)-1-hexahydropyridinecarboxylic acid dimercapto Ethyl bromide (0.05 M) was added with bromination (II) (10 equivalents). The resulting suspension was sonicated for 15 minutes and stirred at room temperature for 13 hours. The reaction was quenched by the addition of Et.sub. The aqueous phase was separated and extracted with EtOAc. The combined organic extracts were further washed with water and brine &lt;&quot;&quot;&quot;&quot; The crude product thus obtained was purified by flash chromatography (EtOAc: EtOAc (EtOAc) MS (ESI+, Μ+Η): 514. Example 77

反式-N-環丙基-N-{[4-氟基-1-(4-吡啶基曱基)_ih-啕哚-3-基]曱 基}-4-(1-曱基-2-酮基-1,2-二氫-4-ρ比唆基)-3-六氫p比咬叛醯胺 根據實例76中所述之程序製成,但在步驟1中,替代地 使用氣化4-曱基吡啶作為烷基化作用試劑。獲得標題化合 物,為白色泡沬物。MS (ESI+,M+H) : 514。人類腎素冗5〇(緩 衝劑):0,2 nM。人類腎素IC50(血渡):〇.5 nM。 實例78 反式-N-({3-乙醯基-5-[3-(曱氧基)丙基]苯基}曱基)_N環丙基 -4-(1-曱基-2-酮基-1,2-二氫-4-吡°定基)-3-六氫吡咬竣醯胺 143482-1 -224- 201111364trans-N-cyclopropyl-N-{[4-fluoro-1-(4-pyridylfluorenyl)_ih-indol-3-yl]indenyl}-4-(1-indolyl-2 -Kenyl-1,2-dihydro-4-p-pyridyl)-3-hexahydrop is prepared according to the procedure described in Example 76, but in step 1, instead of using gas 4-Mercaptopyridine is used as an alkylation reagent. The title compound was obtained as a white foam. MS (ESI+, M+H): 514. Human renin is 5 〇 (buffer): 0, 2 nM. Human renin IC50 (blood): 〇.5 nM. Example 78 trans-N-({3-Ethyl-5-[3-(indolyl)propyl]phenyl}indolyl)-N-cyclopropyl-4-(1-indolyl-2-one Base-1,2-dihydro-4-pyridyl)-3-hexahydropyridinium 143482-1 -224- 201111364

根據實例1中所述之程序製成,但替代地使用胺69作為 起始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 480。 實例79It was made according to the procedure described in Example 1, but instead using amine 69 as the starting material. The title compound was obtained as a white foam. MS (ESI+, M+H): 480. Example 79

反式-Ν·({1,3-雙[3-(甲氧基)丙基]_2,4二酮基四氫_5_嘧啶 基}曱基)-N-環丙基斗(1_甲基么酮基_u·二氫斗吡啶基)_3•六 氫吡啶羧醯胺Trans-Ν·({1,3-bis[3-(methoxy)propyl]_2,4diketotetrahydro-5-pyrimidinyl}indenyl)-N-cyclopropyl (1_ Methyl ketone _u·dihydropyridinyl)_3•hexahydropyridine carboxamide

根據實例1中所述之程序製成’但替代地使用胺作為 起始物質。獲得標題化合物,為白色泡沫物。ms邸1+, M+H). 544人類腎素1(:5〇(緩衝劑” π—。人類腎素%。(血 漿):75 nM。 實例80 反式-N-%丙基·ν_({2,3·二甲基_5 [3_(甲氧基)丙基]苯基)甲基)_ 4 (1甲基2酮基-n一氫’咳基)·3_六氫峨咬幾酿胺 143482-1 -225- 201111364 根據實例 起始物質。 M+H) : 466。It was made according to the procedure described in Example 1 but using an amine as a starting material instead. The title compound was obtained as a white foam. Ms 邸 1+, M+H). 544 human renin 1 (: 5 〇 (buffer) π - % human renin. (plasma): 75 nM. Example 80 trans-N-% propyl·ν_ ({2,3·Dimethyl_5 [3_(methoxy)propyl]phenyl)methyl)_ 4 (1 methyl 2 keto-n-hydro 'c-yl)·3_hexahydroindole Bite a few amines 143482-1 -225- 201111364 starting materials according to the examples. M+H): 466.

1中所述之程序製成’但替代地使用胺71作為 獲知私題化合物,為白色泡洙物。MS (ESI+, 實例81 反式-N-[(2-氣基_5·{[2_(甲氧基)乙基]氧基}苯基)曱基]*環丙 基斗(1-曱基-2-酮基_ι,2-二氫_4_吡啶基)3六氩吡啶羧醯胺The procedure described in 1 was made 'but instead of using amine 71 as the known compound, it was a white foam. MS (ESI+, Example 81 trans-N-[(2-carbyl_5·{[2_(methoxy)ethyl)oxy}phenyl)indolyl]*cyclopropylidene (1-indolyl) -2-keto-I,2-dihydro-4-pyridyl)3 hexafluoropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用胺72作為 起始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 474。 實例82 反式-N-環丙基-4-(1-曱基-2-酮基-1&gt;二氫冬吡啶基)-N-(2_莕基 曱基)-3-六氫吡啶羧醯胺It was made according to the procedure described in Example 1, but instead using amine 72 as the starting material. The title compound was obtained as a white foam. MS (ESI+, M+H): 474. Example 82 trans-N-cyclopropyl-4-(1-indolyl-2-keto-1&gt;dihydrotertylpyridyl)-N-(2-hydrazinyl)-3-hexahydropyridinecarboxylate Guanamine

根據實例1中所述之程序製成,但替代地使用胺73作為 143482-1 -226- 201111364 起始物質。獲得標題化合物,為白色泡沫物。Ms (ESI+, M+H) : 416。 實例83 反式-N-環丙基-4-(1-甲基·2_酮基_u二氩冰毗啶基)N_({3_[(三 氟甲基)硫基]苯基}曱基)各六氫吡啶羧醯胺It was made according to the procedure described in Example 1, but instead using amine 73 as the starting material of 143482-1 -226-201111364. The title compound was obtained as a white foam. Ms (ESI+, M+H): 416. Example 83 trans-N-cyclopropyl-4-(1-methyl-2-oxoyl_u diargonyl) N_({3_[(trifluoromethyl)thio]phenyl}anthracene Hexahydropyridine carboxamide

MeMe

根據實例1中所述之程序製成,但替代地使用胺74作為 起始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 466。 實例84 反式-N-環丙基-4-(1-甲基_2_酮基巧}二氫_4-吡啶基)_ν_{[5·[3· (曱氧基)丙基]-2-(甲硫基)苯基]甲基卜3_六氫吡咬緩醯胺It was made according to the procedure described in Example 1, but instead using amine 74 as the starting material. The title compound was obtained as a white foam. MS (ESI+, M+H): 466. Example 84 trans-N-cyclopropyl-4-(1-methyl-2-keto)-dihydro-4-pyridyl)_ν_{[5·[3·(decyloxy)propyl]- 2-(methylthio)phenyl]methyl b 3_hexahydropyridylamine

MeMe

OMe 根據實例1中所述之程序製成,但替代地使用胺%作為 起始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H): 484 〇人類腎素緩衝劑):47 nM。人類腎素1(:5〇(血 漿):12.3 nM。 實例85 反式-N-({3-演基-4-甲基-5-[3-(甲氧基)丙基]苯基}甲基)_N_環丙 143482-1 -227- 201111364 基_4-(l-甲基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺OMe was prepared according to the procedure described in Example 1, but instead using amine % as the starting material. The title compound was obtained as a white foam. MS (ESI+, M+H): 484 〇 human renin buffer): 47 nM. Human renin 1 (: 5 〇 (plasma): 12.3 nM. Example 85 trans-N-({3-exyl-4-methyl-5-[3-(methoxy)propyl)phenyl} Methyl)_N_cyclopropene 143482-1 -227- 201111364 _4-(l-methyl-2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用胺76作為 起始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 530。1H NMR (CDC13) 6 (ppm) : 0.65-0.72 (m,1H),0.76-0.82 (m, 1H), 0.89-1.00 (m, 2H), 1.66-1.90 (m, 5H), 2.33 (s, 3H), 2.41-2.47 (s, φ 1H), 2.69 (t, 2H), 2.78-2.91 (m, 2H), 2.98-3.05 (m, 1H), 3.21-3.27 (m, 2H), 3.35-3.41 (m, 5H), 3.45-3.54 (m, 4H), 4.20 (d, J = 14.5 Hz, 1H), 4.54 (d, j =14.5 Hz, 1H), 6.05-6.09 (m, 1H), 6.41 (s, 1H), 6.88 (s, 1H), 7.08 (s, 1H), 7.12(d’J = 6.9Hz,lH)。人類腎素lC5〇(緩衝劑):〇9nM。人類 腎素 IC5 〇 (血聚):1.3 nM。 反式-N-({3-漠基-4-甲基-5_[3_(曱氧基)丙基]苯基}曱基)n環丙It was made according to the procedure described in Example 1, but instead using amine 76 as the starting material. The title compound was obtained as a white foam. MS (ESI+, M+H): 530.1H NMR (CDC13) 6 (ppm): 0.65-0.72 (m, 1H), 0.76-0.82 (m, 1H), 0.89-1.00 (m, 2H), 1.66- 1.90 (m, 5H), 2.33 (s, 3H), 2.41-2.47 (s, φ 1H), 2.69 (t, 2H), 2.78-2.91 (m, 2H), 2.98-3.05 (m, 1H), 3.21 -3.27 (m, 2H), 3.35-3.41 (m, 5H), 3.45-3.54 (m, 4H), 4.20 (d, J = 14.5 Hz, 1H), 4.54 (d, j = 14.5 Hz, 1H), 6.05-6.09 (m, 1H), 6.41 (s, 1H), 6.88 (s, 1H), 7.08 (s, 1H), 7.12 (d'J = 6.9Hz, lH). Human renin lC5 〇 (buffer): 〇 9 nM. Human renin IC5 〇 (blood aggregation): 1.3 nM. trans-N-({3-Molyl-4-methyl-5_[3_(decyloxy)propyl]phenyl}indenyl) n-cyclopropyl

基-4-(1-曱以-酮基_U·二氮-4_,比B定基)冬六氮峨錢酿胺鹽 酸鹽 1 於上述化合物(1當量)之乙腈溶液(0.07M)中,逐滴添加] (4M二氧陸園溶液,1〇當量)。使混合物在室溫下靜置4〇 鐘,於此段期間内晶體係自溶液沉澱。然後,將其以第 丁基二=基趟稀釋’直到沒有產物之進—步㈣可辨識 止。接著,使所形成之懸浮液溫和地溫熱,並音振,= 使其在室溫下熟成18小時。如此獲得之標題化合物^ 過滤被單離成白色結晶性固體。 、、’&amp; 143482-1 •228· 201111364 替代程序:4-(1-indole-keto-U-diazepine-4_, specific B) hexamethylene hydrazone hydrochloride salt 1 in the above compound (1 equivalent) in acetonitrile solution (0.07 M) , added dropwise] (4M dioxane solution, 1 〇 equivalent). The mixture was allowed to stand at room temperature for 4 Torr, during which time the internal crystal system precipitated from the solution. Then, it is diluted with butyl bis = hydrazine until no product is advanced - step (4) is identifiable. Next, the resulting suspension was gently warmed and sonicated, = allowed to mature at room temperature for 18 hours. The title compound thus obtained was filtered to form a white crystalline solid. ,,&&&;143482-1 •228· 201111364 Alternative Procedures:

DMF,氣化草醯 ch2ci2DMF, gasification grasshopper ch2ci2

使(3S,4S)-1'-曱基-2,-酮基-3,4,5,6,Γ,2ΐ-六氫-2Η-[4,4·]聯吡啶基 -1,3-二羧酸1-第三-丁酯(羧酸1 ; 1.0當量)溶於二氣曱烷(1〇份 體積)中。裝填DMF (0.2當量),並使溶液冷卻至_15°C。添加 氣化草醯(0.95當量),歷經2.5小時。使N-[3-溴基-5-(3-甲氧基 丙基)-4-甲苄基]環丙胺甲烷績酸鹽(胺76 ; 〇 9〇當量)溶於二 Φ 氣曱烧(2份體積)中,然後在~-15°C下,添加i-Pr2NEt (3.3當量) ,歷經1小時。以水(1〇份體積)使反應淬滅,並將液層切割, 且以NaHC〇3溶液洗滌有機層。將液層切割,並以HC1溶液洗 滌有機層使有機層濃縮至~5.7份體積。添加2_丙醇(0.57份 體積),接著為濃HC1 (6.〇當量)。使反應混合物在351下熟 成75分鐘,然後添加水(57份體積)。將液層切割且於水 層中’添加二氯甲院(11.4份體積)。添加氫氧化鈉(67當量), 並將液層切割。將有機層以水(5.7份體積)洗條,及濃縮至 〜5份體積。添加2-丙醇(8份體積),並將殘留二氣甲院藉蒸 143482-1 201111364 餾移除。接著,添加IPA (0.11份體積)中之濃HCl (0.2當量, 37%) ’並使此批料熟成3〇分鐘。添加另外之在IPA (0.5份體 積)中之濃HC1 (0.9當量,37%),歷經1小時。添加MTBE (5.4 份體積),且使此批料熟成1小時。將所形成之漿液過濾, 並將固體以MTBE洗滌,而得(3S,4R)-N-({3-溴基斗甲基-5-[3-(曱 氧基)丙基]苯基}甲基)-N-環丙基-4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺鹽酸鹽,為白色固體。1 η NMR (500 MHz, dmso-d6) δ 9.45 (br s, 2H), 7.57 (d, J = 6.9 Hz, 1H), 6.96 (d, J = 0.9(3S,4S)-1'-mercapto-2,-keto-3,4,5,6,Γ,2ΐ-hexahydro-2Η-[4,4·]bipyridyl-1,3- The 1-carboxylic acid di-butyrate (carboxylic acid 1; 1.0 equivalent) was dissolved in dioxane (1 part by volume). DMF (0.2 eq.) was charged and the solution was cooled to _15 °C. Gasified grasshopper (0.95 equivalent) was added over 2.5 hours. N-[3-bromo-5-(3-methoxypropyl)-4-methylbenzyl]cyclopropylamine methane acid salt (amine 76; 〇9 〇 equivalent) was dissolved in two Φ gas smoldering ( In 2 parts by volume, then i-Pr2NEt (3.3 equivalents) was added at ~-15 °C for 1 hour. The reaction was quenched with water (1 part by volume), and the liquid layer was cleaved, and the organic layer was washed with NaHC? The liquid layer was cut and the organic layer was washed with a HCl solution to concentrate the organic layer to ~ 5.7 parts. Add 2-propanol (0.57 parts by volume) followed by concentrated HC1 (6. 〇 equivalent). The reaction mixture was aged at 351 for 75 minutes and then water (57 parts by volume) was added. The liquid layer was cut and the dichlorocarbyl (11.4 parts by volume) was added to the aqueous layer. Sodium hydroxide (67 equivalents) was added and the liquid layer was cut. The organic layer was washed with water (5.7 parts by volume) and concentrated to ~5 parts by volume. 2-propanol (8 parts by volume) was added, and the residual two gas chamber was removed by steaming 143482-1 201111364. Next, concentrated HCl (0.2 equivalents, 37%) in IPA (0.11 parts by volume) was added and the batch was cooked for 3 minutes. An additional concentrated HC1 (0.9 eq, 37%) in IPA (0.5 parts by volume) was added over 1 hour. MTBE (5.4 parts by volume) was added and the batch was cooked for 1 hour. The resulting slurry was filtered, and the solid was washed with MTBE to give (3S,4R)-N-({3-bromopiperidin-5-[3-(decyloxy)propyl]phenyl} Methyl)-N-cyclopropyl-4-(1-methyl-2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide hydrochloride, white solid. 1 η NMR (500 MHz, dmso-d6) δ 9.45 (br s, 2H), 7.57 (d, J = 6.9 Hz, 1H), 6.96 (d, J = 0.9

Hz, 1H), 6.79 (d, J = 0.9 Hz, 1H), 6.13 (d, J = 1.7 Hz, 1H), 6.04 (dd, J = 6.9, 1.7, 1H), 4.58 (d, J = 14.9 Hz, 1H), 4.12 (td, J = 11.5, 3,5, 1H), 4.05 (d, J = 14.9 Hz, 1H), 3.48 (dd, J = 12.2, 3.5 Hz, 1H), 3.34 (s, 1H), 3.32 (m, 1H), 3.30 (t, J = 6.2 Hz, 1H), 3.24 (s, 1H), 3.07-2.97 (om, 2H), 2.85 (m, 1H), 2.57 (m, 1H), 2.04 (qd, J = 13.0, 3.8 Hz, 1H), 1.82 (m, 1H), 1.65 (m, 1H),0_98 (m,1H),0.91-0.82 (om,2H),0.61 (m,1H)。HRMS (ES,M+H) 計算值530.2018.實測值530.2008。 X-射線粉末繞射: X-射線粉末繞射研究係被廣泛地用以特徵鑒定分子結 構、結晶度及多晶型現象。χ_射線粉末繞射圖樣係在具有 PW3040/60控制臺之Philips分析x,Pert PR0又_射線繞射系統上 產生。PW3373/00陶瓷Cu LEF X-射線管κ-α放射係作為來源 使用。圖5係說明結晶形式I,(3S,4R)_N_({3溴基_4甲基_5 [3_(甲 氧基)丙基]苯基}甲基)-N-環丙基·4-(ι·曱基酮基-1,2-二氫_4-吡啶基)-3-六氫吡啶羧醯胺鹽酸鹽之特徵性χ_射線繞射圖 樣。形式I係顯示相應於下表9中列示之d•間距之特徵性反 143482-1 230· 201111364 射· 表9 d-間距[人] 高度[cts] 10.59 945.75 7.04 1736.99 4.24 1588.22 4.22 1312.59 3.88 3855.93 3.58 1166.01 3.51 1569.66 3.31 860.32 3.08 1148.31 固態NMR :Hz, 1H), 6.79 (d, J = 0.9 Hz, 1H), 6.13 (d, J = 1.7 Hz, 1H), 6.04 (dd, J = 6.9, 1.7, 1H), 4.58 (d, J = 14.9 Hz) , 1H), 4.12 (td, J = 11.5, 3,5, 1H), 4.05 (d, J = 14.9 Hz, 1H), 3.48 (dd, J = 12.2, 3.5 Hz, 1H), 3.34 (s, 1H ), 3.32 (m, 1H), 3.30 (t, J = 6.2 Hz, 1H), 3.24 (s, 1H), 3.07-2.97 (om, 2H), 2.85 (m, 1H), 2.57 (m, 1H) , 2.04 (qd, J = 13.0, 3.8 Hz, 1H), 1.82 (m, 1H), 1.65 (m, 1H), 0_98 (m, 1H), 0.91-0.82 (om, 2H), 0.61 (m, 1H) ). HRMS (ES, M+H) calcd. 530.2018. Found 530.2008. X-ray powder diffraction: X-ray powder diffraction studies are widely used to characterize molecular structure, crystallinity, and polymorphism. The χ-ray powder diffraction pattern was generated on a Philips analysis x, Pert PR0 _ ray diffraction system with a PW3040/60 console. PW3373/00 ceramic Cu LEF X-ray tube κ-α radiation system is used as a source. Figure 5 is a diagram showing the crystalline form I, (3S, 4R)_N_({3 bromo-4 methyl_5 [3_(methoxy)propyl]phenyl}methyl)-N-cyclopropyl·4- A characteristic χ-ray diffraction pattern of (ι·decyl keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide hydrochloride. Form I shows the characteristic inverse corresponding to the d•pitch listed in Table 9 below. 143482-1 230· 201111364 Shooting · Table 9 d-spacing [person] Height [cts] 10.59 945.75 7.04 1736.99 4.24 1588.22 4.22 1312.59 3.88 3855.93 3.58 1166.01 3.51 1569.66 3.31 860.32 3.08 1148.31 Solid state NMR:

除了上述X-射線粉末繞射圖樣以外,結晶形式I係藉由其 固態碳-13核磁共振(NMR)光譜被進一步特徵鑒定。碳-13光 譜係使用Brnker 4毫米HX CPMAS探針記錄。碳-13光譜係利 用質子/碳-13可變振幅正交偏振(VACP),以5毫秒之接觸時 間與10秒之脈衝延遲收集,同時在10 kHz下使試樣進行魔 角旋轉(MAS)。於Fourier變換之前,將10 Hz之線條變寬應用 至碳-13光譜。化學位移係以TMS尺度作報告,使用甘胺酸 之羰基碳(176.03 ppm)作為次要參考物。圖2係說明關於結晶 形式I之固態碳-13 CPMAS NMR光譜。形式I係顯示相應於下 表10中列示之化學位移之特徵性吸收峰: 143482-1 -231 - 201111364 表ίο 吸收峰 相對 (ppm) 強度 120.1 100 31.2 76 17.1 73 43.5 71 41.6 71 .29.4 68 58.5 67 71.4 66 28.7 64 42.5 64 138.3 60 143.6 58In addition to the above X-ray powder diffraction pattern, crystalline Form I was further characterized by its solid carbon-13 nuclear magnetic resonance (NMR) spectroscopy. The carbon-13 spectrum was recorded using a Brnker 4 mm HX CPMAS probe. The carbon-13 spectroscopy uses proton/carbon-13 variable amplitude orthogonal polarization (VACP) to collect with a 5 millisecond contact time and a 10 second pulse delay, while the sample is subjected to magic angle rotation (MAS) at 10 kHz. . Apply a 10 Hz line widening to the carbon-13 spectrum before the Fourier transform. Chemical shifts were reported on the TMS scale using carbonyl carbon (176.03 ppm) of glycine as a secondary reference. Figure 2 illustrates the solid carbon-13 CPMAS NMR spectrum for crystalline Form I. Form I shows the characteristic absorption peaks corresponding to the chemical shifts listed in Table 10 below: 143482-1 -231 - 201111364 Table ί Absorption peak relative (ppm) Intensity 120.1 100 31.2 76 17.1 73 43.5 71 41.6 71 .29.4 68 58.5 67 71.4 66 28.7 64 42.5 64 138.3 60 143.6 58

示差掃描卡計法: DSC數據係使用TA儀器DSC 2910或相當物獲取。將2與6 毫克間之试樣稱重置於淺盤中’並加蓋。然後,將此淺盤 搂曲,並放置在卡計元件中之試樣位置上。將空淺盤放置 在參考位置上。將卡計元件關閉,並使氮之流動通過此元籲 件。設定加熱程序’以將試樣在1〇〇c /分鐘之加熱速率下加 熱至大約250 C之溫度。開始加熱程序。當操作完成時,數 據係使用被包含在系統軟體中之DSC分析程式分析。熱事 件係在高於與低於涵蓋發現熱事件之溫度範圍之基線溫度 點之間進行積分。所報告之數據為展開溫度、尖峰溫度及 給°圖4係說明關於結晶形式I之示差掃描卡計法曲線。 熱重分析·· 143482-1 •232 · 201111364 TG數據係使用Perkin Elmer TGA7型獲取。實驗係在氮之流 動下,及使用ιοί /分鐘之加熱速率,進行至大約250〇c之最 高溫度。於自動地量測天平重量後,將5至2〇毫克試樣添加 至鉑淺盤中,將爐子升高,並開始加熱程序。重量/溫度數 據係自動地藉由儀器收集。其結果之分析係藉由選擇儀器 軟體内之ΔΥ功能,及選擇欲於其間計算重量損失之溫度而 進行。重量損失係經報告直到分解/蒸發之展開。圖3係說 明關於結晶形式I之熱重分析曲線。 純度 在需要時,純度可經由在異丙醇中配成漿液而被升級。 物質 MW 當量 莫耳 量 HC1 鹽 566.96 1.0 16.74 9.491 公斤 178公斤 IPA (d = 0.786)Differential Scanning Card Method: The DSC data is obtained using the TA Instruments DSC 2910 or equivalent. Retain the sample between 2 and 6 mg in a shallow pan' and cap it. The tray is then distorted and placed in the position of the sample in the card component. Place the empty tray in the reference position. The card meter element is turned off and the flow of nitrogen is passed through this element. The heating procedure was set to heat the sample to a temperature of about 250 C at a heating rate of 1 〇〇c / minute. Start the heating process. When the operation is complete, the data is analyzed using the DSC analysis program included in the system software. The thermal event is integrated between a baseline temperature point above and below the temperature range that covers the discovery of the thermal event. The reported data are the unfolding temperature, the peak temperature, and the differential scanning calorimetry curve for crystalline Form I. Thermogravimetric Analysis·· 143482-1 •232 · 201111364 TG data was acquired using Perkin Elmer TGA7. The experiment was carried out under nitrogen flow and at a heating rate of ιοί /min to a maximum temperature of about 250 °C. After automatically measuring the balance weight, 5 to 2 mg of the sample was added to the platinum tray, the furnace was raised, and the heating procedure was started. The weight/temperature data is automatically collected by the instrument. The analysis of the results is performed by selecting the ΔΥ function in the instrument soft body and selecting the temperature at which the weight loss is to be calculated. The weight loss is reported until the decomposition/evaporation begins. Figure 3 is a graph showing the thermogravimetric analysis curve for crystalline Form I. Purity Purity can be upgraded via slurrying in isopropanol when needed. Substance MW Equivalent Molar HC1 Salt 566.96 1.0 16.74 9.491 kg 178 kg IPA (d = 0.786)

將HC1鹽(9491公斤)在異丙醇(149公斤,190升)中配成漿液。 使漿液溫熱至68°C ’歷經2小時,然後冷卻至20°C,歷經1 小時’接著過濾’以異丙醇(38升,29公斤)洗滌。使固體 在真空下’於4(TC下以N2掃射乾燥,以86%產率獲得產物 (8.203 公斤)。 實例86 反式-N-[3,5-雙(3-曱氧基丙基)竿基]_N_環丙基-4-(1-曱基·2-酮基 -1,2-二氫-4-Ρ比咬基)-3-六氫Ρ比η定叛醯胺 143482-1 -233 - 201111364The HCl salt (9491 kg) was slurried in isopropanol (149 kg, 190 liters). The slurry was allowed to warm to 68 ° C for 2 hours, then cooled to 20 ° C and washed with isopropanol (38 L, 29 kg) over 1 hour &apos; The solid was dried under vacuum at <RTI ID=0.0>(4 </RTI> <RTI ID=0.0></RTI> </RTI> <RTI ID=0.0></RTI> </RTI> <RTIgt; Sulfhydryl]_N_cyclopropyl-4-(1-indolyl-2-keto-1,2-dihydro-4-indole ratio)-3-hexahydroindole ratio η 醯 醯 143 143482- 1 -233 - 201111364

根據實例1中所述之程序製成,但替代地使用胺77作為 起始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 510 〇 實例87 反式-N-環丙基·Ν_[3_(3_曱氧基丙基)_5_曱芊基]_4_(1_曱基_2酮 基-1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺It was made according to the procedure described in Example 1, but instead using amine 77 as the starting material. The title compound was obtained as a white foam. MS (ESI+, M+H): 510 〇 Example 87 trans-N-cyclopropyl·Ν_[3_(3_methoxypropyl)_5_indenyl]_4_(1_mercapto-2-one -1,2-dihydro-4-pyridyl)_3_hexahydropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用胺78作為 起始物質。獲得標題化合物,為白色泡沐物。Ms (ESI+, M+H) : 452。 實例88 反式-N-[2-溴基-3,5-雙(3-曱氧基丙基)罕基]-N-環丙基-4-(1-甲基 -2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺It was made according to the procedure described in Example 1, but instead using amine 78 as the starting material. The title compound was obtained as a white foam. Ms (ESI+, M+H): 452. Example 88 trans-N-[2-Bromo-3,5-bis(3-decyloxypropyl)hanyl]-N-cyclopropyl-4-(1-methyl-2-keto- 1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用胺79作為 143482-1 •234· 201111364 起始物質。獲得標題化合物,為白色泡;:末物。M:S (ESI+, M+H) : 589。 實例89 反式-N-[2-氣基-3,5-雙(3-曱氧基丙基)辛基]-N_環丙基冰(1_曱基 -2-鋼基-1,2-二氫-4-p比咬基)-3-六氫p比咬叛醒胺Prepared according to the procedure described in Example 1, but instead using amine 79 as the starting material for 143482-1 • 234 201111364. The title compound was obtained as a white foam; M: S (ESI+, M+H): 589. Example 89 trans-N-[2-carbyl-3,5-bis(3-decyloxypropyl)octyl]-N-cyclopropyl ice (1_mercapto-2-steel-yl-1, 2-dihydro-4-p ratio octyl)-3-hexahydrop ratio

MeMe

根據實例1中所述之程序製成,但替代地使用胺8〇作為 起始物質。獲得標題化合物’為白色泡沫物。MS (ESI+, M+H) : 544。4 NMR(CDC13) (5 (ppm) : 0.62-0.68 (m,1H),0.74-0.79 (m, 1H), 0.82-0.90 (m, 2H), 1.63-1.93 (m, 8H), 2.46-2.55 (m, 2H), 2.55-2.61 (br m, 1H), 2.72-2.89 (m, 4H), 3.05 (dt, J = l〇.l, 5.5 Hz, 1H), 3.22 (br m, 1H), 3.32-3.37 (m, 9H), 3.38 (t, d = 7.2 Hz, 1H), 3.50-3.58 (m, 4H), 4.23 (d, J = 13.5 Hz, 1H), 4.70 (d, J = 13.5 Hz, 1H), 6.12 (d, J = 7.0 Hz, 1H),6.47 (s, 1H), 6.52 (s, 1H), 6.92 (s, 1H), 7.18 (d,J = 7.0 Hz,1H)。 人類腎素IC50(緩衝劑):0.2 nM。人類腎素IC50(血漿):0.5 nM ° 實例90 反式-N-環丙基-N-[2-甲氧基-3,5-雙(3-甲氧基丙基)节基]-4-(1-甲 基-2-_基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺 143482-1 -235· 201111364It was made according to the procedure described in Example 1, but instead using amine 8 as the starting material. The title compound was obtained as a white foam. MS (ESI+, M+H): 544. 4 NMR (CDC13) (5 (ppm): 0.62-0.68 (m, 1H), 0.74-0.79 (m, 1H), 0.82-0.90 (m, 2H), 1.63 -1.93 (m, 8H), 2.46-2.55 (m, 2H), 2.55-2.61 (br m, 1H), 2.72-2.89 (m, 4H), 3.05 (dt, J = l〇.l, 5.5 Hz, 1H), 3.22 (br m, 1H), 3.32-3.37 (m, 9H), 3.38 (t, d = 7.2 Hz, 1H), 3.50-3.58 (m, 4H), 4.23 (d, J = 13.5 Hz, 1H), 4.70 (d, J = 13.5 Hz, 1H), 6.12 (d, J = 7.0 Hz, 1H), 6.47 (s, 1H), 6.52 (s, 1H), 6.92 (s, 1H), 7.18 ( d, J = 7.0 Hz, 1H) Human renin IC50 (buffer): 0.2 nM. Human renin IC50 (plasma): 0.5 nM ° Example 90 trans-N-cyclopropyl-N-[2- Oxy-3,5-bis(3-methoxypropyl)benzyl]-4-(1-methyl-2-yl-1,2-dihydro-4-pyridyl)-3-hexa Hydrogen pyridine carboxamide 143482-1 -235· 201111364

根據實例1中所述之程序製成,但替代地使用胺81作為 起始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 540。 實例91 反式-N-環丙基_N-[3-(3-曱氧基丙基)_5_(三氟曱基)芊基]_4_(1_曱 基-2-嗣基-i,2-二氫-4-峨D定基)_3_六氫p比咬缓醯胺It was made according to the procedure described in Example 1, but instead using amine 81 as the starting material. The title compound was obtained as a white foam. MS (ESI+, M+H): 540. Example 91 trans-N-cyclopropyl_N-[3-(3-methoxypropyl)_5_(trifluoromethyl)indenyl]_4_(1_mercapto-2-indenyl-i, 2 -dihydro-4-indole D-based)_3_hexahydro-p ratio

根據實例1中所述之程序製成,但替代地使用胺82作為 起始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 506。 實例92 反式環丙基_N_[3_羥基_5_(3_曱氧基丙基)字基曱基_2· 酉同基-1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺It was made according to the procedure described in Example 1, but instead using amine 82 as the starting material. The title compound was obtained as a white foam. MS (ESI+, M+H): 506. Example 92 transcyclopropyl_N_[3_hydroxy_5_(3_methoxypropyl)-based fluorenyl 2·indolyl-1,2-dihydro-4-pyridyl)_3_6 Hydropyridine carboxamide

MeMe

根據實例1中所述之程序製成,但替代地使用胺83作 為 143482-1 •236· 201111364 起始物質。獲得標題化合物,為白色料物。ms㈣+, Μ+ίί) : 454。 實例93 反式仰_苯甲酿基士漠基羊基)-Ν·環丙基邻-曱基·2-酮基 -1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺It was prepared according to the procedure described in Example 1, but instead using amine 83 as the starting material of 143482-1 • 236·201111364. The title compound was obtained as a white material. Ms (four) +, Μ + ίί) : 454. Example 93 trans-p-benzoyl-based ketone-based ketone)-oxime-cyclopropyl-indolyl-2-keto-1,2-dihydro-4-pyridyl)_3_hexahydropyridinecarboxylate Guanamine

步驟1 :反式-3-UC3-填基_5·破基宇基)(環丙基)胺基]幾基}_4_屮 甲基-2-酮基-1,2-二氫吡啶_4_基)小六氫吡啶羧酸第三-丁酯 於反式-1-{[(1,1-二曱基乙基)氧基]羰基丨斗(1曱基·2酮基 -1,2_二氫-4-吡啶基)·3-六氫吡啶羧酸(1當量,實例i步驟6)、 Hrniig氏鹼(3當量)及胺84(1當量kDMF(〇1M)溶液中,分次 添加六氟磷酸0-(7-氮笨并三唑小基)…凡乂仏四曱基錄叫 • 當量)。將所形成之反應溶液在室溫下攪拌48小時。將目前 黃色溶液以EtOAc稀釋,並以10%HC1水溶液、1NNa〇H水溶 液及鹽水相繼洗條。然後,使有機萃液以Na2 S〇4脫水乾燥, 過;慮,及使;慮液在真空中濃縮,而得帶紅橘色油。如此獲 得之粗產物經由急驟式層析之純化(Si〇2,97:3 (ν/ν) (:ϋ2α2 : 在MeOH中之2.0Μ ΝΗ3),獲得標題化合物,為黃色油。 步驟2 :反式-3-{[(3-苯曱醯基-5-溴基苄基)(環丙基)胺基]羰 基)-4-(1-曱基-2-酮基-1,2-二氫吡啶_4-基)六氫吡啶小羧酸第三 -丁酯 143482-1 -237- 201111364 在-78°C下,於1,5-雙(演基鎂)戊烷(1〇當量)在THF (〇 〇5M) 中之溶液内’添加製自CuCN (1.〇當量)與Lid (2.0當量)之 CuCN-2LiCl在THF (0.9M,相對於CuCN)中之溶液。將所形成 之混合物於-78 C下撥拌30分鐘。然後,添加得自前一步驟 之反式-3-{[(3-漠基-5-碘基苄基)(環丙基)胺基獵基卜4_(1_曱基 -2-酮基-1,2-二氫p比啶-4-基)_ι_六氫吡啶羧酸第三-丁酯(1〇當 I )在THF (0.2M)中之溶液’並使反應混合物溫熱至室溫, 歷經1小時。最後,添加氣化苯曱醯(1 5當量),且將反應混 合物再攪拌1小時。藉由添加水使反應混合物淬滅,接著以0 EtOAc萃取。使合併之有機萃液以Na2S〇4脫水乾燥,過濾, 及使濾液在真空中濃縮。如此獲得之粗產物經由急驟式層 析之純化(Si02,2:98 (v/v)-&gt;15:85 (v/v) MeOH: CH2C12),獲得 標題化合物,為褐色油。 步驟3:反式-N-(3-苯甲醯基_5_溴基芊基)_N_環丙基_4 (1_曱基_2_ _基-1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺 於得自前一步驟之反式_3_{[(3_苯甲醯基_5_溴基苄基)(環丙 基)胺基]獄基}-4-(1-甲基_2-酮基-1,2-二氫吡啶斗基)六氫吡啶 -1-羧酸第三-丁酯(1當量)之CH2C12溶液(0.1M)中,添加HC1 (4.0M二氧陸圜溶液,30當量)。將所形成之溶液在室溫下 攪拌45分鐘。於真空令移除揮發性物質之後,將所形成之Step 1: trans-3-UC3-substrate_5·breaking base)(cyclopropyl)amino]]yl}_4_屮methyl-2-keto-1,2-dihydropyridine_ 4_yl) small hexahydropyridinecarboxylic acid tert-butyl ester in trans-1-{[(1,1-didecylethyl)oxy]carbonyl oxime (1 fluorenyl-2-keto-1 , 2_dihydro-4-pyridyl)·3-hexahydropyridinecarboxylic acid (1 equivalent, Example i, Step 6), Hrniig's base (3 equivalents), and amine 84 (1 equivalent of kDMF (〇1M) solution, Add hexafluorophosphate 0-(7-aza-benzotriazole small base) in fractions. The resulting reaction solution was stirred at room temperature for 48 hours. The current yellow solution was diluted with EtOAc and washed sequentially with a 10% aqueous HCl solution, 1 N NaH aqueous solution and brine. Then, the organic extract was dehydrated and dried with Na2S〇4, and the solution was concentrated in vacuo to give a red-brown oil. The crude product thus obtained was purified by flash chromatography (EtOAc: EtOAc: EtOAc: EtOAc: EtOAc: 3-{[(3-Benzenyl-5-bromobenzyl)(cyclopropyl)amino]carbonyl)-4-(1-indol-2-yl-1,2-di Hydropyridine-4-yl)hexahydropyridine small carboxylic acid tert-butyl ester 143482-1 -237- 201111364 at -78 ° C in 1,5-bis (magnesium) pentane (1 〇 equivalent) A solution of CuCN-2LiCl in THF (0.9 M, relative to CuCN) was added from a solution of CuCN (1. 〇 equivalent) and Lid (2.0 eq.) in THF (〇〇5M). The resulting mixture was stirred at -78 C for 30 minutes. Then, the trans-3-{[(3-carbyl-5-iodobenzyl)(cyclopropyl)amine-based sylvestris 4_(1_mercapto-2-one-) derived from the previous step was added. a solution of 1,2-dihydrop-pyridin-4-yl)-i-piperidinecarboxylic acid, a third-butyl ester (1 〇1) in THF (0.2 M) and warming the reaction mixture to room Warm, after 1 hour. Finally, gasified phenylhydrazine (15 equivalents) was added, and the reaction mixture was further stirred for 1 hour. The reaction mixture was quenched by the addition of water then EtOAc. The combined organic extracts were dried over Na2SO4, filtered and filtered and evaporated. The crude product thus obtained was purified by flash chromatography (EtOAc, EtOAc (EtOAc) Step 3: trans-N-(3-Benzylfluorenyl-5-bromoindenyl)_N_cyclopropyl_4 (1_fluorenyl-2-yl-1,2-dihydro-4-pyridine Base)_3_hexahydropyridine carboxamide in trans _3_{[(3_benzylidene-5_bromobenzyl)(cyclopropyl)amino]peptidyl}-4 from the previous step Addition of HC1 to a solution of 1-(1-methyl-2-keto-1,2-dihydropyridinyl)hexahydropyridine-1-carboxylic acid tert-butyl ester (1 equivalent) in CH2C12 (0.1 M) (4.0 M dioxane solution, 30 equivalents). The resulting solution was stirred at room temperature for 45 minutes. After the vacuum is removed to remove volatile substances, it will be formed

殘留物直接地裝填至以93:7 (v/v) CH2C12 :在MeOH中之2.0M NH3填充之Si〇2管柱上。以相同溶劑系統之溶離,獲得標題 化合物。MS (ESI+,M+H) : 548。 實例94 143482-1 •238 · 201111364 反式-N-{3-漠基-5-[(1Ε)-3-曱氧基-1-丙烯_ι_基]节基卜N-環丙基 -4-(1-曱基-2-酮基-U-二氫-4-吡啶基)-3-六氫吡啶羧醯胺The residue was directly loaded onto a 2.0:7 (v/v) CH2C12: 2.0M NH3 filled Si2 column in MeOH. The title compound was obtained by dissolving in the same solvent system. MS (ESI+, M+H): 548. Example 94 143482-1 •238 · 201111364 trans-N-{3-Momot-5-[(1Ε)-3-曱oxy-1-propene_ι_yl]] benzyl N-cyclopropyl- 4-(1-mercapto-2-keto-U-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide

步驟1:反式-3-{[{3-溴基-5-[(1Ε)-3-曱氧基丙-1-烯-1-基]爷基}博 鲁 丙基)胺基]幾基M-(l-曱基-2-酮基-l,2-二氫p比唆-4-基)六氫p比 啶-1-羧酸第三-丁酯 將反式-3-{[(3-漠基-5-碘基芊基)(環丙基)胺基機基}·4_(1甲 基-2-酮基-I,2-二氫ρ比咬-4-基)小六氫ρ比咬缓酸第三_丁酯〇 〇 當量’實例93步驟1)、2-[(1Ε)-3-甲氧基丙-1-烯-1·基;1_4,4,5,5•四 甲基-1,3,2- 一氧硼伍圜(1.2當量)、碳酸鈉(4.5當量)及 Pd(dppf)C12 (〇,1當量)在二氧陸園(〇 1Μ)中之混合物重複抽 氣,並以氮逆充填。將混合物於室溫下,在黑暗中攪拌2 # 小時。將目前黑色懸浮液以鹽水稀釋,且以EtOAc萃取。使 合併之有機萃液以Na] SO#脫水乾燥,過濾,及使濾液在真 空中濃縮。如此獲得之粗產物經由急驟式層析之純化 (Si02 ’ EtOAc-^ 4:96 (v/v )在 MeOH 中之 2M NH3 : EtOAc),獲得 標題化合物,為淡橘色油。 步驟2 :反式-Ν·{3_溴基_5·[(1Ε)各曱氧基小丙烯小基]爷基} N_ 環丙基-4-(1-甲基_2_酮基·u_二氫斗吡啶基)3_六氫吡啶羧醯胺 於得自前—步驟之反式-3-{[{3-溴基-5-[(1Ε)-3-甲氧基丙-1-稀_1·基]午基)(環丙基)胺基]羧基)-4-(1-曱基-2·酮基-1,2-二氫吡 143482-1 201111364 啶-4-基)六氫吡啶小羧酸第三_丁醋(1當量)之CH2cl2溶液 (0.1M)中,添加HC1 (4.0M二氧陸圜溶液,30當量)。將所形 成之溶液在室溫下攪拌45分鐘。於真空中移除揮發性物質 之後,將所形成之殘留物直接地裝填至以93:7 (v/v) CH2Cl2 : 在MeOH中之2.0M NH3填充之Si〇2管柱上。以相同溶劑系統 之溶離’獲得標題化合物。MS (ESI+,M+H) : 516。 實例95 反式-N-{3-&gt;臭’基-5-[(2-經乙基)硫基]节基}_N-環丙基甲基 -2-銅基-1,2-二氩-4-p比咬基)-3-六氫p比。定叛醯胺Step 1: trans-3-{[{3-bromo-5-[(1Ε)-3-decyloxyprop-1-en-1-yl]-aryl}boruryl)amino] M-(l-fluorenyl-2-keto-l,2-dihydrop-indol-4-yl)hexahydrop-pyridyl-1-carboxylic acid tert-butyl ester will be trans-3-{ [(3-Mosyl-5-iodohydrazino)(cyclopropyl)amino group}·4_(1methyl-2-keto-I,2-dihydroρ than -4-yl) Small hexahydro ρ ratio to biting acid third _butyl ester oxime equivalent 'Example 93 Step 1), 2-[(1Ε)-3-methoxyprop-1-ene-1·yl; 1_4, 4, 5 ,5•Tetramethyl-1,3,2-monooxaboron (1.2 equivalents), sodium carbonate (4.5 equivalents) and Pd(dppf)C12 (〇, 1 equivalent) in dioxere (〇1Μ) The mixture in the mixture was repeatedly evacuated and counter-filled with nitrogen. The mixture was stirred at room temperature for 2 hours in the dark. The current black suspension was diluted with brine and extracted with EtOAc. The combined organic extracts were dried over Na~SO~, filtered, and concentrated in vacuo. The crude product thus obtained was purified by flash chromatography eluting elut elut elut elut elut elut elut Step 2: trans-Ν·{3_bromo group_5·[(1Ε) each methoxy propylene small base] 基 }} N_cyclopropyl-4-(1-methyl-2-keto- U_Dihydropyridinyl)3_hexahydropyridine carboxamide in trans-{{3-bromo-5-[(1Ε)-3-methoxyprop-1) from the previous step -diluted-yl group) (cyclopropyl)amino]carboxy)-4-(1-indolyl-2.keto-1,2-dihydropyridyl 143482-1 201111364 pyridine-4-yl To a solution of the hexahydropyridine small carboxylic acid in the third butyl vinegar (1 eq.) in CH 2 Cl 2 (0.1 M), HCl (4.0 M dioxane solution, 30 eq.) was added. The resulting solution was stirred at room temperature for 45 minutes. After removal of the volatiles in vacuo, the resulting residue was loaded directly onto a &lt;RTI ID=0.0&gt;&gt;&gt;&gt; The title compound was obtained by dissolving from the same solvent system. MS (ESI+, M+H): 516. Example 95 trans-N-{3-&gt;Smelly'yl-5-[(2-ethyl)thio]]}N-cyclopropylmethyl-2-copperyl-1,2-di Argon-4-p ratio to hexahydropyrene. Detamine

步驟1 :反式-3-{[{3-溴基-5-[(2-經乙基)硫基]辛基}(環丙基)胺 基]幾基}-4-(1-甲基-2-酮基-1,2-二氫ρ比咬-4-基)六氫!τ比咬_ι_緩 酸第三-丁酯 於反式-3-{ [(3-漠基-5-碟基爷基)(環丙基)-胺基]|炭基卜4-(1-甲 基-2-酮基-1,2-二氫p比1•定-4-基)-1-六氫p比β定叛酸第三-丁醋(1.〇 當量,實例93步驟1)在DMF (0_3Μ)中之溶液内,添加青銅(L1 當量)與2,二硫基二乙醇(0.6當量)。將反應混合物加熱至 110°C,歷經24小時,冷卻,並以EtOAc稀釋。將所形成之懸 浮液於室溫下授拌20分鐘,經過石夕藻土過渡,且將不溶物 以EtOAc進一步沖洗。將如此獲得之濾液以濃NH4 OH :飽和 NH4C1水溶液之3:1 (v/v)混合物、水及鹽水相繼洗滌,以 201111364Step 1: trans-3-{[{3-bromo-5-[(2-ethyl)thio]octyl}(cyclopropyl)amino]]yl}-4-(1-A Keto-2-keto-1,2-dihydroρ than biti-4-yl) hexahydro! τ than biting_ι_slow acid third-butyl ester in trans-3-{ [(3-Mosyl-5-discyl) (cyclopropyl)-amino]|Carbyl 4-( 1-methyl-2-keto-1,2-dihydrop ratio 1 • 1,4-yl)-1-hexahydrop ratio β-determination of taurine third-butyl vinegar (1. 〇 equivalent, example 93 Step 1) Bronze (L1 equivalent) and 2, dithiodiethanol (0.6 equivalents) were added to the solution in DMF (0_3 Torr). The reaction mixture was heated to 110 &lt;0&gt;C over 24 h, cooled and diluted with EtOAc. The resulting suspension was stirred at room temperature for 20 minutes, transitioned through Shixia, and the insoluble material was further rinsed with EtOAc. The filtrate thus obtained was washed successively with a 3:1 (v/v) mixture of concentrated NH4OH: saturated NH4C1 aqueous solution, water and brine to 201111364

MgS〇4脫水乾燥,過濾,及使濾液在真空中濃縮。如此獲得 之粗產物經由急驟式層析之純化(Si〇2,EtOAc— 4:96 (ν/ν)在 MeOH中之2M NH3 : EtOAc),獲得標題化合物,為無色油。 步驟2:反式-N-{3-溴基-5-[(2-經乙基)硫基]字基}_Ν•環丙基斗(1_ 甲基-2-¾基-1,2-二氫-4-Ρ比咬基)-3-六氫ρ比β定叛醯胺 於得自前一步驟之反式-3-{[{3-溴基-5-[(2-經乙基)硫基]爷 基}(環丙基)胺基]幾基}-4-(1-甲基-2-酮基-1,2-二氫ρ比咬_4·基)六 氫吡啶-1-羧酸第三-丁酯(1當量)之CH2C12溶液(Ο.ιμ)中,添 加HC1 (4.0M二氧陸園溶液,30當量)。將所形成之溶液在室 溫下攪拌45分鐘。於真空中移除揮發性物質之後,將所形 成之殘留物直接地裝填至以90:10 (v/v) CH2C12 :在MeOH中之 2.0M NH3填充之Si〇2管柱上。以相同溶劑系統之溶離,獲得 標題化合物。MS (ESI+,M+H) : 520。 實例96 反式-N-環丙基-N-[3-[2-(環丙基氧基)乙氧基]_5-(3_曱氧基丙基) φ 芊基]-4_(1_曱基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺The MgS 4 was dehydrated, filtered, and the filtrate was concentrated in vacuo. The crude product thus obtained was purified by flash chromatography eluting elut elut elut elut elut elut elut Step 2: trans-N-{3-bromo-5-[(2-ethyl)sulfanyl]}}Ν·cyclopropyl (1_methyl-2-3⁄4yl-1,2- Dihydro-4-indole ratio -3- hexahydro ρ ratio β 醯 醯 醯 于 于 于 于 于 于 于 于 于 于 于 于 于 -3- -3- -3- -3- -3- -3- -3- { { { { { { { { { { Thio]-yl}(cyclopropyl)amino]]yl}-4-(1-methyl-2-keto-1,2-dihydro-p-biti-4-yl)hexahydropyridine- To a solution of 1-carboxylic acid tert-butyl ester (1 equivalent) in CH2C12 (Ο.ιμ), HCl (4.0 M dioxane solution, 30 equivalents) was added. The resulting solution was stirred at room temperature for 45 minutes. After removal of the volatiles in vacuo, the resulting residue was loaded directly onto a &lt;RTI ID=0.0&gt;&gt;&gt;&gt; The title compound was obtained by dissolving in the same solvent system. MS (ESI+, M+H): 520. Example 96 trans-N-cyclopropyl-N-[3-[2-(cyclopropyloxy)ethoxy]_5-(3-methoxypropyl) φ fluorenyl]-4_(1_ Mercapto-2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide

步驟1:反式-3-({環丙基[3_[2-(環丙基氧基)乙氧基;]_5_(3_曱氧基 丙基)罕基]胺基}羰基)-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)-1-六氫p比唆叛酸第三-丁酉旨 於反式-3-({環丙基[3_羥基_5_(3_曱氧基丙基)苄基]胺基}羰 143482-1 •241- 201111364 基)-4-(1-曱基-2-酮基-i,2-二氫_4_吡啶基)-1_六氫吡啶鲮酸第三_ 丁酯(1.0當量,實例92)在DMF (0.1M)中之溶液内,添加碳酸 铯(2當量)、碘化鈉(005當量)及(2_氯乙氧基)環丙烷當量) 。將反應混合物在lOOt下加熱22小時。於冷卻至室溫後, 以飽和氯化銨水溶液使反應淬滅,並以Et〇 Ac萃取。將合併 之有機萃液以水與鹽水進一步洗滌,以MgS〇4脫水乾燥,過 濾,及使濾液在真空中濃縮。如此獲得之粗產物經由急驟 式層析之純化(Si〇2,95:5 (v/v) (¾¾ : MeOH),獲得標題化 合物,為無色油。 步驟2 :反式-N-環丙基-N-[3-[2-(環丙基氧基)乙氧基]_5_(3_甲氧 基丙基)爷基]-4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶 羧醯胺 於得自前一步驟之反式-3-({環丙基[3-[2-(環丙基氧基)乙氧 基]-5-(3-甲氧基丙基)苄基]胺基丨羰基)_4_(ι_曱基_2_酮基12二 氫-4-吡啶基)-1-六氫吡啶羧酸第三_ 丁酯(1當量)之CH2Cl2溶 液(0.1M)中’添加HC1 (4.0M二氧陸圜溶液,30當量)。將所 形成之溶液在室溫下授拌4小時。於真空中移除揮發性物質 之後’將所形成之殘留物直接地裝填至以93:7 (v/v) CH2 Cl2 : 在MeOH中之2·0Μ NH3填充之Si02管柱上。以相同溶劑系統 之溶離’獲得標題化合物。MS (ESI+, M+H) : 538。 實例97 反式-N-環丙基-N-{3-(3-曱氧基丙基)-5-[2-(4-嗎福啉基)乙氧基] 芊基甲基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺 143482-1 -242- 201111364 根據實例96 使用4-(2-氣乙 M+H) : 567 〇Step 1: trans-3-({cyclopropyl[3_[2-(cyclopropyloxy)ethoxy];_5_(3-methoxypropyl)hanyl]amino}carbonyl)-4 -(1-mercapto-2-keto-1,2-dihydro-4-pyridyl)-1-hexahydrop is more specific than -3- ({cyclopropyl) [3_hydroxy_5_(3_methoxypropyl)benzyl]amino}carbonyl 143482-1 •241- 201111364 base)-4-(1-mercapto-2-keto-i,2-di Hydrogen_4_pyridyl)-1_hexahydropyridinic acid tert-butyl ester (1.0 eq., Example 92) In a solution of DMF (0.1 M), cesium carbonate (2 eq.), sodium iodide ( 005 equivalents) and (2_chloroethoxy)cyclopropane equivalent). The reaction mixture was heated at 100 Torr for 22 hours. After cooling to room temperature, the reaction was quenched with saturated aqueous ammonium chloride and extracted with EtOAc. The combined organic extracts were further washed with water and brine, dried over MgSO 4 , filtered, and evaporated. The crude product thus obtained was purified by flash chromatography (EtOAc: EtOAc: EtOAc (EtOAc) -N-[3-[2-(cyclopropyloxy)ethoxy]_5_(3-methoxypropyl)-yl]-4-(1-methyl-2-keto-1,2 -dihydro-4-pyridyl)-3-hexahydropyridine carboxamide in trans-3-({cyclopropyl[3-[2-(cyclopropyloxy))ethoxy) from the previous step ]-5-(3-methoxypropyl)benzyl]aminoindole carbonyl)_4_(ι_indolyl-2-keto 12-dihydro-4-pyridyl)-1-hexahydropyridinecarboxylic acid Add HCl (4.0 M dioxane solution, 30 equivalents) in a solution of tri-butyl ester (1 equivalent) in CH 2 Cl 2 (0.1 M). The resulting solution was mixed for 4 hours at room temperature. After the volatiles were added, the resulting residue was directly loaded onto a SiO2 column packed with 93:7 (v/v) CH2Cl2: MeOH in MeOH. Dissolution from the same solvent system. The title compound was obtained. MS (ESI+, M+H): 538. </RTI> Example 97 trans-N-cyclopropyl-N-{3-(3-methoxypropyl)-5-[2-(4-? Phenyloxy) decylmethyl-2- Yl-1,2-dihydro-4-pyridinyl) -3-piperidine-2carboxamide 143482-1-242- 201 111 364 according to Example 96 using 4- (2-ethyl gas M + H): 567 billion

MeMe

Ο 基)嗎福琳作為烷基化作用試劑。MS (ESI+, 實例98 4_嗎福啉羧酸反式各[(環丙基{[4-(1-甲基-2-酮基-U-二氫斗吡 啶基&gt;3·六氫吡啶基]羰基I胺基)曱基]-5-(3-甲氧基丙基)苯酯 MeΟ )) whallin as an alkylation reagent. MS (ESI+, Example 98 4_N-Phofolinecarboxylic acid trans-[[cyclopropyl{[4-(1-methyl-2-keto-U-dihydropyridinyl]&gt;3·hexahydropyridine Alkyl]carbonyl Iamino)indenyl]-5-(3-methoxypropyl)phenyl Me

根據實例96中所述之程序製成,但在步驟1中,替代地 使用嗎福 林-4-氣化破醯作為烧基化作用試劑,三乙胺作為 鹼,及 DMAP 作為觸媒。MS (ESI+,M+H) : 567。 實例99 反式-N-環丙基-N-[6-(3-甲氧基丙基)-2,3-二氫-1H-茚-1-基]-4-(1-甲基-2-酮基-1,2-二氫-4-毗啶基)-3-六氫吡啶羧醯胺 143482-1 • 243 - 201111364It was prepared according to the procedure described in Example 96, but in step 1, alternatively, wortene-4-vaporized dross was used as the alkylating agent, triethylamine was used as the base, and DMAP was used as the catalyst. MS (ESI+, M+H): 567. Example 99 trans-N-cyclopropyl-N-[6-(3-methoxypropyl)-2,3-dihydro-1H-indol-1-yl]-4-(1-methyl- 2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide 143482-1 • 243 - 201111364

根據實例1中所述之程序製成非對映異構物之混合物, 但替代地使用胺85作為起始物質。MS (ESI+,M+H) : 464。再 者’可將兩種非對映異構物在製備型逆相HPLC上分離,然 後移除BOC-保護基。 實例100 反式-N-環丙基_N_[7_(3_曱氧基丙基)四氫小莕基] 曱基-2-酮基-l,2-二氫_4-P比。定基)-3-六氫p比咬缓醯胺A mixture of diastereomers was prepared according to the procedure described in Example 1, but using amine 85 as a starting material instead. MS (ESI+, M+H): 464. Alternatively, the two diastereomers can be separated on preparative reverse phase HPLC and the BOC-protecting group removed. Example 100 trans-N-cyclopropyl_N_[7-(3-methoxypropyl)tetrahydroindenyl]nonyl-2-keto-l,2-dihydro-4-p ratio. Fixed base)-3-hexahydrop ratio

根據實例1中所述之程序製成非對映異構物之混合物, 但替代地使用胺86作為起始物質。再者,可將兩種非對映 異構物在製備型逆相HPLC上分離,然後移除B〇c保護基。 非對映異構物A: MS(ESI+,M+H): 478。人類腎素忙5〇(緩衝 劑):0.3nM。人類腎素%〆血漿):UnM。非對映異構物&amp; MS(ESI+,M+H): 478。人類腎素 IC5〇(緩衝劑):36nM。人類 腎素 IC50(血漿):16.2 nM。 實例101 143482-1 -244- 201111364 反式-N-[3-溴基-5-(3-羥丙基)-4-甲苄基],N-環丙基_4·(1_曱基_2 酮基-1,2-一風-4-ρ比咬基)_3_六氫;7比咬緩醯胺A mixture of diastereomers was prepared according to the procedure described in Example 1, but using amine 86 as the starting material instead. Alternatively, the two diastereomers can be separated on preparative reverse phase HPLC and the B〇c protecting group removed. Diastereomer A: MS (ESI+, M+H): 478. Human renin is busy 5 缓冲 (buffer): 0.3 nM. Human renin % 〆 plasma): UnM. Diastereomer &amp; MS (ESI+, M+H): 478. Human renin IC5 〇 (buffer): 36 nM. Human renin IC50 (plasma): 16.2 nM. Example 101 143482-1 -244- 201111364 trans-N-[3-bromo-5-(3-hydroxypropyl)-4-methylbenzyl], N-cyclopropyl_4·(1_fluorenyl) _2 keto-1,2-one wind-4-ρ ratio bite base)_3_hexahydrogen; 7 than biting slow guanamine

根據實例1中所述之程序製成,但替代地使用胺87作為 起始物質。獲得標題化合物,為白色泡沫物。Ms (esi+ φ M+Na) : 538。 實例102 反式-N-[3-演基-5-(3-乙氧基丙基)-4-曱苄基]·Ν·環丙基_4_(1甲 基-2-酮基-1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺It was made according to the procedure described in Example 1, but instead using amine 87 as the starting material. The title compound was obtained as a white foam. Ms (esi+ φ M+Na): 538. Example 102 trans-N-[3-Acyl-5-(3-ethoxypropyl)-4-indolyl]-indolyl-4-yl-2-yl-2-yl-1 ,2-dihydro-4-pyridyl)_3_hexahydropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用胺88作為 起始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 544 ° 實例103 反式-N-{3-演基-5-[3-(二氟甲氧基)丙基]_4_曱苄基}·Ν_環丙基 -4-(1-甲基酮基-以-二氫-4-吡啶基)_3_六氫吡啶羧醯胺 143482-1 -245- 201111364It was made according to the procedure described in Example 1, but instead using amine 88 as the starting material. The title compound was obtained as a white foam. MS (ESI+, M+H): 544 ° Example 103 trans-N-{3-exyl-5-[3-(difluoromethoxy)propyl]_4_曱benzyl}·Ν_cyclopropyl 4-(1-methylketo-iso-dihydro-4-pyridyl)_3_hexahydropyridine carboxamide 143482-1 -245- 201111364

根據實例1中所述之程序製成,但替代地使用作為起始 物質之胺89及如在實例14步驟8中之溴化鋅(II)-促進之BOC-去除保護。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H): 566。人類腎素IC5〇(緩衝劑):〇·3ηΜ。人類腎素IC50(血 衆):1.4 nM 〇 實例104 反式-N-(3-芊基-5-甲芊基)-N-環丙基-4-(1-甲基-2-酮基_1,2_二氫 -4-吡啶基)-3-六氫吡啶羧醯胺The procedure described in Example 1 was followed, but instead the amine 89 as the starting material and the zinc (II) bromide-promoted BOC-removal protection as in Example 8 Step 8. The title compound was obtained as a white foam. MS (ESI+, M+H): 566. Human renin IC5 (buffer): 〇·3ηΜ. Human renin IC50 (blood group): 1.4 nM 〇 Example 104 trans-N-(3-mercapto-5-methylindolyl)-N-cyclopropyl-4-(1-methyl-2-keto) _1,2_Dihydro-4-pyridyl)-3-hexahydropyridine carboxamide

