DK154553B - METHOD OF ANALOGUE FOR THE PREPARATION OF ETHER OR THIOETHERMERCAPTOACYL PROLINES - Google Patents
METHOD OF ANALOGUE FOR THE PREPARATION OF ETHER OR THIOETHERMERCAPTOACYL PROLINES Download PDFInfo
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- C07D207/02—Heterocyclic compounds containing five-membered rings not condensed with other rings, with one nitrogen atom as the only ring hetero atom with only hydrogen or carbon atoms directly attached to the ring nitrogen atom
- C07D207/04—Heterocyclic compounds containing five-membered rings not condensed with other rings, with one nitrogen atom as the only ring hetero atom with only hydrogen or carbon atoms directly attached to the ring nitrogen atom having no double bonds between ring members or between ring members and non-ring members
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- C07D207/18—Heterocyclic compounds containing five-membered rings not condensed with other rings, with one nitrogen atom as the only ring hetero atom with only hydrogen or carbon atoms directly attached to the ring nitrogen atom having one double bond between ring members or between a ring member and a non-ring member
- C07D207/22—Heterocyclic compounds containing five-membered rings not condensed with other rings, with one nitrogen atom as the only ring hetero atom with only hydrogen or carbon atoms directly attached to the ring nitrogen atom having one double bond between ring members or between a ring member and a non-ring member with hetero atoms or with carbon atoms having three bonds to hetero atoms with at the most one bond to halogen, e.g. ester or nitrile radicals, directly attached to ring carbon atoms
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- C07D207/04—Heterocyclic compounds containing five-membered rings not condensed with other rings, with one nitrogen atom as the only ring hetero atom with only hydrogen or carbon atoms directly attached to the ring nitrogen atom having no double bonds between ring members or between ring members and non-ring members
- C07D207/10—Heterocyclic compounds containing five-membered rings not condensed with other rings, with one nitrogen atom as the only ring hetero atom with only hydrogen or carbon atoms directly attached to the ring nitrogen atom having no double bonds between ring members or between ring members and non-ring members with hetero atoms or with carbon atoms having three bonds to hetero atoms with at the most one bond to halogen, e.g. ester or nitrile radicals, directly attached to ring carbon atoms
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Description
iin
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oisland
Den foreliggende opfindelse angår en analogifremgangsmåde til fremstilling af hidtil ukendte ether- og thio-ethermercaptoacylproliner med formlen X-lf 5 R2 HC/t>( I 2| 2 1The present invention relates to an analogous process for the preparation of novel ether and thio-ether mercaptoacyl prolines of the formula X-If 5 R 2 HC / t> (I 2 | 2 1
R4- S- CH 2- CH — CO-*N-c — COORR4- S- CH 2- CH - CO- * N-c - COOR
HH
hvori X-R -gruppen er anbragt i prolinringens 3- eller 4-10 -stilling, X er oxygen eller svovl, R er hydrogen eller alkyl, R"*" er C^_^ alkyl eller phenyl, eventuelt substitueret med et halogenatom eller en methyl- eller methoxygrup-pe, R er hydrogen eller C^_^ alkyl, og R^"er' hydrogen, C^_^ alkanoyl eller benzoyl, eller salte heraf.wherein the XR group is positioned in the 3 or 4-10 position of the proline ring, X is oxygen or sulfur, R is hydrogen or alkyl, R "*" is C 1-6 alkyl or phenyl, optionally substituted with a halogen atom or a methyl or methoxy group, R is hydrogen or C 1-6 alkyl and R 4 is hydrogen, C 1-6 alkanoyl or benzoyl, or salts thereof.
15 De ved fremgangsmåden ifølge opfindelsen fremstil lede ether- og thioethermercaptoacylproliner med ovenstående formel I er nyttige anti-hypertensive midler.The ether and thioether mercaptoacyl prolines of the formula I prepared by the process of the invention are useful anti-hypertensive agents.
Fra tysk offentliggørelsesskrift nr. 2.703.828 kendes beslægtede forbindelser med samme type aktivitet, nemlig 20 hypotensiv virkning. Disse kendte forbindelsers struktur adskiller sig fra ovennævnte formel I, idet de ikke udviser substituent gruppen XR^, men i stedet er enten usubstituerede (dvs. har hydrogen) eller bærer en hydroxy- eller alkylgruppe. Den mest bemærkelsesværdige blandt disse kendte forbindelser 25 er den usubstituerede, der forhandles kommercielt under navnet "Captopril", og som har strukturen ?h3 IsFrom German Publication No. 2,703,828, related compounds of the same type of activity are known, namely 20 hypotensive effects. The structure of these known compounds differs from the above Formula I in that they do not exhibit the substituent group XR 2 but instead are either unsubstituted (i.e., have hydrogen) or carry a hydroxy or alkyl group. The most notable of these known compounds 25 is the unsubstituted, commercially sold under the name "Captopril" and having the structure?
HS-CH,-CH-C0-N_I-COOHHS-CH, -CH-C 0 -C-COOH N_I
30 1-(3-mercaptopropanoyl)-D-prolin ("Captopril") kendt fra DE 2.703.8281- (3-mercaptopropanoyl) -D-proline ("Captopril") known from DE 2,703,828
Denne forbindelse er i nedenstående sammenlignings-forsøg (jfr. "Biologisk afprøvning") afprøvet sammen med den 35 ifølge nedenstående eksempel 13 fremstillede tilsvarende 4- 2This compound has been tested in the following comparative experiments (cf. "Biological test") together with the corresponding 4- (2) prepared according to Example 13 below.
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o phenylthioforbindelse med formlen ?H3o phenylthio compound of formula? H3
5 HS-CH2“CH-CO-N__COOHHS-CH2 “CH-CO-N__COOH
1-(D-3-mercapto-2-methyl-l-oxopropyl)-cis.-4-phenyl -thio-L-prolin, hvor sidstnævnte forbindelse udviser et højere aktivitetsni-10 veau.1- (D-3-mercapto-2-methyl-1-oxopropyl) -cis.-4-phenyl-thio-L-proline, the latter compound exhibiting a higher activity level.
alkanoylgrupper er acylgrupper i fedtsyrer som f.eks. acetyl, propionyl, butyryl og isobutyryl, hvoraf acetyl er særlig foretrukket.alkanoyl groups are acyl groups in fatty acids such as e.g. acetyl, propionyl, butyryl and isobutyryl, of which acetyl is particularly preferred.
Produkterne med formlen I forekommer i stereoisome-15 re former eller som racemiske blandinger deraf. Alle disse kan fremstilles ved fremgangsmåden ifølge opfindelsen. Den nedenfor beskrevne syntese kan benytte racematet eller en af enantiomererne som udgangsmateriale. Når der til syntesen anvendes det racemiske udgangsmateriale, kan de stereoisomere, 20 der fås i slutproduktet, adskilles ved gængse chromatografiske eller fraktionelle krystallisationsmetoder. X-R"*"-gruppen kan også give anledning til cis-trans-isomeri.The products of formula I occur in stereoisomeric forms or as racemic mixtures thereof. All of these can be prepared by the process of the invention. The synthesis described below may use the racemate or one of the enantiomers as starting material. When the racemic starting material is used for the synthesis, the stereoisomers obtained in the final product can be separated by conventional chromatographic or fractional crystallization methods. The X-R "*" group may also give rise to cis-trans isomerism.
Fortrinsvis er det asymmetriske center ved C2 i prolinringen i L-konfiguration, og hvis der er et asymmetrisk 25 center i mercaptoacylsidekæden, er det i D-konfiguration.Preferably, the asymmetric center at C2 in the proline ring is in L configuration, and if there is an asymmetric center in the mercaptoacyl side chain, it is in D configuration.
Særlig foretrukne blandt ovenstående forbindelser er sådanne med formlen I, hvor X er oxygen, R^ er methyl eller 2 ethyl, især methyl, R er hydrogen eller methyl, især methyl, 4 1 R er hydrogen, og XR -gruppen er i 4-stillingen i prolinrin-30 gen, især når -XR^-gruppen er i cis-konfiguration.Particularly preferred among the above compounds are those of Formula I wherein X is oxygen, R 1 is methyl or 2 ethyl, especially methyl, R is hydrogen or methyl, especially methyl, 4 1 R is hydrogen and the XR group is in the position in the prolinrin gene, especially when the -XRR group is in cis configuration.
Etherne og thioetherne med formlen I fås ved fremgangsmåden ifølge opfindelsen, som er ejendommelig ved, at en prolinforbindelse med formlen 35The ethers and thioethers of formula I are obtained by the process of the invention, which is characterized in that a proline compound of formula 35
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33
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r<r <
HN__COORHN__COOR
5 hvori R, R1 og X har den ovenfor anførte betydning, kobles med en syre med formlen R25 wherein R, R1 and X are as defined above are coupled with an acid of formula R2
r,4-s-ch2-ch-cooh IIIr, 4-s-ch2-ch-cooh III
10 2 4 hvori R er som ovenfor anført, R' er alkanoyl eller benzoyl, eller et funktionelt derivat deraf, til dannelse af 4 et produkt, hvori R er C^_4 alkanoyl eller benzoyl, og at produktet om ønsket hydrolyseres til dannelse af et produkt, 4 12 15 hvori R er hydrogen, og R, R , R og X er som ovenfor anført, hvorpå en eventuelt dannet syre om ønsket overføres i et salt deraf.Wherein R is as above, R 'is alkanoyl or benzoyl, or a functional derivative thereof, to form 4 a product wherein R is C 1-4 alkanoyl or benzoyl and, if desired, the product is hydrolyzed to form a product, 4 12 15 wherein R is hydrogen and R, R, R and X are as indicated above, whereupon an optionally formed acid is, if desired, transferred into a salt thereof.
Denne reaktion kan udføres i nærværelse af et koblingsmiddel såsom dicyclohexylcarbodiimid eller lignende, el-20 ler syren kan aktiveres ved dannelse af de blandet anhydrid, symmetrisk anhydrid, syrehalogenid, aktiv ester eller anvendelse af Woodward-reagens K, N-ethoxycarbonyl-2-ethoxy-l,2-di-hydroquinolin eller, lignende. Med hensyn til acetyleringsme-toder henvises til Methoden der Organischen Chemie (Houben-25 -Weyl), bd. XV, del II, side 1 ff. (1974). Fortrinsvis omsættes syrehalogenidet, især syrechloridet, med formlen III med syren med formlen II.This reaction may be carried out in the presence of a coupling agent such as dicyclohexylcarbodiimide or the like, or the acid may be activated by forming the mixed anhydride, symmetric anhydride, acid halide, active ester or use of Woodward reagent K, N-ethoxycarbonyl-2-ethoxy. -1,2-dihydroquinoline or the like. Regarding acetylation methods, see the Methods der Organischen Chemie (Houben-25-Weyl), vol. XV, Part II, page 1 et seq. (1974). Preferably, the acid halide, especially the acid chloride, of formula III is reacted with the acid of formula II.
Esterforbindelserne (formel I hvori R er alkyl) kan omdannes til den frie syre (dvs. R er hydrogen) på gængs måde.The ester compounds (formula I wherein R is alkyl) can be converted to the free acid (i.e., R is hydrogen) by conventional means.
30 Hvis f.eks. R er t-butyl, giver behandling med trifluoreddi-kesyre og anisol den frie syre.For example, if R is t-butyl, treatment with trifluoroacetic acid and anisole gives the free acid.
Produktet med formlen I isoleres fortrinsvis og renses ved krystallisation, f.eks. ved at danne dicyclohexylamin-saltet og derefter omdanne saltet til den frie syreform ved be-35 handling med en vandig opløsning af en syre såsom surt kaliumsulfat.The product of formula I is preferably isolated and purified by crystallization, e.g. by forming the dicyclohexylamine salt and then converting the salt to the free acid form by treatment with an aqueous solution of an acid such as acidic potassium sulfate.
4 44 4
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Produkter med formlen I, hvori R er alkanoyl, eller benzoyl, kan omdannes til produkter med formlen I, hvor 4 R er hydrogen, ved gængs hydrolyse eller ammonolyse.Products of formula I wherein R is alkanoyl or benzoyl may be converted to products of formula I wherein 4 R is hydrogen by conventional hydrolysis or ammonolysis.