根據實例1中所述之程序製成,但替代地使用胺9〇作為 起始物質。獲得標題化合物,為白色泡沫物。Ms (ESI+ M+H): 。人類腎素IC5 〇 (緩衝劑):7.5 nM。人類腎素% 〇 (血 漿):21 nM。 實例105 反式-N-[3-溴基-5-(3-氳苄基)-4-曱苄基]_N_環丙基_4 (1曱基-2_ 酮基-1,2-二氫-4-p比咬基)-3-六氫吡咬羧醯胺 143482-1 -246- 201111364It was made according to the procedure described in Example 1, but instead using amine 9 as a starting material. The title compound was obtained as a white foam. Ms (ESI+ M+H): . Human renin IC5 缓冲 (buffer): 7.5 nM. Human renin % 血 (blood): 21 nM. Example 105 trans-N-[3-Bromo-5-(3-indolyl)-4-indolyl]-N-cyclopropyl-4 (1indol-2-yl-1,2-di) Hydrogen-4-p ratio octyl)-3-hexahydropyridylcarboxamide 143482-1 -246- 201111364

根據實例1中所述之程序製成,但替代地使用胺91作為 起始物質β獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 566。 實例106It was made according to the procedure described in Example 1, but the title compound was obtained as a white foam by using the amine 91 as the starting material. MS (ESI+, M+H): 566. Example 106

反式-N-[3-溴基-5-(3-氟苯曱醯基)-4-曱芊基]·Ν-環丙基-4-(1-曱 基-2-酮基-1,2-二氫-4-咐π定基)-3-六氫p比咬缓醯胺trans-N-[3-Bromo-5-(3-fluorophenylindenyl)-4-indenyl]-indole-cyclopropyl-4-(1-indol-2-one-1 ,2-dihydro-4-indolyl)-3-hexahydrop ratio

MeMe

根據實例1中所述之程序製成,但替代地使用胺92作為 起始物質。獲得標題化合物,為白色泡沫物。MS (ESI+, M+H) : 582。 實例107 反式-Ν·{3_漠基-5-[(3-氟苯基)(羥基)曱基]-4-甲苄基卜N-環丙基 -4-(1-曱基-2,基二氫斗吡啶基)各六氫吡啶羧醯胺 143482-1 • 247· 201111364It was made according to the procedure described in Example 1, but instead using amine 92 as the starting material. The title compound was obtained as a white foam. MS (ESI+, M+H): 582. Example 107 trans-Ν·{3_漠基-5-[(3-fluorophenyl)(hydroxy)indolyl]-4-methylbenzylib N-cyclopropyl-4-(1-indolyl- 2, quinone dihydropyridinyl) each hexahydropyridine carboxamide 143482-1 • 247· 201111364

MeMe

於反式-N-[3-漠基-5-(3-氟苯甲醯基)_4_甲字基]_N_環丙基_4_ (1-曱基-2-_基-1,2-一虱-4-ρ比咬基)_3_六氫p比咬-缓醯胺(1當量 ’實例106)之MeOH (0.09M)溶液中,添加硼氫化鈉(1 4當量)。 將所形成之溶液在室溫下攪拌15小時,然後於真空中移除 揮發性物質。於所形成之殘留物中,小心地添加1〇% Ηα水 溶液’接著為IN NaOH水溶液,以致使最後溶液之pH值為 〜10。以EtOAc萃取後,將合併之有機萃液以鹽水進一步洗 滌,以NaaSO4脫水乾燥,過濾,及使濾液在真空中濃縮。 經由管柱層析之進一步純化(Si〇2 ’ 93:7 (v/v) CH2Cl2 :在Me〇H 中之2.0M NH3),獲得標題化合物,為非對映異構物之混合 物。MS (ESI+,M+H) : 584。 實例108 反式-N-[2-氣基-5-(2-甲氧基乙基)芊基]_N•環丙基_4羥基_4 (1_ 曱基-2-酮基-1,2-二氫-4-吡咬基)_3-六氫?比π定敌醯胺In trans-N-[3-Molyl-5-(3-fluorobenzhydryl)_4_yl]]N_cyclopropyl_4_(1-indolyl-2-yl-1,2 Sodium borohydride (14 eq.) was added to a solution of MeOH (0.09 M). The resulting solution was stirred at room temperature for 15 hours and then the volatiles were removed in vacuo. To the residue formed, carefully add 1% aqueous solution of Ηα, followed by aqueous IN NaOH, so that the pH of the final solution was 〜10. After extraction with EtOAc, the combined organic extracts were washed with brine, dried over Na NaSOs, filtered, and evaporated. The title compound was obtained as a mixture of diastereomers. </ RTI> </ RTI> </ RTI> </ RTI> <RTIgt; </ RTI> <RTIgt; MS (ESI+, M+H): 584. Example 108 trans-N-[2-Alkyl-5-(2-methoxyethyl)indenyl]-N•cyclopropyl-4hydroxyl-4 (1-decyl-2-keto-1,2 -dihydro-4-pyridyl)_3-hexahydro?

MeMe

步驟1 . 3-{[[2-氣基-5-(2-甲氧基乙基)芊基κ環丙基)胺基]羰 基M-酮基-1-六氫ρ比°定叛酸第三-丁酯 143482-1 -248- 201111364 將4-酮基-1,3-六氫吡啶二羧酸ι_第三_丁基3_乙酯(丨當量)、 胺4 (1 §罝)及DMAP (0.2當1 )在14〇°C下加熱5小時。如此獲 得之粗產物經由管柱層析之純化(Si〇2,95:5— 3:7 (v/v)己烧: EtOAc) ’接著在9:1 (Wv)己烷:EtzO中涮漱,獲得標題化合 物,為白色固體。 步驟2:反式-4-[2-(爷氧基)-4-吡啶基]_3_{[[2_氣基_5_(2_曱氧基乙 基)苹基](環丙基)胺基]幾基}-4-經基-1-六氫p比咬竣酸第三_丁 醋 在-78°C下,於芳環4之THF溶液(0.05M)中,添加正_ 丁基鋰 (在己烷中之2.5M溶液,2.1當量)。於_78〇C下攪拌3〇分鐘後, 以一快速部份添加固體溴化鎂(2.5當量),並將所形成之混 合物在-78 C下授拌20分鐘。然後,使反應混合物慢慢地溫 熱至〇°C,歷經30分鐘,且以THF溶液添加得自前一步驟之 3-{[[2-氣基-5-(2-曱氧基乙基)芊基](環丙基)胺基]幾基卜4酮基 -1-六氫吡啶羧酸第三-丁醋(1當量^接著,將反應混合物於 φ 〇°C下攪拌1小時,及在室溫下30分鐘《然後,藉由添加飽 和NH4 C1水溶液與喊使反應淬滅。分離水層,並以醚逆萃取。 將合併之有機萃液以鹽水進一步洗滌,以Mgs〇4脫水乾燥, 過滤’及使濾液在真空中濃縮。如此獲得之粗產物經由管 柱層析之純化(Si〇2,96:4— 93:7 (v/v)丙酮:甲苯),獲得標題 化合物。 步驟3 :反式-3_{[[2_氯基_5_(2_曱氧基乙基)爷基](環丙基)胺基] 幾基}-4-羥基-4-(2-酮基-1,2-二氫-4-吡啶基&gt;1-六氫吡啶羧酸第 三-丁酯 143482-1 -249- 201111364 於得自前一步驟之反式_4-[2-(苄氧基)_4·吡啶基]_3_{[[2-氣 基-5-(2-甲氧基乙基)节基](環丙基)胺基]羰基} 4羥基小六氫 吡啶羧酸第三-丁酯(1當量)在EtOAc (0.08M)中之溶液内,添 加鈀(10%w/w,於碳上,〇.5當量)與醋酸(11當量)。將所形 成之懸浮液在氫氣瓶大氣下攪拌4小時。以二氣甲烷使反應 淬滅’並經由過濾’經過矽藻土墊移除不溶物。如此獲得 之濾液之濃縮’獲得標題化合物。 步驟4 :反式-3-{[[2-氣基-5-(2-曱氧基乙基)宇基](環丙基)胺基] 羰基H-羥基-4-(1-甲基-2-酮基-1,2-二氫_4_吡啶基)4_六氫吡啶 羧酸第三-丁酯 在〇°C下,於得自前一步驟之反式_3_{[[2_氣基_5(2甲氧基 乙基)卞基](環丙基)胺基]羰基}-4-羥基-4-(2-酮基-1,2-二氫-4-吡 啶基)-ι-六氫吡啶羧酸第三-丁酯(1當量)之曱醇溶液(〇1M) 中,添加NaOH (2N水溶液,3當量)與疏酸二曱酯(3當量)。 然後,將所形成之混合物在室溫下攪拌12小時。接著,於 真空中移除揮發性物質,並使殘留物於水與二氣曱烧之間 作分液處理。分離水層,且以二氣曱烷逆萃取。將合併之 有機萃液以鹽水進一步洗滌,以MgS〇4脫水乾燥,過濾,及 使濾液在真空中濃縮。如此獲得之粗產物經由管柱層析之 純化(Si〇2 ’ 96:3 (v/v) CHA : MeOH) ’獲得標題化合物。 步驟5 :反式-N-[2-氣基!(2-甲氧基乙基)爷基]_N_環丙基斗羥 基-4-(l-曱基-2-酮基-1,2-二氫-4-吡啶基)_3_六氫吡啶羧醯胺 於得自前一步驟之反式-3-{[[2-氣基-5-(2-甲氧基乙基)芊 基](環丙基)胺基]羰基卜4-羥基-4-(1-甲基-2-酮基-1,2-二氫斗吡 143482-1 -250. 201111364 啶基)-1-六氫吡啶羧酸第三·丁酯(1當量)之CH2Cl2溶液 (0.05M)中’添加HC1 (4ΌΜ二氧陸園溶液,30當量)。將所形 成之溶液在室溫下攪拌3小時。於真空中移除揮發性物質之 後’將所形成之殘留物直接地裝填至以94:6 (v/v) CH2 Cl2 :在 MeOH中之2.0M NHS填充之Si〇2管柱上。以相同溶劑系統之 溶離’獲得標題化合物。]VIS (ESI+,M+H) : 474。 實例109 反式-N-C2-氣基-5-(2-甲氧基乙基)节基;|_N_環丙基_4_甲氧基 -4-(1-甲基-2-酮基-1,2-二氫-4-吡啶基)-3-六氫吡啶羧醯胺Step 1. 3-{[[2-Hydroxy-5-(2-methoxyethyl)indolyl κcyclopropyl)amino]carbonyl M-keto-1-hexahydrop-ratio Third-butyl ester 143482-1 -248- 201111364 4-keto-1,3-hexahydropyridinedicarboxylic acid ι_t-butyl 3-ethyl ester (丨 equivalent), amine 4 (1 § 罝And DMAP (0.2 when 1) was heated at 14 ° C for 5 hours. The crude product thus obtained was purified by column chromatography (Si 〇 2, 95:5 - 3:7 (v/v) hexanes: EtOAc) and then in 9:1 (Wv)hexane:EtzO The title compound was obtained as a white solid. Step 2: trans-4-[2-(yloxy)-4-pyridyl]_3_{[[2_carbyl_5_(2-methoxyethyl)phenyl](cyclopropyl)amine ] 几 } -4- -4- -4- -1- -1- _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ _ Lithium (2.5 M solution in hexane, 2.1 equivalents). After stirring at _78 ° C for 3 minutes, solid magnesium bromide (2.5 equivalents) was added in a quick portion, and the resulting mixture was stirred at -78 C for 20 minutes. Then, the reaction mixture was slowly warmed to 〇 ° C for 30 minutes, and the 3-{[[2-[2-[2-(2-oxyethyl))) Mercapto](cyclopropyl)amino] benzylidene-4-keto-1-pyropyridinecarboxylic acid tert-butyl vinegar (1 equivalent) followed by stirring the reaction mixture at φ ° C for 1 hour, and After 30 minutes at room temperature, the reaction was then quenched by the addition of a saturated aqueous solution of NH.sub.4Cl. The filtrate was filtered and concentrated in vacuo. The crude product thus obtained was purified by column chromatography (Si.sub.2, 96:4-93:7 (v/v) acetone: toluene) to give the title compound. 3: trans-3_{[[2_chloro-5-(2-methoxyethyl)-yl](cyclopropyl)amino] benzyl}-4-hydroxy-4-(2-keto) -1,2-dihydro-4-pyridyl&gt; 1-hexahydropyridinecarboxylic acid tert-butyl ester 143482-1 -249- 201111364 in the previous step of trans-4-[2-(benzyloxy) Base)_4·pyridyl]_3_{[[2-carbo-5-(2-methoxyethyl)] benzyl](cyclopropyl)amine a solution of a carbonyl group of 4 hydroxy hexahydropyridine carboxylic acid in a butyl (0.08 M) solution, palladium (10% w/w on carbon, 〇. 5 eq.) Acetic acid (11 eq.). The resulting suspension was stirred under a hydrogen atmosphere for 4 hours. The reaction was quenched with di-methane and filtered to remove insolubles from celite pad. 'The title compound was obtained. Step 4: trans-3-{[[2-carbyl-5-(2-decyloxyethyl)ylidene](cyclopropyl)amino]carbonyl H-hydroxy-4- (1-methyl-2-keto-1,2-dihydro-4-pyridyl) 4_hexahydropyridinecarboxylic acid tert-butyl ester at 〇 ° C, obtained from the previous step _ 3_{[[2_气基_5(2methoxyethyl)indolyl](cyclopropyl)amino]carbonyl}-4-hydroxy-4-(2-keto-1,2-dihydro Add NaOH (2N aqueous solution, 3 equivalents) to didecyl succinate (3N) in a solution of 1,4-pyridyl)-i-piperidinecarboxylic acid in a butyl alcohol (1 eq.) in decyl alcohol (〇1M). Equivalent). The resulting mixture was then stirred at room temperature for 12 hours. Then, the volatiles were removed in vacuo and left to dry. The liquid layer was separated from the water and the gas mixture, and the aqueous layer was separated and extracted with dioxane. The combined organic extracts were further washed with brine, dried with MgS〇4, filtered, and filtrated. Concentration in vacuo. The crude product thus obtained was purified by column chromatography (Si </ RTI> <RTIgt; </RTI> <RTIgt; Step 5: Trans-N-[2- gas base! (2-methoxyethyl) aryl]_N_cyclopropyl hydroxy-4-(l-fluorenyl-2-keto-1,2-dihydro-4-pyridyl)_3_hexahydropyridine Carboxylamidine in trans-3-{[[2-carbyl-5-(2-methoxyethyl)indenyl](cyclopropyl)amino]carbonyl-4-hydroxy-from the previous step 4-(1-methyl-2-keto-1,2-dihydrobupyridyl 143482-1 -250. 201111364 pyridine)-1-hexahydropyridinecarboxylic acid tert-butyl ester (1 equivalent) of CH2Cl2 Add HCl (4 ΌΜ dioxygen ore solution, 30 equivalents) to the solution (0.05 M). The resulting solution was stirred at room temperature for 3 hours. After removal of the volatiles in vacuo, the resulting residue was directly loaded onto a column of &lt;RTI ID=0.0&gt;&gt;&gt;&gt; The title compound was obtained by dissolving from the same solvent system. ]VIS (ESI+, M+H): 474. Example 109 trans-N-C2-carbyl-5-(2-methoxyethyl));|_N_cyclopropyl_4_methoxy-4-(1-methyl-2-one Base-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide

步驟1 :反式-4-[2-(苄氧基-4-吡啶基)-3-{[[2-氯基-5-(2-甲氧基乙 基)爷基](環丙基)胺基]幾基}-4-甲氧基-1-六氫?比D定叛酸第三 丁酯 於反式-4-[2-(苄氧基)-4-吡啶基]-3-{ [[2-氯基-5-(2-甲氧基乙 基)字基](環丙基)胺基]幾基}-4-經基-1-六氫p比。定缓酸第三_丁 醋(1當量’實例108步驟2)之DMF溶液(0.18M)中,添加氫化 鈉(1.2當量)與碘甲烷(1.2當量)。將反應混合物在室溫下擾 拌30分鐘’然後將其以醚與水稀釋。分離有機層,並以水 與鹽水進一步洗滌’以MgS〇4脫水乾燥,過濾,及使濾液在 真空中濃縮。如此獲得之粗產物經由管柱層析之純化(Si〇2, 3:2 (v/v)己烷:EtOAc— EtOAc),獲得標題化合物。 143482-1 •251 · 201111364 步驟2 .反式_3-{[[2-氣基-5-(2-甲氧基乙基)爷基](環丙基)胺基] 羰基M-曱氧基-4-(2-酮基-1,2-二氫_4_吡啶基)小六氫吡啶羧酸 第三-丁醋 於得自則一步驟之反式_4-[2-(宇氧基-4-吡啶基)-3-{[[2-氣基 -5-(2-甲氧基乙基件基](環丙基)胺基]羰基}_4甲氧基^六氫 吡啶羧酸第三-丁酯(1當量)在Et〇Ac (〇 1M)中之溶液内,添加 鈀(10% w/w,於碳上,〇.5當量)與醋酸(1〗當量)。將所形成 之懸浮液在氫氣瓶大氣下攪拌4小時。以二氯曱烷使反應淬 滅’並經由過濾’經過矽藻土墊移除不溶物。如此獲得之 濾液之濃縮’獲得標題化合物。 步驟3 :反式-3-{[[2-氯基-5-(2-曱氧基乙基)苄基](環丙基)胺基] 幾基}-4-曱氧基_4-(1_曱基_2_酮基-i,2-二氩-4-吡啶基)小六氫吡 咬叛酸第三-丁酯 在〇°C下,於得自前一步驟之反式_3_{[[2_氣基_5_(2甲氧基 乙基)爷基](環丙基)胺基]羰基}-4-曱氧基-4-(2-酮基-1,2-二氫-4-峨咬基)-1-六氫吡啶羧酸第三-丁酯(1當量)之曱醇溶液 (0.07M)中,添加Na〇H (2N水溶液,3當量)與硫酸二曱酯(4 當量)。然後,將所形成之混合物在室溫下攪拌12小時。接 著’於真空中移除揮發性物質,並使殘留物於水與二氯甲 烧之間作分液處理。分離水層,且以二氣曱烷逆萃取。將 合併之有機萃液以鹽水進一步洗滌,以MgS04脫水乾燥,過 滤’及使濾液在真空中濃縮。如此獲得之粗產物經由管柱 層析之純化(Si〇2,96:3 (v/v) CH2C12 : MeOH),獲得標題化合 物0 143482-1 -252· 201111364 步驟5 :反式-N-[2-氣基-5-(2-甲氧基乙基件基]_N_環丙基_4曱 氧基-4-(1-曱基-2-酮基-1,2-二氫-4-吡啶基)_3-六氫吡啶羧醯胺 於得自前一步驟之反式-3-{[[2-氯基-5-(2-曱氧基乙基)节 基](環丙基)胺基機基}-4-甲氧基-4-(1-曱基_2_酮基_u_二氮·4_ 峨咬基)-1-六氫咕啶羧酸第三-丁酯(1當量)之CH2Cl2溶液 (0.05M)中’添加HC1 (4.0M二氧陸圜溶液,30當量)。將所形 成之溶液在室溫下授拌3小時。於真空中移除揮發性物質之 ^ 後’將所形成之殘留物直接地裝填至以94:6 (v/v) CH2C12 :在 MeOH中之2.0M NH3填充之Si〇2管柱上。以相同溶劑系統之 溶離,獲得標題化合物。MS(ESI+,M+H): 488。iHNMR (丙 酮-d6) : 5 (ppm) 0.77-1.03 (m,4H),2.22-2.36 (m,2H),2.52-2.59 (br m, 1H), 2.74-2.85 (br m, 2H), 3.03 (s, 3H), 3.12-3.17 (br m, 2H), 3,28 (s, 3H), 3.32-3.37 (m, 4H), 3.49 (s, 3H), 3.53 (t, d = 7.0 Hz, 1H), 3.91 (br s, 1H), 4.53 (d, J = 13.2 Hz, 1H), 4.75 (d, J = 13.2 Hz, 1H), 6.41 (m, 1H), 6.52 (s, 1H), 7.11-7.15 (m, 2H), 7.31 (d, J = 7.0 Hz, 1H), 7.58 (d, J = 7.〇 Hz, φ 1H)。人類腎素1匚5〇(緩衝劑):1.3nM。人類腎素1(:5〇(血漿)·_ 3.2 nM。 實例110 反式-N-環丙基-4-羥基-N-[3-(2-曱氧基乙氧基)-5-(3-曱氧基丙 基)爷基M-(l-甲基-2-酮基-1,2-二氫-4-p比咬基)-3-六氫?比。定缓醞胺Step 1: trans-4-[2-(benzyloxy-4-pyridyl)-3-{[[2-chloro-5-(2-methoxyethyl)-aryl](cyclopropyl) Amino]]yl}-4-methoxy-1-hexahydro? T-butyric acid tert-butyl ester in trans-4-[2-(benzyloxy)-4-pyridyl]-3-{[[2-chloro-5-(2-methoxyethyl) ) (based on the group) (cyclopropyl)amino]]}}-trans-l-hexahydro-p ratio. Sodium hydride (1.2 eq.) and methyl iodide (1.2 eq.) were added to a DMF solution (0.18 M). The reaction mixture was spoiled at room temperature for 30 minutes' and then it was diluted with ether and water. The organic layer was separated and washed with water and brine &lt;&quot;&quot;&quot;&quot;&quot;&quot;&quot;&quot;&quot; The crude product thus obtained was purified by EtOAc EtOAc EtOAc (EtOAc: 143482-1 •251 · 201111364 Step 2. Trans-_3-{[[2-carbo-5-(2-methoxyethyl)-yl](cyclopropyl)amino]carbonyl M-oxime 4-(2-keto-1,2-dihydro-4-pyridyl) small hexahydropyridinecarboxylic acid, third-butyric acid, obtained from a one-step trans-4-[2-(yu Oxy-4-pyridyl)-3-{[[2-carboethyl-5-(2-methoxyethyl)](cyclopropyl)amino]carbonyl}_4methoxy^hexahydropyridine Palladium (10% w/w on carbon, 〇. 5 eq.) and acetic acid (1 eq.) were added to a solution of the carboxylic acid tert-butyl ester (1 eq.) in Et EtOAc (1M). The resulting suspension was stirred under a hydrogen atmosphere for 4 hours. The reaction was quenched with dichloromethane and filtered to afford insoluble material. Step 3: trans-3-{[[2-chloro-5-(2-decyloxyethyl)benzyl](cyclopropyl)amino] benzyl}-4-decyloxy-4- (1_mercapto-2-oxo-i,2-di-ar- 4-pyridyl) small hexahydropyridyl acid tert-butyl ester at 〇 ° C, obtained from the previous step _ 3_{[[2_气基_5_(2methoxyethyl) aryl] (cyclopropyl) Amino]carbonyl}-4-methoxy-4-(2-keto-1,2-dihydro-4-indole)-1-hexahydropyridinecarboxylic acid tert-butyl ester (1 equivalent) To a solution of decyl alcohol (0.07 M), Na 〇H (2N aqueous solution, 3 eq.) and dimethyl sulphate (4 eq.) were added. Then, the resulting mixture was stirred at room temperature for 12 hours. The volatiles are removed and the residue is partitioned between water and methylene chloride. The aqueous layer is separated and back-extracted with dioxane. The combined organic extracts are further washed with brine to The title compound 0 143482- was obtained as the title compound (yield: EtOAc, EtOAc). 1 -252· 201111364 Step 5: trans-N-[2-carbyl-5-(2-methoxyethyl)]N-cyclopropyl-4-thiol-4-(1-indenyl) 2-keto-1,2-dihydro-4-pyridyl)-3-hexahydropyridine carboxamide in trans-3-{[[2-chloro-5-(2-) from the previous step曱oxyethyl)]]](cyclopropyl)amino group}-4-methoxy-4-(1-indolyl-2-keto-_u_diaza·4_ 峨 bite Adding HCl (4.0 M dioxane solution, 30 equivalents) to a solution of 1-hexahydroacridinecarboxylic acid in a solution of tri-butyl hydride (1 equivalent) in CH 2 Cl 2 (0.05 M). The mixture was warmed for 3 hours. After removing the volatiles in a vacuum, the resulting residue was directly charged to 94:6 (v/v) CH2C12: 2.0 M NH3 filled Si in MeOH. 〇 2 on the column. The title compound was obtained by dissolving in the same solvent system. MS (ESI+, M+H): 488. iHNMR (Acetone-d6): 5 (ppm) 0.77-1.03 (m, 4H), 2.22-2.36 (m, 2H), 2.52-2.59 (br m, 1H), 2.74-2.85 (br m, 2H), 3.03 (s, 3H), 3.12-3.17 (br m, 2H), 3,28 (s, 3H), 3.32-3.37 (m, 4H), 3.49 (s, 3H), 3.53 (t, d = 7.0 Hz, 1H), 3.91 (br s, 1H), 4.53 (d, J = 13.2 Hz, 1H), 4.75 (d, J = 13.2 Hz, 1H), 6.41 (m, 1H), 6.52 (s, 1H), 7.11 -7.15 (m, 2H), 7.31 (d, J = 7.0 Hz, 1H), 7.58 (d, J = 7.〇Hz, φ 1H). Human renin 1匚5〇 (buffer): 1.3 nM. Human renin 1 (: 5 〇 (plasma) · _ 3.2 nM. Example 110 trans-N-cyclopropyl-4-hydroxy-N-[3-(2-decyloxyethoxy)-5-( 3-methoxypropyl) aryl M-(l-methyl-2-keto-1,2-dihydro-4-p ratio dimethyl)-3-hexahydro-pyramine