Esterne med formlen I, hvor R er C1-4 alkyl, kan 5 fås ud fra carboxylsyreforbindelserne, dvs. hvor R er hydrogen, ved gængse esterificeringsmetoder, f.eks. ved esterifi-cering med en diazoalkan såsom diazomethan, 1-alkyl-3-p-to-lyltriazin såsom l-n-butyl-3-p-tolyltriazen eller lignende.The esters of formula I wherein R is C 1-4 alkyl can be obtained from the carboxylic acid compounds, i.e. wherein R is hydrogen, by conventional esterification methods, e.g. by esterification with a diazoalkane such as diazomethane, 1-alkyl-3-p-tolyltriazine such as 1-n-butyl-3-p-tolyltriazine or the like.
Prolinreaktanterne med formlen II kan fremstilles 10 på forskellig måde. F.eks. kan et hydroxy- eller mercapto-prolin med formlenThe proline reactants of formula II can be prepared in various ways. Eg. can be a hydroxy or mercapto-proline of the formula
XHXH
"Ή"Ή
HN—>— C-COOHHN -> - C-COOH
15 |15 |
HH
acetyleres med et acetyleringsmiddel såsom eddikesyreanhy-drid, acetylchlorid, propionsyreanhydrid, smørsyreanhydrid, 20 benzylchlorformiat eller lignende for at beskytte nitrogenet. R^-gruppen indføres derefter ved at omsætte den N-beskyttede form for forbindelsen med formlen 17med et halogenid, R^-hal, hvor hal er et halogen, fortrinsvis iod, i nærværelse af sølvoxid, natriumhydrid, natriumhydroxid eller lignende, hvorved 25 der fås et mellemproduktet med formlen beskyttet-N-C-COOR1 30 'is acetylated with an acetylating agent such as acetic anhydride, acetyl chloride, propionic anhydride, butyric anhydride, benzyl chloroformate or the like to protect the nitrogen. The R 2 group is then introduced by reacting the N-protected form of the compound of formula 17 with a halide, R 2 hal, where hal is a halogen, preferably iodine, in the presence of silver oxide, sodium hydride, sodium hydroxide or the like, whereby is obtained an intermediate of the formula protected-NC-COOR1 30 '
HH
Alkalisk hydrolyse af mellemproduktet ined formlen V med en base såsom bariumhydroxid, natriumhydroxid, kaliumhydroxid eller lignende giver den frie syre (COOH) og derefter hydro-35 lyse med en mineralsyre såsom svovlsyre giver udgangsmaterialet med formlen II.Alkaline hydrolysis of the intermediate of formula V with a base such as barium hydroxide, sodium hydroxide, potassium hydroxide or the like gives the free acid (COOH) and then hydrolysis with a mineral acid such as sulfuric acid gives the starting material of formula II.
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55
En anden fremgangsmåde til fremstilling af prolin-reaktanterne med formlen II er at behandle den N-beskyttede tosyloxyprolinester, fortrinsvis methylesteren med formlen 5Another method of preparing the proline reactants of formula II is to treat the N-protected tosyloxyproline ester, preferably the methyl ester of formula 5
beskyttet-N-C-COOalkyl VIprotected-N-C-COOalkyl VI
10 I10 I
HH
med et natriumsalt med formlenwith a sodium salt of the formula
R1-X-Na VIIR1-X-Na VII
15 hvilket giver mellemproduktet med formlen15 to give the intermediate of formula
2o Η2ί^><Γ VIII2o Η2ί ^> <Γ VIII
beskyttet-N-(jl-COOalkylprotected-N- (l-COOalkyl
HH
I formlen VI er symbolet Ts -S02“ ^-CH^, og den N-beskyt- 25 tende gruppe er benzyloxycarbony1, der er foretrukket, eller andre almindeligt benyttede acylbeskyttende grupper. Dersom tosylatgruppen er i cis-konfiguration, vil XR^-gruppen ved denne reaktion være i trans-konfiguration, og hvis tosyloxy- gruppen er i trans-konfiguration,vil XR^gruppen være i cis-30 -konfiguration. Mellemproduktet med formlen VIII omsættes derefter for at fjerne alkylestergruppen og omsættes derefter med hydrogenbromid, hvilket giver HBr-saltet af prolinreak-tanten med formlen II, der derefter kan kobles med syren, fortrinsvis syrechloridet, med formlen III.In the formula VI, the symbol Ts is -SO 2 + 3 -CH 2, and the N-protecting group is preferred benzyloxycarbonyl or other commonly used acyl protecting groups. If the tosylate group is in cis configuration, the XR 2 group in this reaction will be in the trans configuration, and if the tosyloxy group is in the trans configuration, the XR 2 group will be in the cis 30 configuration. The intermediate of formula VIII is then reacted to remove the alkyl ester group and then reacted with hydrogen bromide to give the HBr salt of the proline reactant of formula II which can then be coupled with the acid, preferably the acid chloride, of formula III.
35 635 6
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proiinudgangsmaterialerne med formlen II, hvor X er svovl, og XR^-gruppen er knyttet til prolinets 3-stil-ling, kan også fås ved at behandle en 1,2-dehydroprolinester, fortrinsvis t-butylesteren, med formlen 5the proin starting materials of formula II wherein X is sulfur and the XR 2 group attached to the 3-position of the proline can also be obtained by treating a 1,2-dehydroproline ester, preferably the t-butyl ester, of formula 5
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N ~==-i— COOalkyl med et acyleringsmiddel såsom benzylchlorformiat, acetylchlo-10 rid etc., hvilket giver 4,5-dehydroforbindelsen Γ'TiN ~ == - COOalkyl with an acylating agent such as benzyl chloroformate, acetyl chloride, etc. to give the 4,5-dehydro compound Γ'Ti
beskyttet N-COOalkyl Xprotected N-COOalkyl X
15 som derefter omsættes med mercaptanen R^-SH, hvilket giver rf*15 which is then reacted with the mercaptan R 2 -SH to give rf *
beskyttet N--COOalkyl XIprotected N - COOalkyl XI
20 hvor -S-R^-substituenten er i transkonfiguration. De N-be-skyttende og alkylgrupperne fjernes derefter, hvorved fås det ønskede udgangsmateriale.Wherein the -S-R 2 substituent is in trans-configuration. The N-protecting and alkyl groups are then removed to give the desired starting material.
Prolinudgangsmaterialerne med formlen II, hvor R"*" 25 er phenyl, substitueret phenyl, phenyl-lavere alkylen eller substitueret phenyl-lavere alkylen, kan ligeledes fås ved at behandle benzylesteren af det N-beskyttede prolin med formlen IV med alkoholen R-OH i nærværelse af triphenylphosphin og diethylazodicarboxylat ifølge den metode, der er beskrevet 30 af Bittner m.fl. i Chemistry and Industry, 15. marts 1975, side 281. Fjernelse af den N-beskyttende gruppe og benzyl-estergruppen giver udgangsmaterialet med formlen II.The proline starting materials of formula II, wherein R "+" is phenyl, substituted phenyl, phenyl-lower alkylene or substituted phenyl-lower alkylene, can also be obtained by treating the benzyl ester of the N-protected proline of formula IV with the alcohol R-OH in presence of triphenylphosphine and diethyl azodicarboxylate according to the method described by Bittner et al. in Chemistry and Industry, March 15, 1975, page 281. Removal of the N-protecting group and the benzyl ester group gives the starting material of formula II.
Der henvises ligeledes til de følgende publikationer med hensyn til yderligere oplysning vedrørende fremstil-35 ling af udgangsmaterialer og mellemprodukter: USA patentskrifterne nr. 4.046.889, 4,105.776 og 4.145.935, Neuberger, J.Reference is also made to the following publications for further information regarding the preparation of starting materials and intermediates: United States Patent Nos. 4,046,889, 4,105,776 and 4,145,935 to Neuberger, J.
Chem. Soc., 1945, side 429-432, Patchett m.fl., J. Amer. Chem.Chem. Soc., 1945, pages 429-432, Patchett et al., J. Amer. Chem.
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Soc. 79, side 185-192 (1957), Baer irt.fl., Can. J. Biochem. and Phys., 37, side 583-587 (1959), Sheenan m.fl., J. Amer.Soc. 79, pages 185-192 (1957), Baer et al., Can. J. Biochem. and Phys., 37, pp. 583-587 (1959), Sheenan et al., J. Amer.
Chem. Soc. 85, side 3863-3865 (1963), og Magerlein, J. Med.Chem. Soc. 85, pp. 3863-3865 (1963), and Magerlein, J. Med.
Chem. 10, side 1161-1163 (1967). De deri omtalte metoder 5 kan benyttes som almene metoder ved syntesen og stereoom-lejringen af forbindelser, der fremstilles ved fremgangsmåden ifølge opfindelsen.Chem. 10, pp. 1161-1163 (1967). The methods mentioned therein 5 can be used as general methods in the synthesis and stereo-storage of compounds prepared by the process of the invention.
Yderligere eksperimentelle detaljer er omtalt i eksemplerne, der er foretrukne udførelsesformer og også kan 10 tjene som modeller til fremstillingen af andre forbindelser inden for gruppen.Further experimental details are discussed in the examples which are preferred embodiments and also may serve as models for the preparation of other compounds within the group.
Forbindelserne, der fremstilles ved fremgangsmåden ifølge opfindelsen, danner basiske salt med forskellige uorganiske og organiske baser. Det saltdannende ion, der stam-15 mer fra sådanne baser, kan være metalioner, f.eks. aluminium-, alkalimetalioner, såsom natrium eller kalium, jordalkalime-talioner såsom calcium eller magnesium, eller et aminsaltion, hvoraf et antal er kendt til dette formål, f.eks. aralkylami-ner såsom dibenzylamin, Ν,Ν-dibenzylethylendiamin, lavere al-20 kylaminer såsom methylamin, t-butylamin, procain, lavere alky lpiperidiner såsom N-ethylpiperidin, cycloalkylaminer såsom cyclohexylamin eller dicyclohexylamin, 1-adamantanamin, benzathin eller salte af aminosyrer såsom arginin, lysin o. lign. De fysiologisk acceptable salte såsom natrium- eller 25 kaliumsalte, kan anvendes medicinsk som beskrevet nedenfor og er fortrukket. Disse og andre salte, der ikke nødvendigvis er fysiologisk acceptable, er anvendelige til isolering eller rensning af et produkt, der er acceptabelt til de nedenfor beskrevne formål som belyst med dicyclohexylaminsaltet og 30 cyclohexylaminsaltet i eksemplerne. Saltene fremstilles ved at omsætte forbindelsens syreform med 1 ækvivalent af basen, der giver den ønskede basiske ion, i et middel, hvor saltet udfældes, eller i vandigt medium og derefter lyofilisere.The compounds prepared by the process of the invention form basic salts with various inorganic and organic bases. The salt-forming ion derived from such bases may be metal ions, e.g. aluminum, alkali metal ions such as sodium or potassium, alkaline earth metal ions such as calcium or magnesium, or an amine salt, a number of which are known for this purpose, e.g. aralkylamines such as dibenzylamine, Ν, Ν-dibenzylethylenediamine, lower alkylamines such as methylamine, t-butylamine, procaine, lower alkylpiperidines such as N-ethylpiperidine, cycloalkylamines such as cyclohexylamine or dicyclohexylamine, 1-adamantinamine, arginine, lysine and the like. The physiologically acceptable salts such as sodium or potassium salts can be used medically as described below and are preferred. These and other salts, which are not necessarily physiologically acceptable, are useful for isolating or purifying a product acceptable for the purposes described below as illustrated by the dicyclohexylamine salt and the cyclohexylamine salt of the Examples. The salts are prepared by reacting the acid form of the compound with 1 equivalent of the base giving the desired basic ion, in a salt precipitating agent, or in aqueous medium and then lyophilizing.
Den frie syreform kan fås af saltet ved konventionel neutra-35 liseringsteknik, f.eks. med kaliumbisulfat, saltsyre etc.The free acid form can be obtained from the salt by conventional neutralization technique, e.g. with potassium bisulfate, hydrochloric acid etc.