143482-1 -253 201111364 根據實例108中所述之程序製成’但替代地使用胺11作為 起始物質。MS (ESI+,M+H) ·· 514。 實例111 反式-N-環丙基-4-甲氧基-N-[3-(2-甲氧基乙氧基曱氧基 丙基)节基]-4-(1-甲基-2-酮基-1,2-二氫-4^比°定基)_3_六氫峨咬叛 醯胺143482-1 -253 201111364 Made according to the procedure described in Example 108, but using amine 11 as a starting material instead. MS (ESI+, M+H) ·· 514. Example 111 trans-N-cyclopropyl-4-methoxy-N-[3-(2-methoxyethoxymethoxypropyl)] benzyl]-4-(1-methyl-2 -keto-1,2-dihydro-4^ ratio ° base)_3_hexahydroquinone bite retinodine

MeMe

根據實例109中所述之程序製成,但替代地使用胺11作為 起始物質。MS (ESI+,M+H) : 528。 實例112 証實生物學活性之檢測 人類重組腎素之抑制 使在 50 mM MOPS pH 7.4, 100 mM NaCl,0.002% Tween 20 中,於 最後濃度為100 pM下之人類重組腎素(Proteos)以得自50倍濃籲 DMSO 溶液與 6 μΜ 内部驟冷螢光肽:DNP-Lys-His-Pro-Phe-His-Leu-Val-Ile-His-D,L-Amp (順序識別碼:1)之抑制劑培養; Paschalidou K.等人,所/·,2004, 3S2, 1031)。反應係在 37°C 下,於Costar 384井黑色板(#3573)中進行3小時。螢光係於時 間0與3小時下,以設定在328毫微米激發波長及388毫微米 發射波長下之SpectraMax Gemini EM讀取器度量。將t=0下之背 景螢光自t=3小時下之度量值扣除。化合物之抑制活性係以 143482-1 -254- 201111364 IC5〇表示。 在人類血漿中之腎素之抑制 使人類EDTA-收集之血漿在溫水中快速地解凍,並於4°c 下,在2900克下離心15分鐘。收集上層清液,並於1 nM之 最後濃度下添加重組腎素(Ptoteos)。將血漿轉移至c〇star黑色 384井板(#3573)。由17.5倍濃DMS0溶液添加腎素抑制劑,並 在37°C下預培養10分鐘。將内部驟冷螢光肽QXL520TM -Lys-His-Pro-Phe-His-Leu-Val-Ile-His-Lys (5-FAM) (Anaspec)在 3M Tris pH • 7.2、200 mM EDTA中稀釋,並添加至血漿中。最後濃度為: 6 受質,342 mM Tris,23 mM EDTA。將板於 37°C 下培養 1 小時。板係在時間0與1小時下,於設定在490毫微米激發波 長及520毫微米發射波長下之SpectraMax Gemini EM讀取器中 讀取。將t=0下之背景螢光自t=l小時之度量值扣除。化合物 之抑制活性係以IC50表示。 活體内動物模式 φ 雌性雙重轉基因大白鼠係購自RCC公司,Fiillingsdorf,Made according to the procedure described in Example 109, but instead using amine 11 as the starting material. MS (ESI+, M+H): 528. Example 112 Confirmation of Detection of Biological Activity The inhibition of human recombinant renin was obtained from human recombinant renin (Proteos) at 50 mM MOPS pH 7.4, 100 mM NaCl, 0.002% Tween 20 at a final concentration of 100 pM. 50 times concentrated DMSO solution and 6 μΜ internal quenching fluorescent peptide: DNP-Lys-His-Pro-Phe-His-Leu-Val-Ile-His-D, L-Amp (sequence identification code: 1) inhibition Agent culture; Paschalidou K. et al., /, 2004, 3S2, 1031). The reaction was carried out in a Costar 384 well black plate (#3573) for 3 hours at 37 °C. Fluorescence was measured at a time of 0 and 3 hours with a SpectraMax Gemini EM reader set at an excitation wavelength of 328 nm and an emission wavelength of 388 nm. The background fluorescence at t = 0 is deducted from the metric at t = 3 hours. The inhibitory activity of the compound is represented by 143482-1 -254-201111364 IC5〇. Inhibition of renin in human plasma Human EDTA-collected plasma was rapidly thawed in warm water and centrifuged at 2900 g for 15 minutes at 4 °C. The supernatant was collected and recombinant renin (Ptoteos) was added at a final concentration of 1 nM. Plasma was transferred to c〇star black 384 well plate (#3573). The renin inhibitor was added from a 17.5-fold concentrated DMS0 solution and pre-incubated at 37 ° C for 10 minutes. The internal quenching fluoropeptide QXL520TM-Lys-His-Pro-Phe-His-Leu-Val-Ile-His-Lys (5-FAM) (Anaspec) was diluted in 3M Tris pH • 7.2, 200 mM EDTA, and Add to the plasma. The final concentrations were: 6 substrate, 342 mM Tris, 23 mM EDTA. The plate was incubated at 37 ° C for 1 hour. The plates were read at a time of 0 and 1 hour in a SpectraMax Gemini EM reader set at an excitation wavelength of 490 nm and an emission wavelength of 520 nm. The background fluorescence at t = 0 is deducted from the measure of t = 1 hour. The inhibitory activity of the compound is represented by IC50. In vivo animal model φ Female double transgenic mouse is purchased from RCC, Fiillingsdorf,

Switzerland。全部動物均被保持在相同條件下,且可自由獲 取正常粒狀大白鼠食物與水。首先,將大白鼠在2個月期間 以安那拉普利(enalapril) (1毫克/公斤/天)治療。於安那拉普 利(enalapril)治療停止後大約兩週之後,雙重轉基因大白鼠變 成具高血壓,且達到平均動脈血壓在160-170毫米Hg之範圍 内。 淨送器禮 A -使用 90 毫克 / 公斤 Ketamin-HCl (Ketavet,Parke-Davis,Berlin FRG)與 10 毫克 / 公斤曱苯”塞畊(Rompun, Bayer, 143482-1 - 255 - 201111364Switzerland. All animals were kept under the same conditions and free access to normal granular rat food and water. First, the rats were treated with enalapril (1 mg/kg/day) during 2 months. Approximately two weeks after the cessation of enalapril treatment, the double transgenic rats became hypertensive and reached an average arterial blood pressure in the range of 160-170 mm Hg. Net delivery device A - use 90 mg / kg Ketamin-HCl (Ketavet, Parke-Davis, Berlin FRG) with 10 mg / kg of benzene" (Rompun, Bayer, 143482-1 - 255 - 201111364

LeVerk麵,FRG)之混合物,以腹膜腔内方式使大白鼠麻醉。 將堡力傳以在無菌條件下植人腹膜腔中,其中感測導管 係被放置在指向上游之腎叙 ,d 腎動脈下方之下降主動脈中。將傳 送器縫合至腹肌,並將皮膚閉合。 遙源U旄-遙測術單元#锃 干几係得自 Data Sciences (St. Paul,MN))。 植入之感測係包含經遠垃古立I l ^ 、 丄運接至咼度地安定低傳導應變計壓 力傳感器之流體充填導營7〇 几丹等e (0.7宅未直徑,8公分長;TAllpA_ C40型)’該傳感器係度量相對於真空之絕對動脈壓力,與 射頻傳送H ;!字導皆之頂端以會防止血液回流之黏稠凝膠 充填,並以抗凝血酶原薄膜塗覆,以抑制錢形成。植入 物(長度=2.5公分,直徑_】9八 θ 且虹-1.2么分)重1為9克,且具有6個 月之典型電池壽命〇姑^典怒了 接又益平台(RPC-1 ’ Data Sciences)係將 ’’’、線U連接至數字化之輸入量’其係被送至專用個人電 遂(ompaq deskpro)。動脈壓力係利用得自周圍壓力參考物 ^ Data Sciences)之輸入作校準。收縮、平均及舒張灰 壓係以水銀之毫米(毫米Hg)表示。 立廣鸢力彦里-使具有植入壓力傳送器之雙重轉基因大 白鼠藉由口腔灌食法服用媒劑或1〇毫克/公斤之試驗物質 (每組η-6),並連續地監測平均動脈血壓。試驗物質之作用 係以治療組相對於對照組中《平均動脈壓力(ΜΑρ)之最大 降低表示。 結果 根據本案之化合物為活性,在腎素緩衝劑與血漿兩種檢 測中顯不IC50 &lt;1必I。關於某些化合物之數據係提供在整個 143482-1 • 256· 201111364 上文實例中。 實例113 在經遙測之雌性雙重轉基因大白鼠中,比較待測化合物反 式·Ν·({3-演基-4·甲基·5·[3.(甲氧基)丙基]苯基丨曱基)_N.環丙基 ·4·(1-曱基-2-酮基_1,2·二氫-4-P比啶基)·3·六氫吡啶羧醯胺之口 服與經皮投藥之動物研究 雌性雙重轉基因大白鼠(人類腎素與血管收縮素之轉基 因大白鼠(參閱,例如 Bohlender 等人,J Am Soc Nephrol 11 : 2056 (2000))係經發展出。全部動物均被保持在相同條件下,且可 自由獲取正常粒狀大白鼠食物與水。首先,將大白鼠以安 那拉普利(enalaPril)(l毫克/公斤/天)治療,於生產後3週開始 及在9週期間。遙測傳送器係在安那拉普利(enalaprii)治療停 止後之2至4週内植入。於安那拉普利(enalapril)治療停止後 大約兩週之後,雙重轉基因大白鼠係具高血壓,具有平均 動脈血壓在160-170毫米Hg之範圍内。 #送器禮入-使用異弗烷(isoflurane)(經由吸入,使大 白鼠麻醉。將壓力傳送器在無菌條件下植入腹膜腔中,其 中感測導管係被放置在指向上游之腎動脈下方之下降主動 脈中。將傳送器縫合至腹肌,將皮膚閉合,並將大白鼠個 別地收容於籠子中,放置在遙測接受器墊片上,以使得能 夠在自麻醉恢復期間及之後收集血壓數據。將大白鼠單^ 關在籠子中’歷經遙測術數據之記錄期間。 道你漱名、統-遙測術單元係得自Data Sciences國際①沿汾 Paul MN))。植入之感測器係包含經連接至高度地安定低傳 143482-1 - 257 - 201111364 導應變計壓力傳感器之流體充填導管(。7毫米直徑,8公分 長;TA11PA_C4㈣),該傳感器係度量相對於真空之絕對動 脈壓力,與射頻傳送器。將導f之頂端以會防止血液回流 之黏稠凝膠充填。植入物(長度=2·5公分,直徑=12公分) 重量為9克,且具有6個月之典型電池壽命。接受器平台 (RPC 1 DSI)係將無線k 5虎連接至數字化之輸人量,其係被 送至專用個人電腦。動脈壓力係利用得自周圍壓力參考物 (APR-1 ’ DSI)之輸人作校準。收縮、平均及舒張血壓係以水 銀之毫米(毫米Hg)表示。 相跨㈣結-使藉由接受器所接收之信號在5〇舰下 每5分鐘數字化K)秒。自此信號,導出平均動脈壓力(MAp)、 收縮與舒張血壓(SBP與DPB)、脈壓(pp)、心跳速率(hr)及活 動力(ACT)。數據之—小時移動平均係接著藉由⑽分析軟 體進行。然後’將數據輸出至咖模板,用於計算組群統 计學、在曲線間之面積(ABC)、最大作用及MAp降低之延續 時間。 ##授#-對於口服傳輸,係使具有植入壓力傳送器之雙 重轉基因大白鼠藉由σ腔灌食法服用媒劑(α5%⑽此心5 毫升/公斤)或試驗物質(30毫克/5毫升/公斤)之單一大丸劑 (每組n=5)。在服藥後,使大白鼠返回其籠子。血壓數據係 於經口服藥後收集至高5天。 對於經皮傳輸,具有經植入壓力傳送器之雙重轉基因大 白鼠係在大白鼠之經刮毛皮膚上被給予媒劑(25〇微升1〇〇% DMSO; n=4)或待測化合物(1〇毫克,在25〇微升l〇〇% dms〇中, 143482-1 -258· 201111364 .¾即33毫克/公斤;n=5)之單次塗敷。在2 5%異弗烷(is〇flurane) 麻醉下使大白鼠稍微地鎮靜,並將其背部刮毛,涵蓋4平方 公分面積。使動物返回其籠子,以自麻醉恢復。二十四小 時後,在2.5%異弗烷麻醉下使大白鼠稍微地鎮靜,並將經 到毛之區域以乙醇消毒3次。 於乙醇療·發後,將體積為250微升之只有1〇〇% DMS〇或已 溶於100% DMSQ溶液中之化合物,使用微量吸管塗敷在經 到毛之區域上。於DMSO溶液之完全蒸發後(在塗敷後之5 ^鐘内),將閉塞性透明防水薄膜(()pSite)以黏貼至動物之背 部’涵蓋經刮毛之區域’並將夾套安裝在動物上。停止異 弗烧吸入’並將動物個別地關在籠子中,以供遙測術數據 收集血壓數據係於化合物麵8〇溶液塗敷後收集至高5 天。 /在POMD傳輸後,試驗物質對於ΜΑΡ之作用之舉例結果 係示於圖1與下表7中。A mixture of LeVerk, FRG) was anesthetized in a peritoneal manner. The force is transmitted to the peritoneal cavity under aseptic conditions, wherein the sensing catheter is placed in the descending aorta below the renal artery, which is directed upstream. The transmitter is sutured to the abdominal muscles and the skin is closed. The remote source U旄-telemetry unit #锃 几 is obtained from Data Sciences (St. Paul, MN)). The implanted sensing system consists of a fluid filling guide, which is connected to the low-conductivity strain gauge pressure sensor, which is connected to the 垃度古立I l ^, 丄 〇 〇 〇 〇 〇 〇 〇 〇 〇 〇 ( ( ( ( 0.7 0.7 0.7 0.7 0.7 0.7 0.7 0.7 0.7 0.7 0.7 0.7 0.7 0.7 0.7 0.7 0.7 0.7 ;TAllpA_ C40 type) 'The sensor measures the absolute arterial pressure relative to the vacuum, and the RF transmission H;! The top of the word guide is filled with a sticky gel that prevents blood from flowing back, and is coated with an anti-prothrombin film. To suppress the formation of money. Implant (length = 2.5 cm, diameter _] 9 VIII and rainbow - 1.2 s) weight 1 is 9 gram, and has a typical battery life of 6 months 〇 ^ 典 典 典 又 又 又 益 益 ( (RPC- 1 'Data Sciences' is the connection of ''', line U to digitized input', which is sent to a dedicated personal computer (ompaq deskpro). Arterial pressure is calibrated using inputs from ambient pressure reference ^ Data Sciences. Shrinkage, average, and diastolic gray pressure are expressed in millimeters of mercury (mm Hg).立广鸢力彦里--A double-transgenic mouse with an implanted pressure transmitter is administered with a vehicle or a test substance of 1 mg/kg (n-6 per group) by oral feeding, and the average is continuously monitored. Arterial blood pressure. The effect of the test substance was expressed as the maximum decrease in mean arterial pressure (ΜΑρ) in the treatment group relative to the control group. Results According to the activity of the compound of the present invention, IC50 &lt;1 must be I in both renin buffer and plasma. Data on certain compounds are provided throughout the 143482-1 • 256· 201111364 example above. Example 113 Comparison of the test compound trans-Ν·({3-基基-4·methyl·5·[3.(methoxy)propyl]phenylhydrazine in a telephotometric female double-transgenic mouse. Oral and transdermal of fluorenyl)-N. cyclopropyl·4·(1-mercapto-2-keto-1,2·dihydro-4-P-pyridyl)·3·hexahydropyridine carboxamide Injecting animal studies Female double-transgenic mice (human renin and angiotensin-transgenic mice (see, for example, Bohlender et al., J Am Soc Nephrol 11 : 2056 (2000)) were developed. All animals were maintained. Under the same conditions, the normal granular rat food and water can be obtained freely. First, the rats are treated with enalapril (lmg/kg/day), starting at 3 weeks after production and at During the 9-week period, the telemetry transmitter was implanted within 2 to 4 weeks after the treatment of enalaprii was stopped. After about two weeks after the treatment of enalapril, the double-transgenic mouse was used. The system has hypertension and has an average arterial blood pressure in the range of 160-170 mm Hg. #送器礼入- Using isoflurane (via suction) The rats are anesthetized. The pressure transmitter is implanted into the peritoneal cavity under aseptic conditions, wherein the sensing catheter is placed in the descending aorta below the upstream renal artery. The transmitter is sutured to the abdominal muscles, the skin is placed Closed and the rats were individually housed in cages and placed on the telemetry receptor pad to enable blood pressure data to be collected during and after recovery from anesthesia. The rats were kept in the cages' telemetry data. During the recording period, you are named after the Data Sciences International 1 (by Paul MN). The implanted sensor consists of a fluid-filled catheter (. 7 mm diameter, 8 cm long; TA11PA_C4 (4)) connected to a highly stable low-pass 143482-1 - 257 - 201111364 guided strain gauge pressure sensor. Absolute arterial pressure in vacuum, with RF transmitter. The tip of the guide f is filled with a viscous gel that prevents blood from flowing back. The implant (length = 2.5 cm, diameter = 12 cm) weighs 9 grams and has a typical battery life of 6 months. The Receiver Platform (RPC 1 DSI) connects the wireless k5 to the digitized input and is sent to a dedicated personal computer. Arterial pressure was calibrated using input from an ambient pressure reference (APR-1 ' DSI). Contraction, mean and diastolic blood pressure are expressed in millimeters of mercury (mm Hg). Phase crossing (four) knot - digitizes the signal received by the receiver under the 5 〇 ship every 5 minutes for K) seconds. From this signal, mean arterial pressure (MAp), systolic and diastolic blood pressure (SBP and DPB), pulse pressure (pp), heart rate (hr), and akinetic (ACT) were derived. The data-hour moving average is then performed by (10) analysis software. Then the data is output to the coffee template for calculating the group statistics, the area between the curves (ABC), the maximum effect, and the duration of the MAp reduction. ##授#- For oral delivery, a double transgenic mouse with an implanted pressure transmitter is administered with a vehicle (α 5% (10) of this heart 5 ml/kg) or test substance (30 mg/). A single bolus of 5 ml/kg) (n=5 per group). After taking the medicine, return the rats to their cages. Blood pressure data was collected up to 5 days after oral administration. For transdermal delivery, a dual transgenic rat with an implanted pressure transmitter is administered a vehicle (25 μL 〇〇1% DMSO; n=4) or test compound on the shaved skin of rats. (1 〇 mg, in a 25 μl l l% dms ,, 143482-1 -258· 201111364 .3⁄4 ie 33 mg / kg; n = 5) single application. The rats were slightly sedated under anesthesia of 25% isoflurane and the back was shaved to cover an area of 4 square centimeters. Return the animal to its cage to recover from anesthesia. After twenty-four hours, the rats were slightly sedated under 2.5% isophora anesthesia and sterilized 3 times with ethanol in the area of hair. After the ethanol treatment, a volume of 250 μl of only 1% DMS or a compound dissolved in 100% DMSQ solution was applied to the area where the hair was applied using a micropipette. After complete evaporation of the DMSO solution (within 5 cm of coating), the occlusive transparent waterproof film (() pSite) was adhered to the back of the animal 'covering the shaved area' and the jacket was mounted On animals. The isofluranic inhalation was stopped and the animals were individually housed in cages for telemetry data. Blood pressure data were collected and collected on compound 8 〇 solution for up to 5 days. /Examples of the effect of the test substance on hydrazine after POMD transfer are shown in Figure 1 and Table 7 below.