Forbindelserne, der fremstilles ved fremgangsmåden ifølge opfindelsen, inhiberer omdannelsen af decapeptidet an- 8The compounds prepared by the method of the invention inhibit the conversion of the decapeptide by
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giotensin I til angiotensin II og er derfor nyttige til nedsættelse eller helbredelse af hypertension. Forbindelserne, der fremstilles ved fremgangsmåden ifølge opfindelsen, griber ind i rækkefølgen renin —^ angiotensinogen —^ 5 angiotensin I —> angiotensin II ved at inhibere det angio-tensinomdannende enzym og reducere eller eliminere dannelsen af pressorstoffet angiotensin II. Når man således indgiver en hypotensivt effektiv mængde af et præparat indeholdende en eller en kombination af forbindelser med formlen I eller 10 et fysiologisk acceptabelt salt deraf, formindskes eller helbredes hypertension hos pattedyrarter, der lider heraf.giotensin I to angiotensin II and are therefore useful in reducing or curing hypertension. The compounds prepared by the process of the invention interfere with the order of renin - angiotensinogen - angiotensin I -> angiotensin II by inhibiting the angiotensin converting enzyme and reducing or eliminating the formation of the angiotensin II pressor substance. Thus, when a hypotensive effective amount of a composition containing one or a combination of compounds of formula I or 10 is administered a physiologically acceptable salt thereof, hypertension in mammalian species suffering from it is reduced or cured.
En enkelt dosis eller fortrinsvis to-fire opdelte daglige doser på basis af ca. 0,1-ca. 100 mg/kg/dag, fortrinsvis ca. 1-ca. 50 mg/kg/dag, nedsættes blodtrykket som 15 anført i dyreforsøg beskrevet af S.L. Engel, T.R.· Schaeffer, M.H. Waugh og B. Rubin i Proc. Soc. Exp. Biol. Med. 143, 483 (1973). Stoffet indgives fortrinsvis oralt, men også parenterale indgivelsesveje såsom subcutant, intramuskulært, intravenøst eller intraperionealt kan anvendes.A single dose or preferably two to four divided daily doses on the basis of approx. 0.1-ca. 100 mg / kg / day, preferably approx. 1-C. 50 mg / kg / day, blood pressure is lowered as indicated in animal studies described by S.L. Engel, T.R. · Schaeffer, M.H. Waugh and B. Rubin in Proc. Soc. Exp. Biol. With. 143, 483 (1973). The drug is preferably administered orally, but also parenteral routes of administration such as subcutaneous, intramuscular, intravenous or intraperionally can be used.
20 Forbindelserne, der fremstilles ved fremgangsmåden ifølge opfindelsen, kan anvendes til opnåelse af en nedsættel-se af blodtryk ved at sammensættes til præparater dermed såsom tabletter, kapsler eller eliksirer til oral indgivelse eller sterile opløsninger eller suspensioner til parenteral 25 indgivelse. Ca. 10-ca. 500 mg af en forbindelse eller blanding af forbindelser med formlen I eller et fysiologisk acceptabelt salt heraf blandes med et fysiologisk acceptabelt bærestof, excipiens, bindemiddel, konserveringsmiddel, stabilisator, smagsstof etc. i en enhedsdoseringsform efter gængs 30 farmaceutisk praksis. Mængden af aktivt stof i disse midler eller præparater er afpasset således, at der fås en passende dosering inden for det angivne interval.The compounds prepared by the method of the invention can be used to obtain a reduction in blood pressure by being formulated into preparations thereof, such as tablets, capsules or elixirs for oral administration or sterile solutions or suspensions for parenteral administration. Ca. 10-C. 500 mg of a compound or mixture of compounds of formula I or a physiologically acceptable salt thereof are mixed with a physiologically acceptable carrier, excipient, binder, preservative, stabilizer, flavoring, etc. in a unit dosage form according to conventional pharmaceutical practice. The amount of active substance in these agents or compositions is adjusted so as to obtain a suitable dosage within the specified range.
Som eksempler på hjælpestoffer, der kan inkorporeres i tabletter, kapsler og lignende, kan nævnes følgende: 35 et bindemiddel såsom gummitragant, akacie, majsstivelse eller gelatine, excipiens såom dicalciumphosphat eller mikro-Examples of excipients which can be incorporated into tablets, capsules and the like include the following: a binder such as gum tragacanth, acacia, corn starch or gelatin, excipients such as dicalcium phosphate or
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krystallinsk cellulose, et disintegreringsmiddel såsom majsstivelse, kartoffelstivelse, algininsyre og lignende, et smøremiddel såsom magnesiumstearat, et sødemiddel såsom sach- carose, lactose eller saccharin, et smagsstof såsom pebermynte, 5 vintergrøntolie eller kirsebæraroma. Når enhedsdoseringsformen er en kapsel, kan den ud over materialer af ovennævnte type indeholde et flydende bærestof såsom en fed olie.crystalline cellulose, a disintegrant such as corn starch, potato starch, alginic acid and the like, a lubricant such as magnesium stearate, a sweetener such as saccharose, lactose or saccharin, a flavoring such as peppermint, winter green oil or cherry flavor. When the unit dosage form is a capsule, it may contain, in addition to materials of the above type, a liquid carrier such as a fatty oil.
Der kan findes forskellige andre materialer såsom overtræk eller andetø der modificerer doseringsenhedens fysiske form.Various other materials may be found such as coatings or other islets which modify the physical form of the dosage unit.
10 Således kan tabletter være overtrukket med shellak, sukker eller begge dele. En sirup eller eliksir kan indeholde den aktive forbindelse, saccharose som sødemiddel, methyl- og propylparabener som konserveringsmidler, et farvestof og et smagsstof såsom kirsebær» eller oranaearoma.Thus, tablets may be coated with shellac, sugar or both. A syrup or elixir may contain the active compound, sucrose as a sweetener, methyl and propyl parabens as preservatives, a dye and a flavoring such as cherry or orange flavor.
15 Sterile præparater til injektion kan sammensættes i overensstemmelse med gængs farmaceutisk praksis ved at opløse eller suspendere det aktive stof i et bærestof såsom vand til injektion, en naturligt forekommende vegetabilsk o-lie såsom sesamolie, kokosnødolie, jordnøddeolie, bomulds-20 frøolie etc.15 Sterile injection preparations can be formulated in accordance with current pharmaceutical practice by dissolving or suspending the active ingredient in a carrier such as water for injection, a naturally occurring vegetable oil such as sesame oil, coconut oil, peanut oil, cotton seed oil, etc.
De følgende eksempler tjener til yderligere belysning af fremgangsmåden ifølge opfindelsen, og til illustration af de fremstillede forbindelsers aktivitet som ovenfor omtalt.The following examples serve to further elucidate the process of the invention and to illustrate the activity of the compounds prepared as discussed above.
25 Eksempel 1 1-(3-Acetylthio-l-oxopropyl)-trans-4-methoxy-L-prolin a) N-Acetyl-trans-4-hydroxy-L-prolinExample 1 1- (3-Acetylthio-1-oxopropyl) -trans-4-methoxy-L-proline a) N-Acetyl-trans-4-hydroxy-L-proline
En omrørt suspension af 26,2 g (0,2 mol) trans-4--hydroxy-L-prolin i 400 ml eddikesyre behandles med 26 ml 30 eddikesyreanhydrid. Det faste stof opløses gradvis efter to timers omrøring ved stuetemperatur. Opløsningen hældes på en 2 liters kolbe, og opløsningsmidlet fjernes i en roterende fordamper ved en badtemperatur på 45°C. Den sirups-agtige remanens (57,5 g) fortyndes med 100 ml ether, hvilket 36 giver et krystallinsk faststof. Efter afkøling natten over .10A stirred suspension of 26.2 g (0.2 mole) of trans-4-hydroxy-L-proline in 400 ml of acetic acid is treated with 26 ml of acetic anhydride. The solid dissolves gradually after two hours of stirring at room temperature. The solution is poured onto a 2 liter flask and the solvent is removed in a rotary evaporator at a bath temperature of 45 ° C. The syrupy residue (57.5 g) is diluted with 100 ml of ether to give a crystalline solid. After cooling overnight .10
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filtreres det faste stof fra, vaskes med kold ether og tørres i en ekssiccator. Dette materiale, der vejer 35,7 g, pulveriseres og suspenderes i 100 ml ether, afkøles og filtreres, hvilket giver 33,8 g (98%) N-acetyl-trans-4-hydroxy-5 -L-prolin, smeltepunkt 128-131°C. Omkrystallisation af 0,5 g af dette materiale ud fra 5 ml acetonitril giver 0,45 g farveløst fast stof, smeltepunkt 130-132°C: [a] ^ -92° (c, 1% i EtOH).the solid is filtered off, washed with cold ether and dried in a desiccator. This material weighing 35.7 g is pulverized and suspended in 100 ml of ether, cooled and filtered to give 33.8 g (98%) of N-acetyl-trans-4-hydroxy-5-L-proline, m.p. 128 -131 ° C. Recrystallization of 0.5 g of this material from 5 ml of acetonitrile gives 0.45 g of colorless solid, mp 130-132 ° C: [α] D -92 ° (c, 1% in EtOH).
b) N-Acetyl-trans-4-methoxy-L-prolin-methylester 10 En blanding af 30,0 g (0,17 mol) N-acetyl-trans-4- -hydroxy-L-prolin og 130 g sølvoxid pulveriseres i en morter, og denne ensartede blanding sættes til en 1-liters kolbe med 300 ml acetone. Opslæmningen omrøres, behandles portionsvis med 130 ml methyliodid, og temperaturen holder under 40°C ved 15 afkøling med koldtvandsbad. Efter omrøring i 7 timer henstår blandingen natten over. Det faste stof filtreres fra, vaskes godt med actone, og filtratet inddampes på en roterende fordamper, hvilket giver 38,3 g sirupsagtig remanens. Denne genopløses i 350 ml acetone og behandles igen med 130 g sølv-20 oxid og 130 ml methyliodid, hvilket giver 41 g remanens. Denne destilleres, hvilket giver 32,2 g destillat, kogepunkt 130-140°C (0,3 mm). Efter opløsning i 30 ml cyclohexan og afkøling vejer den næsten farveløse faste N-acetyl-trans-4--methoxy-L-prolin-methylester 31,4 g, smeltepunkt 71-75°C.b) N-Acetyl-trans-4-methoxy-L-proline methyl ester A mixture of 30.0 g (0.17 mol) of N-acetyl-trans-4-hydroxy-L-proline and 130 g of silver oxide is pulverized. in a mortar, and this uniform mixture is added to a 1-liter flask with 300 ml of acetone. The slurry is stirred, treated portionwise with 130 ml of methyl iodide, and the temperature is kept below 40 ° C by cooling with a cold water bath. After stirring for 7 hours, the mixture is left to stand overnight. The solid is filtered off, washed well with actone and the filtrate is evaporated on a rotary evaporator to give 38.3 g of syrupy residue. This is redissolved in 350 ml of acetone and again treated with 130 g of silver-20 oxide and 130 ml of methyl iodide to give 41 g of residue. This is distilled to give 32.2 g of distillate, boiling point 130-140 ° C (0.3 mm). After dissolving in 30 ml of cyclohexane and cooling, the nearly colorless solid N-acetyl-trans-4-methoxy-L-proline methyl ester weighs 31.4 g, mp 71-75 ° C.
25 Omkrystallisation ud fra 31 ml ethylacetat giver 25,1 g (66%) farveløst fast stof, smeltepunkt 76-77°C. [a]^ -83° (c, 1% i EtOH).Recrystallization from 31 ml of ethyl acetate gives 25.1 g (66%) of colorless solid, mp 76-77 ° C. [α] D -83 ° (c, 1% in EtOH).
c) trans-4-Methoxy-L-prolinc) trans-4-methoxy-L-proline
Til en omrørt opløsning af 27,0 g (0,085 mol) bari- 30 umhydroxid . 8^0 i 525 ml vand (ca. 3,3 N) sættes 11,0 g (0,05 mol) N-acetyl-trans-4-methoxy-L-prolin-methylester.To a stirred solution of 27.0 g (0.085 mole) of barium hydroxide. To 525 ml of water (about 3.3 N) is added 11.0 g (0.05 mol) of N-acetyl-trans-4-methoxy-L-proline methyl ester.
Den fremkomne opløsning omrøres ved 18-20°C i 3 timer, afkøles og behandles med fortyndet svovlsyre (8,8 g koncentreret H2S0^ i 20 ml vand). Den sure suspension henstår natten over.The resulting solution is stirred at 18-20 ° C for 3 hours, cooled and treated with dilute sulfuric acid (8.8 g of concentrated H 2 SO 4 in 20 ml of water). The acidic suspension is left overnight.