表7 :試驗物質之TD對Ρ〇傳輸對於ABC 最高MAP減低及 降低^延續時間之卜少幹 途徑 abc3 6 h 最高MAP減低 '— (毫米Hg*h) (毫米Hg) PO ΙΠ43 \57 TD 514 — _ 30 延續時間(天) 2Table 7: TD vs. Ρ〇 Transmission of Test Substance for ABC Maximum MAP Reduction and Reduction ^ Duration of Time Bud Dry Path abc3 6 h Maximum MAP Reduction '- (mm Hg*h) (mm Hg) PO ΙΠ43 \57 TD 514 — _ 30 Duration (days) 2

,藥物動力φ、藥^i學及生物標記物址炎、 係於PO傳輸後,在TG、T6h&amp;T24hT,於經遙測之滿中藉 由尾部採血或頸靜脈内取得,以敎活性物f在系統循^ 中之試驗物質含量與生物利用率(以曲線下方面積或AUC 143482-1 -259- 201111364 估計)。 、血液試樣(0.3毫升)係於TD傳輸後,在I、、及^下, 於、’i遙測之dTG中藉由尾部採血或頸靜脈内取得,以測定 ’舌性物質在系統循環中之試驗物質含量與生物利用率(以 曲線下方面積或AUC估計)。血㈣素活性(pRA)亦在^與 t4 h下度量。試驗物f對於PR A之作用係以在T4 h對^下慰 抑制之百分比表示。舉例之結果係示於下表8中中。 表8 .於P〇對TD傳輸後,試驗物質之TD對PO傳輸之生物利 途徑 AUC24h(—* 小時) 在4小時下之PRA抑制(%) PO 1.8 n.a. TD 2.9 98 n.a.不可取得 用率比較 【圖式簡單說明】 圖1A-B係說明在dTG大白鼠中,待測化合物之TD對PO傳 輸對於平均動脈血壓之比較。 圖2係說明關於結晶形式I之固態C-13 CPMAS NMR光譜。 圖3係說明結晶形式I之熱重分析曲線。 圖4係說明結晶形式I之示差掃描卡計法(&quot;DSC&quot;)曲線。 圖5係說明結晶形式I之X-射線繞射圖樣。 143482-1 -260-, drug dynamics φ, drug ^i learning and biomarker site inflammation, after PO transmission, in TG, T6h &amp; T24hT, in the telemetry of the full by tail blood collection or jugular vein, to the active substance f The amount of test substance and bioavailability in the system (as estimated by the area under the curve or AUC 143482-1 -259- 201111364). The blood sample (0.3 ml) was taken from the TD after the TD transmission, and was taken in the dTG of the 'i telemetry by tail blood sampling or jugular vein to determine the 'tongue substance in the system cycle. Test substance content and bioavailability (estimated by the area under the curve or AUC). Blood (tetra) activity (pRA) was also measured at ^ and t4 h. The effect of test substance f on PR A is expressed as a percentage of inhibition at T4 h. The results of the examples are shown in Table 8 below. Table 8. PRA inhibition (%) of TD to PO transport biochemical pathway of test substance after P传输 to TD transmission (%) PO 1.8 na TD 2.9 98 na unusable rate comparison BRIEF DESCRIPTION OF THE DRAWINGS Fig. 1A-B is a graph showing the comparison of TD versus PO transmission for mean arterial blood pressure of a test compound in dTG rats. Figure 2 illustrates solid state C-13 CPMAS NMR spectra for crystalline Form I. Figure 3 is a graph showing the thermogravimetric analysis of crystalline Form I. Figure 4 is a graph showing the differential scanning card method (&quot;DSC&quot;) of crystalline Form I. Figure 5 illustrates an X-ray diffraction pattern of crystalline Form I. 143482-1 -260-

Claims (1)