35 Blandingen filtreres gennem et tykt lag "Celite", hvilket giver et "mælkeagtigt" filtrat. Dette inddampes på en roteren de fordamper ved 50°C under anvendelse af en højvakuumpumpe, hvilket giver en mælkeagtig remanens, der vejer 121 g. Dette 11The mixture is filtered through a thick layer of "Celite" to give a "milky" filtrate. This is evaporated on a rotor they evaporate at 50 ° C using a high vacuum pump, giving a milky residue weighing 121 g.
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materiale behandles med fortyndet svovlsyre (19,0 g koncentreret i 75 ml vand), og den fremkomne blanding omrø res og tilbagesvales i 3 timer. Efter afkøling til 30°C behandles blandingen portionsvis med 48 g bariumhydroxid .The material is treated with dilute sulfuric acid (19.0 g concentrated in 75 ml of water) and the resulting mixture is stirred and refluxed for 3 hours. After cooling to 30 ° C, the mixture is treated portionwise with 48 g of barium hydroxide.
5 8H2O,. og pH indstilles fra 6,0 til 4,0 med fortyndet svovl syre. Efter henstand natten over filtreres blandingen gennem et tykt lag "Celite". Det mælkeagtige filtrat inddampes som ovenfor, hvilket giver 50 g farveløs tør remanens. Denne opløses i 200 ml varm chloroform og filtreres gennem et 10 lag "Celite" for at fjerne bariumsulfatet. Det let uklare filtrat inddampes på en roterende fordamper, hvilket giver et gelatinøst materiale (17,7 g), der suspenderes i 100 ml ether og filteres, hvilket giver 7,5 g (94%) næsten farveløst fast stof, smeltepunkt 185-190°C (sønderdeling). Det-15 te materiale suspenderes i 30 ml varm acetonitril, afkøles og filtreres, hvilket giver 4,0 g (50%) af et farveløst fast trans-4-methoxy-L-prolin, smeltepunkt 209-211°C (sønderdeling) ; [aJ^5 -75° (c, 1% i EtOH) .5 8H2O ,. and pH is adjusted from 6.0 to 4.0 with dilute sulfuric acid. After standing overnight, the mixture is filtered through a thick layer of "Celite". The milky filtrate is evaporated as above to give 50 g of colorless dry residue. This is dissolved in 200 ml of warm chloroform and filtered through a 10 layer of "Celite" to remove the barium sulfate. The slightly cloudy filtrate is evaporated on a rotary evaporator to give a gelatinous material (17.7 g) suspended in 100 ml of ether and filtered to give 7.5 g (94%) of almost colorless solid, m.p. 185-190 ° C (decomposition). The material is suspended in 30 ml of hot acetonitrile, cooled and filtered to give 4.0 g (50%) of a colorless solid trans-4-methoxy-L-proline, mp 209-211 ° C (dec.); [α] D = -75 ° (c, 1% in EtOH).
d) 1-(3-Acetylthio-l-oxopropyl)-trans-4-methoxy-L-prolin 20 En opløsning af 3,5 g (0,024 mol) trans-4-methoxy- -L-prolin i 50 ml vand omrøres, afkøles til 5°C, og der tilsættes 3 g natriumcarbonat. Denne blanding behandles med en opløsning af 4,0 g (0,024 mol) 3-acetylthiopropionylchlorid i 5 ml ether i løbet af 10 minutter med intermitterende til-25 sætning af 3 g natriumcarbonat for holde pH på ca. 8,0.d) 1- (3-Acetylthio-1-oxopropyl) -trans-4-methoxy-L-proline A solution of 3.5 g (0.024 mol) of trans-4-methoxy-L-proline in 50 ml of water is stirred. , cool to 5 ° C and add 3 g of sodium carbonate. This mixture is treated with a solution of 4.0 g (0.024 mole) of 3-acetylthiopropionyl chloride in 5 ml of ether over 10 minutes with intermittent addition of 3 g of sodium carbonate to maintain a pH of approx. 8.0.
Blandingen omrøres i isbad i yderligere en time, der tilsættes 25 ml vand og derefter en opløsning af 5 ml koncentreret saltsyre i 25 ml vand (CC^-udvikling). Den stærkt su re opløsning mættes med natriumchlorid og ekstraheres med 50 ml 30 ethylacetat (fire gange). De organiske faser forenes, tørres (MgSO^), filtreres, og opløsningsmidlet afdampes, hvilket giver 6,0 g (90%) farveløst sirupsagtigt 1-(3-acetylthio--1-oxopropyl)-trans-4-methoxy-L-prolin. Denne syre opløses i 25 ml ethylacetat og behandles med 4,7 g dicyclohexylamin, 35 hvilket giver en opløsning, der hurtigt bliver en fast masse.The mixture is stirred in an ice bath for an additional hour, adding 25 ml of water and then a solution of 5 ml of concentrated hydrochloric acid in 25 ml of water (CC The highly acidic solution is saturated with sodium chloride and extracted with 50 ml of 30 ethyl acetate (four times). The organic phases are combined, dried (MgSO 4), filtered and the solvent evaporated to give 6.0 g (90%) of colorless syrupy 1- (3-acetylthio-1-oxopropyl) -trans-4-methoxy-L proline. This acid is dissolved in 25 ml of ethyl acetate and treated with 4.7 g of dicyclohexylamine to give a solution which quickly becomes a solid mass.
Der tilsættes yderligere 15 ml ethylacetat, og blandingen opløses på dampbad, afkøles og filtreres, hvilket giver 8,7 g 12An additional 15 ml of ethyl acetate is added and the mixture is dissolved in a steam bath, cooled and filtered to give 8.7 g of
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dicyclohexylaminsalt, smeltepunkt 170-172°C. Efter krystallisation ud fra 60 ml acetonitril vejer det farveløse faste stof 8,3 g (75%), smeltepunkt 171-173°C; [a]^ -35° (c, 1% i EtOH).dicyclohexylamine salt, mp 170-172 ° C. After crystallization from 60 ml of acetonitrile, the colorless solid weighed 8.3 g (75%), mp 171-173 ° C; [α] D -35 ° (c, 1% in EtOH).