201111364 七、申請專利範圍: 〉鹽,其具有式① 一種式I化合物或其藥學上可接受201111364 VII. Scope of application: 〉Salt, which has the formula 1 a compound of formula I or a pharmaceutically acceptable compound thereof 其中:among them: R1係選自下列組成之崎Acvm'w環烧基、 C2-C6烯基、c3_c6環烯基块基,其中各前述係視情 況被1-3個鹵素及/或Ci_C5烷氧基取代; R^R3係獨立選自下列組成之組群:氫、i素、Cl-C5 錄、C3&lt;«烧基、c2&lt;:5烯基、C3_C8if稀基、w块基、 氰基、q-C5烷氧基、芳基及雜芳基, • 其中該雜芳基含有1至3個雜原子,獨立選自下列 組成之組群:N、〇B,其中各N係視情況呈氧化物之形 式,且各S係視情況呈氧化物之形式,選自下列組成之組 群:S(=〇)與 s(=〇)2, 其中该芳基與雜芳基係視情況被M個鹵素取代, ^ 其中該烷基、環烷基、烯基、環烯基、炔基及烷 乳基係視情況被L3個取代基取代,其每一個係獨立選自 下列組成之組群:齒素、Cj-Cs燒基、C2-C5稀基、氰基及 Cl_C5烷氧基,其令各前述烷基、烯基及烷氧基取代基係視 143482-2 201111364 情況被1-3個鹵素取代; W為環丙基,未經取代或被氟單-、二-、三-、四_ 或五取代, X係選自下列組成之組群:OR4、R4、-(c! -C5伸烷 基)-(〇)〇-1 -芳基及-(q -C5伸烷基)-(0)〇_丨-雜芳基, 其中R4係選自下列組成之組群:氫、C丨-C5烷基、 (:3-(:8環烷基、c2-C5烯基 ' (:3-(:8環烯基、C2-C5炔基、q-cv 氰基、-(C〗-C5 伸烷基)-〇-R5、-(C〗-C5 伸烷基)-N(-R5 )-(:(=〇)-(CVQ 烷基)、-(q-Q 伸烷基 烷基)、謇 -(q-Q 伸烷基)-N(_R5)_c(=0)_0_(Ci_C5 烷基)、-(Ci_C5 伸烷 基)-0-C(=0)-N(-R5 )-((^ -C5 烷基)、-(q -C5 伸烷基)-N(-R5 )-(C丨-C5 烧基)、-(C〗-C5伸烷基)-S·% -C5烷基)、-(C〗-C5伸烷基)-S(=〇)-(Ci -C5 烧基)及 _(Cl _c5 伸烷基)_s(=0)2 _(Ci _c5 烷基), 其中R4 ’除了氫以外,係視情況被u個取代基取 代’取代基獨立選自下列組成之組群:鹵素、C(=〇)〇h、 q-c:5烷基、CyC:5烯基及Ci_C5烷氧基,其中各烷基、烯基 及烧氧基取代基係視情況被1_3個鹵素取代, ® 其中-(q -C:5伸烷基)-(〇)〇M -雜芳基之雜芳基含有 1-3個雜原子’獨立選自下列組成之組群:n、〇及s,其 中各N係視情況呈氧化物之形式,且各s係視情況呈氧化 物之形式’選自下列組成之組群:s(=0)與s(=0)2 , 其中-(q-c:5伸烷基)-(〇)〇_「芳基與_(Ci_C5伸烷基)_ (〇)〇-〖-雜芳基之芳基與雜芳基係個別視情況被14個_素 取代,且 143482-2 -2- 201111364 其中R5係選自下列組成之組群:氫、Cl _c6烷基' q-c:6環燒基、c:2%烯基、c3_C6環烯基及仏^炔基,其中 各前述烧基、環烷基、烯基、環烯基及炔基取代基係視情 況被1-3個鹵素取代; Z為CrQ伸烷基’視情況被μ2個取代基取代,取代 基獨立選自下列組成之組群:il素、q-Cs烷基及C3環烷 基,其中前述烷基與環烷基取代基係視情況被13個鹵素 _ 取代; nl為0或1 ; γ為⑴五-或六-員飽和或不飽和雜環族或碳環族單 衣狀J衣(單環狀環&quot;),或⑼五或六員飽和或不飽和雜環 族或碳裱族環,其係經稠合至五-或六-員飽和或不飽和雜 環族或碳環族環(”稠合環&quot;), 其中⑴或(ii)之雜環含有1_3個獨立選自Ν、〇及s 之雜原子’其中各N係視情況呈氧化物之形式,且各S係 • 視隋/兄呈氧化物之形式,選自下列組成之組群:s(=〇)鱼 S(=〇)2, 、 其中(i)或(ii)之雜環族或碳環族環係視情況經單_ 、 一— 、 一 一 二-、四五-或六取代,其中各取代基係獨立選 自下列組成之組群: 、 (1) 鹵素, (2) -OH » ⑶-NH(R6), (4)酮基, 143482-2 201111364 (5) -C(=0)-R6, (6) -0C(=0)-R6, (7) Q -C5烧基’視情況被1-3個鹵素取代, (8) C3-C8環烷基,視情況被1-3個鹵素取代’ (9) C2-C5稀基,視情況被1-3個鹵素取代, (10) C3-C8環烯基,視情況被1-3個鹵素取代, (11) C2-C5炔基,視情況被1-3個鹵素取代, (12) Q-C5烷氧基,視情況被1-3個鹵素取代’ (13) 氰基, (14) C〗-C5 -氰基’視情況被1-3個鹵素取代’ (15) -〇CF3, (16) -C(R7)3, (17) -(q -C5伸烧基)-OR8,視情況被1-3個鹵素取代, (18) -N(R6 MQ -C5伸烷基)-OR8,視情況被1-3個鹵素 取代, (19) -Ο-Α -C5伸烷基)-OR8,視情況被1-3個鹵素取 代, (20) -S-% -C5伸烧基)-〇R8 ’視情況被1-3個_素取 代, (21) -8(=0)-((1^ -C5伸烧基)-OR8,視情況被i_3個鹵素 取代, (22) -S(=0)2 -(q -C5伸烷基)-OR8,視情況被ι_3個鹵 素取代, (23) -(C! -C5 伸烧基)^(1^6)-(^(=0)-((^ -C5 伸烧基)-R8, -4- 143482-2 201111364 視情況被1-3個鹵素取代’ (24) -((VQ伸烷基)-N(R6)-C(=0)-0R8 ’ 視情況被 1-3 個鹵素取代’ (25) -(C! -C5伸烷基)-N(R6 )(R8),視情況被1-3個鹵素 取代, (26) -O-CCi -C5 伸烷基)-C(R6)2-C(=0)0R8,視情況被 1-3個li素取代’ (27) -(A -C5 伸烷基)-C(R6)2-C(=0)0R8 ’ 視情況被 1-3 ®個鹵素取代, (28) -CKq -C5伸院基)-嗎福淋,視情況被1-3個鹵素 取代, (29) -0C(=0)-嗎福 p林’ (30) -SR8, (31) -S(=0)-Rs, (32) -S(=0)2-R8 ^ (33) -N(R6)(R8), (34) -(q -C5伸烷基)-C(R6 )2 -(R8),視情況被1-3個鹵 素取代, (35) -(R9)〇-iR10 ’ (36) C2 -C5烯基-OR8,視情況被U個鹵素取代, (37) C2-C5炔基-OR8,視情況被1-3個鹵素取代, (38) -(Ci -C5 伸烷基)-(:(=0)-((^ -C:5 伸烷基)-R8,視情 況被1-3個鹵素取代’ (39) -(C1-C5 伸院基)-〇_C(=0)-(Ci -C5 伸淀基)-R8 ’ 視情 143482-2 201111364 況被1-3個鹵素取代, (40) -(CVQ伸烷基)-C(=〇)-N(R6)(R8),視情況被 1_3 個鹵素取代, (41) -(C〗-C5 伸烷基)-〇-C(=〇)-N(R6 )(R8 ),視情況被]μ3 個鹵素取代, (42) -(C! -C:5伸院基)-SR8 ’視情況被1-3個齒素取代, (43) -(Q -C:5伸烷基)-S(=〇)-R8,視情況被i_3個鹵素 取代,及 (44) -(Q -C5伸烷基)-S(=〇)2-R8 ’視情況被i_3個鹵素 取代, 其中R6係選自下列組成之組群:氫、q -C6烷基、 CVC:8環烷基、CyC6烯基、〇:3-0:8環烯基及c2-C6炔基,其中 各前述烷基、環烷基、烯基、環烯基及炔基取代基係視情 況被1-3個鹵素取代, 其中R7為鹵素, 其中R8係選自下列組成之組群:氫、q -C6烷基、 匚3 -Cg環院基、C:2 -C:6烯基、C:3 -C8環稀基及c2 -C6快基,其中 各前述烷基、環烷基、烯基、環烯基及炔基取代基係視情 況被1-3個鹵素取代, 其中R9係選自下列組成之組群:_匚(11)(011)-、-(:(=0)- ' -0C(=0)-、-C(=0)0- ' -0-、-OC(=〇)〇-、Ci-Cs伸烷基、C2-C5 伸烯基、-风116)-、各、-50=〇)-、-8(=〇)2-、_]^(116)-(:(=〇)-、-(:(;=〇;)- N(R6)-、-〇C(=0)-N(R6)-、-N(R6)-C(=〇)〇-、_n(R6)-S(=0)2-、 -S(=0)2_N(R6)-,其中各前述伸烷基與伸烯基取代基係視情 143482-2 -6- 201111364 況被1-3個鹵素取代,且其中尺6係定義於上文,及 ”中R為五_或六-員飽和或不飽和雜環族或碳 環族環,其係視情況經單、二、三_、四·或五取代,其 中各取代基係獨立選自下列組成之組群:鹵素、OH、_sr6、 ^6)(妁、Cl-C5烷基、Μ環烷基、%婦基、㈣環 土、eve#基、Ci&lt;^氧基、及c 該雜環含有⑴個獨立選自N、〇M之雜原子,其各中 係視情況呈氧化物之“ f其中各N 式,選自下歹&quot;且1 且各8係視情況呈氧化物之形 係定義於上文。、组群:S(=〇)W(=〇)2,及其中_R8 2. 如請求項1之化合物, 個別選自下列:R1 is selected from the group consisting of the following Acvm'w cycloalkyl, C2-C6 alkenyl, c3_c6 cycloalkenyl block groups, wherein each of the foregoing is optionally substituted with 1-3 halogens and/or Ci_C5 alkoxy groups; ^R3 is independently selected from the group consisting of hydrogen, i, Cl-C5, C3&lt;>alkyl, c2&lt;:5 alkenyl, C3_C8if dilute, w block, cyano, q-C5 alkane An oxy group, an aryl group and a heteroaryl group, wherein the heteroaryl group contains 1 to 3 hetero atoms independently selected from the group consisting of N, 〇B, wherein each N is optionally in the form of an oxide. And each S is optionally in the form of an oxide selected from the group consisting of S(=〇) and s(=〇)2, wherein the aryl and heteroaryl are optionally substituted by M halogens, Wherein the alkyl, cycloalkyl, alkenyl, cycloalkenyl, alkynyl and alkaneyl groups are optionally substituted by L3 substituents, each of which is independently selected from the group consisting of dentate, Cj a -Cs alkyl group, a C2-C5 dilute group, a cyano group and a Cl_C5 alkoxy group, wherein each of the aforementioned alkyl, alkenyl and alkoxy substituents is substituted by 1-3 halogens depending on the case of 143482-2 201111364; Is a cyclopropyl group, Unsubstituted or substituted by fluorine mono-, di-, tri-, tetra- or penta, X is selected from the group consisting of OR4, R4, -(c! -C5 alkyl)-(〇)〇 -1 -Aryl and -(q -C5alkylene)-(0)〇_丨-heteroaryl, wherein R4 is selected from the group consisting of hydrogen, C丨-C5 alkyl, (:3 -(: 8-cycloalkyl, c2-C5 alkenyl' (: 3-(:8 cycloalkenyl, C2-C5 alkynyl, q-cv cyano, -(C-C5 alkyl)-〇- R5, -(C)-C5 alkylene)-N(-R5)-(:(=〇)-(CVQ alkyl), -(qQalkylalkyl), 謇-(qQ alkyl) -N(_R5)_c(=0)_0_(Ci_C5 alkyl), -(Ci_C5 alkyl)-0-C(=0)-N(-R5)-((^-C5 alkyl), -(( q -C5 alkylene)-N(-R5)-(C丨-C5 alkyl), -(C-C5 alkylene)-S·%-C5 alkyl), -(C)-C5 Alkyl)-S(=〇)-(Ci-C5 alkyl) and _(Cl _c5 alkyl)_s(=0)2 _(Ci _c5 alkyl), wherein R4 'except hydrogen, as the case may be Substituted by u substituents' substituents are independently selected from the group consisting of halogen, C(=〇)〇h, qc:5 alkyl, CyC:5 alkenyl and Ci_C5 alkoxy, wherein each alkyl group, Alkenyl and alkoxy The thiol group is optionally substituted by 1 to 3 halogens, wherein -(q -C:5alkylene)-(〇)〇M-heteroaryl heteroaryl has 1-3 heteroatoms independently selected from the following The group consisting of n, 〇 and s, wherein each N is in the form of an oxide, and each s is in the form of an oxide as the case is selected from the group consisting of: s (=0) and s (=0)2, wherein -(qc:5alkylene)-(〇)〇_"aryl and _(Ci_C5alkyl)-(〇)〇-〖-heteroaryl aryl and heteroaryl The base system is individually substituted by 14 _ 素, and 143482-2 -2- 201111364 wherein R5 is selected from the group consisting of hydrogen, Cl _c6 alkyl 'qc: 6 cycloalkyl, c: 2% olefin a c3_C6 cycloalkenyl group and a decyl alkynyl group, wherein each of the above alkyl, cycloalkyl, alkenyl, cycloalkenyl and alkynyl substituents is optionally substituted with 1 to 3 halogens; Z is a CrQ alkyl group 'Substituted by μ2 substituents, the substituents are independently selected from the group consisting of il, q-Cs alkyl and C3 cycloalkyl, wherein the alkyl and cycloalkyl substituents are optionally treated as 13 Halogen _ substituted; nl is 0 or 1; γ is (1) five- or six-member And or an unsaturated heterocyclic or carbocyclic monocoat J (monocyclic ring), or (9) a five or six membered saturated or unsaturated heterocyclic or carbocyclic ring, which is fused to five Or a six-membered saturated or unsaturated heterocyclic or carbocyclic ring ("fused ring"), wherein the heterocyclic ring of (1) or (ii) contains 1 to 3 heteroatoms independently selected from ruthenium, osmium and s. Each of the N systems is in the form of an oxide, and each S system is in the form of an oxide selected from the group consisting of: s(=〇) fish S(=〇)2, wherein The heterocyclic or carbocyclic ring of (i) or (ii) is optionally substituted by mono-, mono-, di-, tetra- or hexa-, wherein each substituent is independently selected from the group consisting of Group: , (1) Halogen, (2) -OH » (3)-NH(R6), (4) Keto, 143482-2 201111364 (5) -C(=0)-R6, (6) -0C(= 0)-R6, (7) Q-C5 alkyl group is optionally substituted by 1-3 halogens, (8) C3-C8 cycloalkyl, optionally substituted by 1-3 halogens ' (9) C2-C5 a dilute base, optionally substituted with 1-3 halogens, (10) a C3-C8 cycloalkenyl group, optionally substituted with 1-3 halogens, (11) C2-C5 alkynyl, optionally substituted by 1-3 halogens, (12) Q-C5 alkoxy, optionally substituted with 1-3 halo' (13) cyano, (14) C -C5 -Cyano group 'Substituted by 1-3 halogens' (15) -〇CF3, (16) -C(R7)3, (17) -(q -C5 extended alkyl)-OR8, as appropriate Substituted by 1-3 halogens, (18) -N(R6 MQ -C5 alkylene)-OR8, optionally substituted by 1-3 halogens, (19) -Ο-Α-C5 alkylene)-OR8 , as the case may be replaced by 1-3 halogens, (20) -S-% -C5 stretching base) - 〇R8 'replaced by 1-3 _ primes, (21) -8 (=0)-( (1^-C5 extended alkyl)-OR8, optionally substituted by i_3 halogens, (22) -S(=0)2 -(q -C5alkyl)-OR8, optionally substituted by ι_3 halogens, (23) -(C! -C5 Stretching base)^(1^6)-(^(=0)-((^ -C5 extension base)-R8, -4- 143482-2 201111364 Depending on the situation, 1 -3 halogen substitutions '(24) -((VQalkyl)-N(R6)-C(=0)-0R8 'Substituted by 1-3 halogens' (25) -(C! -C5 Alkyl)-N(R6)(R8), optionally substituted with 1-3 halo, (26) -O-CCi-C5 alkyl)-C(R6)2-C(=0)0R8, 1-3 li Generation '(27) -(A -C5alkylene)-C(R6)2-C(=0)0R8 ' is replaced by 1-3 ® halogens as appropriate, (28) -CKq -C5 - 福福, which is replaced by 1-3 halogens as appropriate, (29) -0C(=0)-?福普林' (30) -SR8, (31) -S(=0)-Rs, (32 ) -S(=0)2-R8 ^ (33) -N(R6)(R8), (34) -(q -C5alkyl)-C(R6)2 -(R8), as appropriate -3 halogen substitutions, (35) -(R9)〇-iR10 ' (36) C2 -C5 alkenyl-OR8, optionally substituted by U halogens, (37) C2-C5 alkynyl-OR8, as appropriate 1-3 halogen substitutions, (38) -(Ci -C5 alkylene)-(:(=0)-((^-C:5 alkyl)-R8, optionally substituted by 1-3 halogens '(39) -(C1-C5 伸院基)-〇_C(=0)-(Ci -C5 伸基基)-R8 ' Subject to 143482-2 201111364 Condition replaced by 1-3 halogens, (40 -(CVQalkylene)-C(=〇)-N(R6)(R8), optionally substituted by 1_3 halogens, (41) -(C--C5 alkylene)-〇-C(= 〇)-N(R6)(R8), as the case may be, replaced by μ3 halogens, (42) -(C! -C:5 extension yard)-SR8 'Substituted by 1-3 fangs, ( 43) -(Q -C:5 alkylene)-S(=〇)-R8, as appropriate by i_3 Halogen substitution, and (44) -(Q -C5alkylene)-S(=〇)2-R8 'Substituted by i_3 halogens, wherein R6 is selected from the group consisting of hydrogen, q-C6 Alkyl, CVC: 8-cycloalkyl, CyC6 alkenyl, anthracene: 3-0:8 cycloalkenyl and c2-C6 alkynyl, wherein each of the aforementioned alkyl, cycloalkyl, alkenyl, cycloalkenyl and alkynyl groups The substituent is optionally substituted by 1-3 halogens, wherein R7 is halogen, wherein R8 is selected from the group consisting of hydrogen, q-C6 alkyl, 匚3-Cg ring, C:2-C a 6-alkenyl group, a C:3-C8 ring-and-lith group, and a c2-C6-radical group, wherein each of the aforementioned alkyl, cycloalkyl, alkenyl, cycloalkenyl and alkynyl substituents is optionally 1 to 3 halogens. Substituted, wherein R9 is selected from the group consisting of: 匚(11)(011)-, -(:(=0)- ' -0C(=0)-, -C(=0)0- ' - 0-, -OC(=〇)〇-, Ci-Cs alkylene group, C2-C5 alkenyl group, -wind 116)-, each, -50=〇)-, -8 (=〇) 2-, _]^(116)-(:(=〇)-, -(:(;=〇;)- N(R6)-, -〇C(=0)-N(R6)-, -N(R6) -C(=〇)〇-, _n(R6)-S(=0)2-, -S(=0)2_N(R6)-, wherein each of the aforementioned alkylene and alkenyl substituents is as defined above. 482-2 -6- 201111364 is replaced by 1-3 halogens, and wherein the uldent 6 is defined above, and "wherein R is a five- or six-membered saturated or unsaturated heterocyclic or carbocyclic ring, The substituents are mono-, di-, tri-, tetra- or penta-substituted, wherein each substituent is independently selected from the group consisting of halogen, OH, _sr6, ^6) (妁, Cl-C5 alkyl, Indole cycloalkyl, % cation, (iv) ring, eve#, Ci&lt;^oxy, and c. The heterocyclic ring contains (1) heteroatoms independently selected from N and 〇M, each of which is oxidized as appropriate The "f" of each of the formulas N, selected from the lower jaw" and 1 and each of the 8 systems are defined as oxides as defined above. , group: S (= 〇) W (= 〇) 2, and _R8 2. The compound of claim 1 is selected from the following: 其中Y⑴或⑻之單環狀或稠合環係a single ring or fused ring system of Y(1) or (8) 143482-2 201111364143482-2 201111364 3·如請求項1之化合物,其中R1為-ch3或-CH2CH3。 4.如請求項1之化合物,其中R2與r3係獨立選自下列組成之 組群:Η、-〇ch2〇CH3及-CH3。 5·如請求項1之化合物,其中X為Η ' -OH或-〇CH3。 6·如請求項1之化合物,其中(Z)nl為-CH2-或鍵結。 7. 如請求項2之化合物,其中: R1為視情況被1-3個鹵素取代之q -C2烷基, R2與R3係獨立選自下列組成之組群:氫、鹵素、Ci—q 烷基、q -C:5烷氧基及-ο-% -C5伸烷基)_〇_(CH2 )0 _ 3 -CH3,其 中烧基、烧氧基及_〇_(CrC5伸烷基)_〇_(CH2 )〇 — 3 _CH3係視情況 被1-3個取代基取代’取代基獨立選自下列組成之組群: 齒素、視情況被1-3個鹵素取代之Cl _c5烷基及視情況被1-3 個i素取代之(^-(:5烷氧基, X係選自下列組成之組群:氫、烷氧基, 且 Z為C】-C〗伸烧基。 8. 如睛求項1之化合物,其中γ係 ) 143482-2 201111364 視情况如請求項1中所述經單_、二-、三-、四-或五取代 9.如請求項7之化合物,其具有式(II)3. The compound of claim 1, wherein R1 is -ch3 or -CH2CH3. 4. The compound of claim 1, wherein R2 and r3 are independently selected from the group consisting of hydrazine, -〇ch2〇CH3, and -CH3. 5. The compound of claim 1, wherein X is Η '-OH or -〇CH3. 6. The compound of claim 1, wherein (Z)nl is -CH2- or a bond. 7. The compound of claim 2, wherein: R1 is a q-C2 alkyl group optionally substituted with 1-3 halogens, and R2 and R3 are independently selected from the group consisting of hydrogen, halogen, Ci-q alkane Base, q -C:5 alkoxy and -ο-% -C5 alkyl)_〇_(CH2)0 _ 3 -CH3, wherein alkyl, alkoxy and _〇_(CrC5 alkyl) _〇_(CH2)〇-3 _CH3 is optionally substituted with 1-3 substituents. The substituents are independently selected from the group consisting of dentate, optionally substituted with 1-3 halogens, Cl _c5 alkyl. And optionally substituted by 1-3 i-(^-(:5 alkoxy, X is selected from the group consisting of hydrogen, alkoxy, and Z is C)-C. 8. A compound of claim 1, wherein gamma is 143482-2 201111364, as the case requires, by mono-, di-, tri-, tetra- or penta-substituted 9. The compound of claim 7 , which has the formula (II) 其中:among them: A係選自下列組成之組群: ⑴氫, (2)南素, ⑶ Q-C5烷基, ⑷ q-Cs烷氧基,及 (5) -S-(CH2)0-3-CH3, 其中⑶與(4)係視情況被1-3個鹵素取代, B係選自下列組成之組群: ⑴氫, (2)鹵素, ⑶ G -C5烧基, (4) Q -C5院氧基, (5) -OH, ⑹-CF3, ⑺-C(=0)-CH3, ⑻-〇-(Α -C5伸烷基)-〇·環丙基, (9) -CKq -C5 伸烷基)-〇_(CH2 )〇 _ 2 _CH3, 143482-2 201111364 (10) -(Ci -C5 伸烷基)-0-(CH2 )〇 - 2 -CH3, (11) -0C(=0)-嗎福淋, (12) -CKCi -C5伸炫基)-嗎福淋, (13) -CKCi -C5 伸烷基)-C(CH3 )2 -C(=0)0H, (14) -CKCi -C5 伸烷基)-C(CH3 )2 -c(=o)och3, (15)Group A is selected from the group consisting of: (1) hydrogen, (2) south, (3) Q-C5 alkyl, (4) q-Cs alkoxy, and (5) -S-(CH2)0-3-CH3, Wherein (3) and (4) are replaced by 1-3 halogens, and B is selected from the group consisting of: (1) hydrogen, (2) halogen, (3) G-C5 alkyl, (4) Q-C5 courtyard oxygen Base, (5) -OH, (6)-CF3, (7)-C(=0)-CH3, (8)-〇-(Α-C5 alkyl)-〇·cyclopropyl, (9) -CKq-C5 alkylene Base)-〇_(CH2)〇_ 2 _CH3, 143482-2 201111364 (10) -(Ci -C5 alkyl)-0-(CH2 )〇-2 -CH3, (11) -0C(=0) - 福福淋, (12) -CKCi -C5 stretching base) - 福福,, (13) -CKCi -C5 alkyl)-C(CH3)2 -C(=0)0H, (14) - CKCi -C5 alkyl)-C(CH3 )2 -c(=o)och3, (15) 其中(3),⑷,(8),(9), (10),(12),(13),(14), (15)及(16)係視 情況被1-3個鹵素取代, C係選自下列組成之組群: ⑴氫, (2) G -C5院基,視情況被1-3個鹵素取代’及 (3) C! -C5烷氧基,視情況被1_3個鹵素取代,且 籲 D係選自下列組成之組群: (1) 氫, (2) 鹵素, (3) -C5 烧基, ⑷ CVC5烷氧基, (5) CVC5-氰基, (6) C2 -C5 伸烯基-〇_(ch2 )〇 _ 2 -CH3, 143482-2 -10- 201111364 ⑺-(q -c5 伸烷基)-n(h)-c(=o)-o-(ch2 )G. 2 -CH3, ⑻-(q -C5 伸烷基)-N(H)-C(=0)-(CH2 )Q - 2 -CH3, ⑼-(Ci -c5 伸烷基)-o-chf2, (10) -(q -c5 伸烷基)-o-(ch2 )〇 · 2 -CH3, (11) -CKCi -c5 伸烷基)-o-(ch2 )〇 _ 2 -CH3, (12) -((VC5 伸烷基)-OH, (13) -S-(Ci-C5伸烷基)-OH, (14) -SCF3, (15) -NOIHQ -C5 伸烷基)-〇-(CH2 )〇 _ 2 -CH3,及 (16)Wherein (3), (4), (8), (9), (10), (12), (13), (14), (15) and (16) are replaced by 1-3 halogens, C It is selected from the group consisting of: (1) hydrogen, (2) G-C5, based on the case, substituted by 1-3 halogens, and (3) C! -C5 alkoxy, optionally substituted by 1_3 halogens And D is selected from the group consisting of: (1) hydrogen, (2) halogen, (3) -C5 alkyl, (4) CVC5 alkoxy, (5) CVC5-cyano, (6) C2 - C5 exo alkenyl-〇_(ch2)〇_ 2 -CH3, 143482-2 -10- 201111364 (7)-(q -c5 alkyl)-n(h)-c(=o)-o-(ch2 ) G. 2 -CH3, (8)-(q -C5 alkylene)-N(H)-C(=0)-(CH2)Q - 2 -CH3, (9)-(Ci-c5 alkylene)-o- Chf2, (10) -(q -c5 alkyl)-o-(ch2)〇· 2 -CH3, (11) -CKCi -c5 alkyl)-o-(ch2 )〇_ 2 -CH3, ( 12) -((VC5 alkyl)-OH, (13) -S-(Ci-C5 alkyl)-OH, (14) -SCF3, (15) -NOIHQ -C5 alkyl)-〇- (CH2)〇_ 2 -CH3, and (16) 其中F、G及H係獨立選自下列組成之組群:氫、 鹵素及C! -C3烧基,且 其中R11係選自下列組成之組群:_CH2_、_c⑻(〇H)_ 及-C(=〇)-,及 其中(3),(4),(5),⑹,(7),⑻,⑼,⑽,(11),(12),(13)及 (15)係視情況被1_3個鹵素取代, 或其立體異構物,或其藥學上可接受之鹽,或其立體異構 物之藥學上可接受鹽。 1〇·如請求項1之化合物,其中化合物係選自下列 143482-2 201111364Wherein F, G and H are independently selected from the group consisting of hydrogen, halogen and C!-C3 alkyl, and wherein R11 is selected from the group consisting of: _CH2_, _c(8)(〇H)_ and -C (=〇)-, and its (3), (4), (5), (6), (7), (8), (9), (10), (11), (12), (13) and (15) depending on the situation Substituted by 1-3 halogens, or a stereoisomer thereof, or a pharmaceutically acceptable salt thereof, or a pharmaceutically acceptable salt thereof. 1) The compound of claim 1, wherein the compound is selected from the group consisting of 143482-2 201111364 143482-2 •12- 201111364143482-2 •12- 201111364 143482-2 -13- 201111364143482-2 -13- 201111364 143482-2 -14- 201111364143482-2 -14- 201111364 143482-2 -15- 201111364 或其立體異構物,或其藥學上可接受之鹽,或其立體異構 物之藥學上可接受鹽。 11.如請求項10之化合物,其係為 實例103 CH3143482-2 -15- 201111364 or a stereoisomer thereof, or a pharmaceutically acceptable salt thereof, or a pharmaceutically acceptable salt thereof, or a stereoisomer thereof. 11. The compound of claim 10, which is exemplified by example 103 CH3 或其藥學上可接受之鹽。 12.如請求項10之化合物,其係為 實例89 ch3Or a pharmaceutically acceptable salt thereof. 12. The compound of claim 10, which is exemplified by example 89 ch3 或其藥學上可接受之鹽。 13.如請求項10之化合物,其係為 實例85 ch3Or a pharmaceutically acceptable salt thereof. 13. The compound of claim 10, which is exemplified by example 85 ch3 或其藥學上可接受之鹽。 14.如請求項10之化合物,其係為 143482-2 -16- 201111364 實例80 ch3Or a pharmaceutically acceptable salt thereof. 14. The compound of claim 10 which is 143482-2 -16-201111364 instance 80 ch3 或其藥學上可接受之鹽。 15.如請求項10之化合物,其係為 實例109 ch3Or a pharmaceutically acceptable salt thereof. 15. The compound of claim 10, which is exemplified by example 109 ch3 ch3 或其藥學上可接受之鹽。 16.如請求項10之化合物,其係為 實例5Ch3 or a pharmaceutically acceptable salt thereof. 16. The compound of claim 10, which is example 5 或其藥學上可接受之鹽。 17.如請求項1之化合物,其中Y係Or a pharmaceutically acceptable salt thereof. 17. The compound of claim 1, wherein the Y system 視情況如請求項1中所述經單 取代。 三-、四- 、五-或六 143482-2 -17- 201111364 18.如請求項7 之化合物,其具有式(ΠΙ): III R1It is monosubstituted as described in claim 1. Tri-, tetra-, five- or six 143482-2 -17- 201111364 18. The compound of claim 7, which has the formula (ΠΙ): III R1 其中: A係選自下列組成之組群: (1) 氫, (2) _素, 籲 ⑶ Q -C5烷基,視情況被i_3個i素取代, (4) Q -C5院氧基’視情況被1-3個鹵素取代’及 (5) 氰基,且 B係選自下列組成之組群:氫與齒素, C係選自下列組成之組群: ⑴氫, (2)鹵素, ⑶Q -C5烧基’視情況被i_3個函素取代, ® (4) ci -C5烷氧基,視情況被1-3個鹵素取代’及 (5) 氰基, D係選自下列組成之組群: (1) 氫, (2) 鹵素, ⑶Q -C5烧基’視情況被1-3個鹵素取代, (4) Q-Cs烷氧基,視情況被1_3個鹵素取代, 143482-2 -18- 201111364 (5) (C! -C5 伸烷基)-0-(CH2 )〇 _ 2 -CH3,視情況被 1-3 個 鹵素取代,及 (6) 氰基,且 E係選自下列組成之組群: ⑴氫, (2) 鹵素, (3) CVq烷基, (4) CVQ烯基,Wherein: A is selected from the group consisting of: (1) hydrogen, (2) _ 素, ( (3) Q-C5 alkyl, optionally replaced by i_3 i, (4) Q-C5 Optionally, 1-3 halogens are substituted for 'and (5) cyano groups, and B is selected from the group consisting of hydrogen and dentate, and C is selected from the group consisting of: (1) hydrogen, (2) halogen , (3) Q-C5 alkyl group is replaced by i_3 elements, ® (4) ci -C5 alkoxy, optionally substituted by 1-3 halogens and (5) cyano, D is selected from the following composition Groups: (1) hydrogen, (2) halogen, (3) Q-C5 alkyl groups are optionally substituted by 1-3 halogens, (4) Q-Cs alkoxy groups, optionally replaced by 1_3 halogens, 143482- 2 -18- 201111364 (5) (C! -C5 alkyl)-0-(CH2)〇_ 2 -CH3, optionally substituted by 1-3 halogens, and (6) cyano, and E is selected From the following group: (1) hydrogen, (2) halogen, (3) CVq alkyl, (4) CVQ alkenyl, (5) CVC5烷氧基, (6) 氰基, (7) -(CVCs 伸烷基)-C(CF3)2(H), (8) -(C] -C5 伸烷基)-N(H)-C(=〇HCH2 )〇 _ 2 -CH3, (9) -(q -C5 伸烷基)-0-(CH2 )〇 - 2 -CH3, (10)(5) CVC5 alkoxy, (6) cyano, (7) - (CVCs alkyl)-C(CF3)2(H), (8) - (C) -C5 alkyl)-N ( H)-C(=〇HCH2 )〇_ 2 -CH3, (9) -(q -C5 alkyl)-0-(CH2 )〇-2 -CH3, (10) 143482-2 -19- 201111364 其中(3),(4),(5),(7),⑻及(9)係視情況被1-3個鹵素取代’且 其中(10),(11),(I2)及(13)係視情況被個取代基取代,取代 基獨立選自下列組成之組群:齒素、C〗-C5烷基' C丨-05烷 氧基及氰基, = 其”上可接受之9,或其立趙異構143482-2 -19- 201111364 where (3), (4), (5), (7), (8) and (9) are replaced by 1-3 halogens as appropriate [and (10), (11), (I2) and (13) are optionally substituted by a substituent which is independently selected from the group consisting of dentate, C-C5 alkyl 'C丨-05 alkoxy and cyano, = " Acceptable 9 or its stereoisomer 143482-2 201111364143482-2 201111364 表5 實例59 實例58 實例74Table 5 Example 59 Example 58 Example 74 實例57 實例56 實例71Example 57 Example 56 Example 71 實例51 實例69 實例70Example 51 Example 69 Example 70 實例53 實例52 實例62Example 53 Example 52 Example 62 143482-2 -21 - 201111364143482-2 -21 - 201111364 143482-2 22- 201111364 .... . . 表5 實例67 〇 實例72 CH3 〇 實例55 ch3 0 實例65 ch3 Vo H3V\ o 或 實例77 ch3143482-2 22- 201111364 .... . . Table 5 Example 67 〇 Example 72 CH3 实例 Example 55 ch3 0 Example 65 ch3 Vo H3V\ o or Example 77 ch3 或其立體異構物,或其藥學上可接受之鹽;或其立體異構 物之藥學上可接受鹽。 20.如請求項19之化合物,其係為Or a stereoisomer thereof, or a pharmaceutically acceptable salt thereof; or a pharmaceutically acceptable salt thereof, or a stereoisomer thereof. 20. The compound of claim 19, which is 實例68 ?H3Example 68 ?H3 或其藥學上可接受之鹽。 21.如請求項1之化合物,其中Y係選自下列組成之組群:Or a pharmaceutically acceptable salt thereof. 21. The compound of claim 1 wherein Y is selected from the group consisting of: 143482-2 •23- 201111364143482-2 •23- 201111364 視情況如請求項1中所述經單-、二-、三·、四-或五取代。 22.如請求項7之化合物,其係選自下列組成之組群:Substituting mono-, di-, tri-, tetra- or penta-substituted as described in claim 1. 22. The compound of claim 7, which is selected from the group consisting of: 其中A係選自下列組成之組群: ⑴氫, (2) 鹵素, (3) q -C5 烷基, (4) Ci -C5烧氧基’ (5) 氰基, 143482-2 -24- 201111364 (6) q-CV氰基, ⑺-(q -c5 伸烷基)-n(h)-c(=o)-(ch2 )0.2 -ch3, ⑻-(q -C5 伸烷基)-〇-(CH2 )0 - 2 -CH3,及 ⑼-NOiMCi -C5 伸烷基)-〇-(CH2 )〇. 2 -CH3, 其中⑶,(4),(6),⑺,⑻及⑼係視情況被1-3個鹵素取代; 或其立體異構物’或其藥學上可接受之鹽,或其立體異構 物之藥學上可接受鹽。 23.如°月求項1之化合物’其中化合物係選自下列:Wherein A is selected from the group consisting of: (1) hydrogen, (2) halogen, (3) q-C5 alkyl, (4) Ci-C5 alkoxy' (5) cyano, 143482-2 -24- 201111364 (6) q-CV cyano, (7)-(q-c5 alkyl)-n(h)-c(=o)-(ch2)0.2 -ch3, (8)-(q-C5 alkyl)- 〇-(CH2)0 - 2 -CH3, and (9)-NOiMCi -C5 alkylene)-〇-(CH2)〇. 2 -CH3, wherein (3), (4), (6), (7), (8) and (9) Substituted by 1-3 halogens; or a stereoisomer thereof' or a pharmaceutically acceptable salt thereof, or a pharmaceutically acceptable salt thereof, or a stereoisomer thereof. 23. The compound of claim 1 wherein the compound is selected from the group consisting of: 143482-2 -25· 201111364143482-2 -25· 201111364 實例18 實例21Example 18 Example 21 H3 實例26 實例37 實例23H3 Example 26 Example 37 Example 23 或其立體異構物,或其藥學上可接受之鹽,或其立體異構 物之藥學上可接受鹽。 24.如請求項23之化合物,其係為 實例26Or a stereoisomer thereof, or a pharmaceutically acceptable salt thereof, or a pharmaceutically acceptable salt thereof, or a stereoisomer thereof. 24. The compound of claim 23, which is exemplified by example 26 143482-2 -26- 201111364 或其藥學上可接受之鹽。 25.如請求項1之化合物,其中Y係143482-2 -26- 201111364 or a pharmaceutically acceptable salt thereof. 25. The compound of claim 1, wherein the Y system 視情況如請求項1中所述經單-或二取代。 26.如請求項7之化合物,其係為It is mono- or disubstituted as described in claim 1. 26. The compound of claim 7 which is 其中: A係選自下列組成之組群: (1)氫, ⑵鹵素, (3) q -C5 烷基, (4) CVC5烷氧基,及 • (5) -(C! -C5 伸烷基)-0-(CH2 )〇 _ 2 -CH3, 其中(3),⑷及⑸係視情況被1-3個鹵素取代, B係選自下列組成之組群: (1)氫, (2) 鹵素, (3) CVq烷基, ⑷ 烷氧基, (5) -(C! -C5 伸烷基)-0-(CH2 )〇 _ 2 -CH3,及 143482-2 -27- 201111364 ⑹-NOlMq -c5 伸烷基)-〇-(ch2 )〇 _ 2 -CH3, 其中(3),⑷,⑶及⑹係視情況被μ3個鹵素取代; 或其立體異構物,或其藥學上可接受之鹽,或其 立體異構物之藥學上可接受鹽。 27·如請求項1之化合物,其中化合物係為 實例2 ch3Wherein: A is selected from the group consisting of: (1) hydrogen, (2) halogen, (3) q-C5 alkyl, (4) CVC5 alkoxy, and (5) - (C! - C5 alkylene) Base)-0-(CH2)〇_ 2 -CH3, wherein (3), (4) and (5) are optionally substituted by 1-3 halogens, and B is selected from the group consisting of: (1) hydrogen, (2 Halogen, (3) CVq alkyl, (4) alkoxy, (5) -(C! -C5 alkyl)-0-(CH2)〇_ 2 -CH3, and 143482-2 -27- 201111364 (6)- NOlMq -c5 alkylene)-〇-(ch2)〇_ 2 -CH3, wherein (3), (4), (3) and (6) are optionally substituted by μ3 halogens; or a stereoisomer thereof, or a pharmaceutically acceptable substance thereof A salt acceptable, or a pharmaceutically acceptable salt thereof, of a stereoisomer thereof. 27. The compound of claim 1, wherein the compound is exemplified by example 2 ch3 實例79 ?h3Example 79 ?h3 或其藥學上可接受之鹽。 28. -種(3S,4R)-N-({3-漠基_4_曱基甲氧基)丙基]苯基}曱基)_ N衣丙基4-(1-曱基-2-酮基_ι,2·二氫_4_吡啶基)各六氫吡啶羧 酿胺鹽酸鹽之結晶形其藥學上可接受之水合物。 29. 如清求項28之結晶形式!,其係藉由! 3c ssnmr被特徵黎定 為具有以每百萬份之份數表示之下列化學位移:12〇1,312, 17.1’ 43.5, 41.6, 29.4, 58.5, 71.4, 28.7, 42 5, 138 3 及 143 6。 30·如明求項28之結晶形式工’其特徵為圖2之固態〗3c ssnmr CPMAS核磁共振光譜。 31. 如請求項28之結晶形式I, 32. 如請求項28之結晶形式工, 曲線。 其特徵為圖3之熱重分析曲線。 其特徵為圖4之示差掃描卡計法 33.如請求項28之結晶形式I, 其' 係藉由X-射線粉末繞射被特 143482-2 -28- 201111364 徵馨定為具有相應於d-間距之下列反射:1〇59, 7〇4, 4 24, 4.22, 3.88, 3.58, 3.51,3.31 及 3.08。 34·如請求項28之結晶形式丨,其特徵為圖5之又-射線繞射圖 樣。 35. —種製備下式化合物之方法:Or a pharmaceutically acceptable salt thereof. 28. -(3S,4R)-N-({3-Mosyl_4_fluorenylmethoxy)propyl]phenyl}indenyl)_N-propyl-4-(1-indolyl-2 - Keto group - i, 2, dihydro 4 - pyridyl) each of the hexahydropyridine carboxamide hydrochloride crystal form a pharmaceutically acceptable hydrate thereof. 29. For example, clear the crystal form of item 28! , it is by! 3c ssnmr is characterized by the following chemical shifts expressed in parts per million: 12〇1, 312, 17.1' 43.5, 41.6, 29.4, 58.5, 71.4, 28.7, 42 5, 138 3 and 143 6 . 30. The crystal form of the item 28 is characterized by the solid state of Figure 2, 3c ssnmr CPMAS nuclear magnetic resonance spectrum. 31. As in the crystalline form I of claim 28, 32. as in the crystalline form of claim 28, the curve. It is characterized by the thermogravimetric analysis curve of Figure 3. Characterized by the differential scanning card method of Figure 4, as in the crystalline form I of claim 28, which is characterized by X-ray powder diffraction by 143482-2 -28-201111364 - The following reflections of the spacing: 1〇59, 7〇4, 4 24, 4.22, 3.88, 3.58, 3.51, 3.31 and 3.08. 34. The crystalline form 请求 of claim 28, which is characterized by the re-radiation pattern of Figure 5. 35. A method for preparing a compound of the formula: 其中: R為視情況被1-3個鹵素取代之q _c2烷基, R2與R3係獨立選自下列組成之組群:氫、鹵素、Ci_C5 烷基、q -C5烷氧基及_0_(Ci _c5伸烷基)〇_(CH2 )〇 · 3 _Ch3,其 中烷基、烷氧基及_C5伸烷基)_〇 (CH2 _ 3 _CH3係視情況 被1-3個取代基取代,取代基獨立選自下列組成之組群: 齒素、視情況被1-3個鹵素取代之Cl -c5烷基及視情況被1-3 個鹵素取代之烷氧基, X係選自下列組成之組群:氫、-OH及q -C5烷氧基, (Z)n 1為-C2伸烧基, A係選自下列組成之組群: ⑴氫, (2) _ 素, ⑶Q -C5烷基, 143482-2 -29- 201111364 (4) (VC5烷氧基,及 (5) -S-(CH2 )〇 - 3 -CH3, 其中(3)與(4)係視情況被1-3個函素取代, B係選自下列組成之組群: ⑴氫, (2)鹵素, ⑶ C! -C5烧基, ⑷ eves烷氧基, (5) -OH, ⑹-CF3, (7) -C(=0)-CH3 &gt; ⑻-CMC! -C5 伸烷基)-〇-(CH2 )〇. 2 -CH3, (9) -(q -C5 伸烷基)-〇-(CH2 )〇. 2 -CH3, (10) -O-CCi -C5 伸烷基)-C(CH3 )2 -C(=0)0H, (11) -CKQ-Q伸烷基)-c(ch3)2-c(=o)och3, 其中(3),(4),(8),⑼及(11)係視情況被1-3個鹵素取 代, C係選自下列組成之組群: ⑴氫, (2) q-Cs烷基,視情況被1-3個鹵素取代,及 (3) q -C5烷氧基,視情況被1-3個鹵素取代,且 D係選自下列組成之組群: ⑴氫, (2)鹵素, 143482-2 -30- 201111364 (3) Q -C5 烷基, (4) (VC5烷氧基, (5) CVQ-氰基, (6) C2 -C5 伸烯基-〇-(CH2 )〇 - 2 -CH3, (7) -(q -C5 伸烷基)-N(H)-C(=0)-0-(CH2 )〇. 2 -CH3, (8) -(q -C5 伸烷基)-N(H)-C(=0)-(CH2 )〇 - 2 -CH3, (9) -(Ci -C5 伸烷基)-0-CHF2, (10) -(Ci -C5 伸烷基)-0-(CH2 )〇 - 2 -CH3,Wherein: R is a q _c2 alkyl group optionally substituted by 1-3 halogens, and R 2 and R 3 are independently selected from the group consisting of hydrogen, halogen, Ci_C5 alkyl, q-C5 alkoxy and _0_( Ci _c5 alkylene) 〇_(CH2 ) 〇 · 3 _Ch3, wherein alkyl, alkoxy and _C5 alkyl) 〇 (CH2 _ 3 _CH3 is optionally substituted by 1-3 substituents The group is independently selected from the group consisting of dentate, a Cl-c5 alkyl group optionally substituted by 1-3 halogens, and an alkoxy group optionally substituted by 1-3 halogens, and X is selected from the following constituents. Group: hydrogen, -OH and q-C5 alkoxy, (Z)n 1 is a -C2 alkyl group, and A is selected from the group consisting of: (1) hydrogen, (2) _, (3) Q-C5 alkane Base, 143482-2 -29- 201111364 (4) (VC5 alkoxy, and (5) -S-(CH2)〇-3 -CH3, where (3) and (4) are 1-3 depending on the situation Substituted by a letter, B is selected from the group consisting of: (1) hydrogen, (2) halogen, (3) C! -C5 alkyl, (4) eves alkoxy, (5) -OH, (6)-CF3, (7) - C(=0)-CH3 &gt; (8)-CMC! -C5 alkylene)-〇-(CH2)〇. 2 -CH3, (9) -(q -C5 alkylene)-〇-(CH2 ) -. 2 -CH3, (10) -O-CCi -C5 alkylene)-C(CH3)2 -C(=0)0H, (11) -CKQ-Qalkylene)-c(ch3)2 -c(=o)och3, wherein (3), (4), (8), (9) and (11) are replaced by 1-3 halogens, and C is selected from the group consisting of: (1) hydrogen, (2) a q-Cs alkyl group, optionally substituted by 1 to 3 halogens, and (3) a q-C5 alkoxy group, optionally substituted by 1 to 3 halogens, and D is selected from the group consisting of the following : (1) hydrogen, (2) halogen, 143482-2 -30- 201111364 (3) Q-C5 alkyl, (4) (VC5 alkoxy, (5) CVQ-cyano, (6) C2 - C5 〇-〇-(CH2 )〇-2 -CH3, (7) -(q -C5 alkyl)-N(H)-C(=0)-0-(CH2 )〇. 2 -CH3, (8 -(q -C5 alkylene)-N(H)-C(=0)-(CH2)〇- 2 -CH3, (9) -(Ci -C5 alkylene)-0-CHF2, (10 ) -(Ci -C5 alkylene)-0-(CH2 )〇-2 -CH3, (11) -CKCi -C5 伸烷基)-0-(CH2 )〇 - 2 -ch3, (12) -(A-C5 伸烷基)-OH, (13) -S-CCVCs 伸烷基)-OH, (14) -SCF3,及 (15) -NCHMCi -C5 伸烷基)-0-(CH2 )0 2 -CH3, 其中(3),(4),(5),(6),(7),(8),(9), (l〇), (11), (12),(13)及 (15)係視情況被1-3個鹵素取代, 其係包括下列步驟: (1)使式⑻化合物或其鹽於溶劑存在下偶合至式(b) 化合物或其鹽:(11) -CKCi -C5 alkylene)-0-(CH2)〇-2 -ch3, (12) -(A-C5alkylene)-OH, (13) -S-CCVCs alkylene)- OH, (14) -SCF3, and (15) -NCHMCi -C5 alkylene)-0-(CH2)0 2 -CH3, wherein (3), (4), (5), (6), (7 ), (8), (9), (l〇), (11), (12), (13) and (15) are replaced by 1-3 halogens, which include the following steps: (1) The compound of the formula (8) or a salt thereof is coupled to the compound of the formula (b) or a salt thereof in the presence of a solvent: ⑷ 以形成式(c)化合物或其鹽 143482-2 •31 201111364(4) to form a compound of the formula (c) or a salt thereof 143482-2 • 31 201111364 ⑵藉由移除Boc使化合物(c)去除保護。 36. 如請求項35之方法,其中溶劑為一或多種化合物,選自下 列組成之組群:DMF、氣化草酿及iPr2Net。 37. 如請求項35之方法,其中步驟⑺係以一或多種化合物進行 ,該化合物選自下列組成之組群:HC1、IPA及MTBE。 38. —種製備下式化合物之方法:(2) The compound (c) is deprotected by removing Boc. 36. The method of claim 35, wherein the solvent is one or more compounds selected from the group consisting of DMF, gasification, and iPr2Net. 37. The method of claim 35, wherein step (7) is carried out with one or more compounds selected from the group consisting of HC1, IPA, and MTBE. 38. A method for preparing a compound of the formula: 其係包括下列步驟: 於 (1)使具有Boc基團之式⑻化合物與下文式⑼ DMF、氣化草醯及iPr2NEt存在下偶合:The method comprises the steps of: (1) coupling a compound of the formula (8) having a Boc group with the following formula (9) DMF, gasified grasshopper and iPr2NEt: .0 .Br ,co2h Α V 、Me MsOH ' 、〇Me ⑻ (b) 以形成式(c)化合物 143482-2 -32- 201111364.0 .Br , co2h Α V , Me MsOH ' , 〇Me (8) (b) to form a compound of formula (c) 143482-2 -32- 201111364 (2)使所形成之化合物經過B〇c基團之移除,於hcl、 IPA及MTBE存在下去除保護。 • 39. 40.(2) The formed compound is removed by the B〇c group, and the protection is removed in the presence of hcl, IPA and MTBE. • 39. 40. 41. 一種醫藥組合物,纟包含有效量之如請求項1之化合物或 其藥學上可接受之鹽及藥學上可接受之载劑。 一種如晴求項1之化合物於藥劑製造上之用途該藥劑係 用於治療或預防疾病,其係關於高血壓、鬱血性心衰竭、 肺高血壓、腎機能不全、腎絕血、腎衰竭、腎纖維變性、 。臟機此不全、心臟肥大、心臟纖維變性、心肌絕血、心 肌病、絲球體性腎炎、腎絞痛,由於糖尿病所造成之併發 症,譬如腎病、脈管病及神經病,青光眼、高眼球内壓力、 動脈粥瘤硬化、血管造形術後之再狹窄、在血管或心臟手 術後之併發症、勃起機能障礙、醛固酶過多症、肺纖維變 性、硬皮病、焦慮、認知病症、以免疫壓抑劑治療之併發 症及其他已知與腎素-血管收縮素系統有關聯之疾病。 一種治療或預防疾病之方法,該疾病係關於高血壓、鬱血 性心衰竭 '肺高血壓、腎機能不全、腎絕血、腎衰竭、腎 纖維變性、心臟機能不全、心臟肥大、心臟纖維變性、心 肌絕血、心肌病、絲球體性腎炎、腎絞痛,由於糖尿病所 143482-2 -33- 201111364 造成之併發症’譬如腎病、脈管病及神經病,青光眼、高 眼球内壓力、動脈粥瘤硬化、血管造形術後之再狹窄、在 血管或心臟手術後之併發症、勃起機能障礙、酿固酶過多 症、肺纖維變性、硬皮病、焦慮、認知病症、以免疫壓抑 劑治療之併發症及其他已知與腎素_血管收縮素系統有關 聯之疾病’此方法包括對病患投予醫藥活性量之如請求項 1之化合物。41. A pharmaceutical composition comprising an effective amount of a compound of claim 1 or a pharmaceutically acceptable salt thereof, and a pharmaceutically acceptable carrier. Use of a compound according to claim 1 for the manufacture of a medicament for the treatment or prevention of diseases relating to hypertension, septic heart failure, pulmonary hypertension, renal insufficiency, renal ischemia, renal failure, Renal fibrosis, Dirty insufficiency, cardiac hypertrophy, cardiac fibrosis, myocardial ischemia, cardiomyopathy, spheroid nephritis, renal colic, complications caused by diabetes, such as kidney disease, vascular disease and neuropathy, glaucoma, high eyeball Stress, atherosclerosis, restenosis after angioplasty, complications after vascular or cardiac surgery, erectile dysfunction, hyperaldase, pulmonary fibrosis, scleroderma, anxiety, cognitive disorders, immunity Complications of inhibitor treatment and other diseases known to be associated with the renin-angiotensin system. A method for treating or preventing a disease, which is related to hypertension, septic heart failure, pulmonary hypertension, renal insufficiency, renal blood loss, renal failure, renal fibrosis, cardiac insufficiency, cardiac hypertrophy, cardiac fibrosis, Myocardial hematopoiesis, cardiomyopathy, spheroid nephritis, renal colic, complications caused by diabetes 143482-2 -33- 201111364 'such as nephropathy, vascular disease and neuropathy, glaucoma, high intraocular pressure, atheroma Sclerotherapy, restenosis after angioplasty, complications after vascular or cardiac surgery, erectile dysfunction, hyperactivity of fecal enzymes, pulmonary fibrosis, scleroderma, anxiety, cognitive disorders, concurrent treatment with immunosuppressive agents And other diseases known to be associated with the renin-angiotensin system. This method comprises administering to a patient a pharmaceutically active amount of a compound of claim 1. 143482-2 -34-143482-2 -34-
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