5 Decyclohexylaminsaltet omdannes til l-(3-acetyl- thio-l-oxopropyl)trans-4-methoxy-L-prolin ved at suspendere 8,0 g i 60 ml ethylacetat afkølet i isbad og behandle det portionsvis med 60 ml 10% kaliumbisulfat. De klare lag adskilles, og den vandige del ekstraheres med 60 ml ethylace-10 tat (2 gange). De organiske faser forenes, tørres (MgSO^), filtreres og opløsningsmidlet afdampes, hvilket giver 4,6 g (80%) af en farveløs sirup.The decyclohexylamine salt is converted to 1- (3-acetylthio-1-oxopropyl) trans-4-methoxy-L-proline by suspending 8.0 g in 60 ml of ethyl acetate cooled in an ice bath and treating it portionwise with 60 ml of 10% potassium bisulfate. The clear layers are separated and the aqueous portion is extracted with 60 ml of ethyl acetate (2 times). The organic phases are combined, dried (MgSO 4), filtered and the solvent is evaporated to give 4.6 g (80%) of a colorless syrup.
Eksempel 2 15 1-(3-Mercapto-l-oxopropyl)-trans-4-methoxy-L-prolinExample 2 1- (3-Mercapto-1-oxopropyl) -trans-4-methoxy-L-proline
Til 1-(3-acetylthio-l-oxopropyl)-trans-4-methoxy--L-prolinet, der fremstilles i eksempel 1 (4,6 g, 0,017 mol) sættes en kold opløsning af 9 ml koncentreret ammoniak i 22 ml vand. Basen opløses på ca. 30 minutter, og den fremkomne 20 opløsning (under argon) henstår i 2 timer ved stuetemperatur. Denne opløsning afkøles, ekstraheres med 25 ml ethylacetat (2 gange), og ethylacetatekstrakten kasseres. Opløsningen ekstraheres igen med 25 ml ethylacetat og gøres sur med 17 ml 1:1 saltsyre. Blandingen rystes, skilles, og den vandige 25 fase ekstraheres med 25 ml ethylacetat (3 gange). De organiske faser forenes, tørres (MgSO^), filtreres, og opløsningsmidlet fjernes på den roterende fordamper, hvilket giver 2,3 g (59%) farveløs sirup, 1-(3-mercapto-l-oxopropyl)-trans-4--methoxy-L-prolin, [a]^ -60° (c, 1% i EtOH); R^ 0,49 (MeOH 30 på silicagel, fremkaldt med nitrosoferricyanid som reagens), Analyse: Beregnet for C^H^NO^S. 1/4 H20: C 45,46, H 6,57, N 5,87, S 13,48.To the 1- (3-acetylthio-1-oxopropyl) -trans-4-methoxy-L-proline prepared in Example 1 (4.6 g, 0.017 mol) is added a cold solution of 9 ml of concentrated ammonia in 22 ml. water. The base dissolves in approx. 30 minutes, and the resulting solution (under argon) is left at room temperature for 2 hours. This solution is cooled, extracted with 25 ml of ethyl acetate (2 times) and the ethyl acetate extract discarded. The solution is extracted again with 25 ml of ethyl acetate and acidified with 17 ml of 1: 1 hydrochloric acid. The mixture is shaken, separated and the aqueous phase is extracted with 25 ml of ethyl acetate (3 times). The organic phases are combined, dried (MgSO 4), filtered and the solvent removed on the rotary evaporator to give 2.3 g (59%) of colorless syrup, 1- (3-mercapto-1-oxopropyl) -trans-4- -methoxy-L-proline, [α] 25 -60 ° (c, 1% in EtOH); R f 0.49 (MeOH 30 on silica gel, developed with nitrosoferricyanide as reagent), Analysis: Calculated for C 1/4 H2 O: C 45.46, H 6.57, N 5.87, S 13.48.
Fundet: C 45,42, H 6,78, N 5,96, S 13,27.Found: C 45.42, H 6.78, N 5.96, S 13.27.
35 Der fås yderligere 1,1 g produkt (ialt 3,4 g, 87%) ved at mætte den vandige fase med natriumchlorid og ekstrahere med 25 ml ethylacetat (2 gange).An additional 1.1 g of product (3.4 g, 87% in total) is obtained by saturating the aqueous phase with sodium chloride and extracting with 25 ml of ethyl acetate (2 times).
1313
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Natriumsaltet dannes ved at behandle siruppen med vandigt natriumbicarbonat og frysetørre.The sodium salt is formed by treating the syrup with aqueous sodium bicarbonate and freeze-drying.
Eksempel 3 5 (trans)-1»[D-3-(Acetylthio)-2-methyl-l-oxopropyl]-4-metho- oxy-L-prolinExample 35 (trans) -1 »[D-3- (Acetylthio) -2-methyl-1-oxopropyl] -4-methoxy-L-proline
En opløsning af 4,3 g (0,029 mol) trans-4-methoxy--L-prolin i 50 ml vand omrøres, afkøles til 5°C, og der tilsættes 3 g natriumcarbonat. Denne opløsning behandles med 10 5,2 g (0,029 mol) D-3-(acetylthio)-2-methylpropionylchlorid i 5 ml ether i løbet af 10 minutter med intermitterende tilsætning af 3 g natriumcarbonat for at holde pH på ca. 8,0.A solution of 4.3 g (0.029 mol) of trans-4-methoxy-L-proline in 50 ml of water is stirred, cooled to 5 ° C and 3 g of sodium carbonate is added. This solution is treated with 5.2 g (0.029 mol) of D-3- (acetylthio) -2-methylpropionyl chloride in 5 ml of ether over 10 minutes with the intermittent addition of 3 g of sodium carbonate to maintain the pH of ca. 8.0.
Denne blanding omrøres i isbad i 1,5 time, der tilsættes 25 ml vand og derefter en opløsning af 6 ml koncentreret salt-15 syre i 25 ml vand (CC^-udvikling). Den fremkomne stærkt sure opløsning ekstraheres med 50 ml ethylacetat (fire gange).This mixture is stirred in an ice bath for 1.5 hours, then 25 ml of water is added and then a solution of 6 ml of concentrated hydrochloric acid in 25 ml of water (CC The resulting strongly acidic solution is extracted with 50 ml of ethyl acetate (four times).
De organiske faser forenes, tørres (MgS04), filtreres, og opløsningsmidlet afdampes, hvilket giver 6,1 g (73%) (trans)--1-[D-3-(acetylthio)-2-methyl-l-oxopropyl]-4-methoxy-L-pro-20 lin som en svagt gul sirupsagtig remanens. Denne syre opløses i 50 ml ethylacetat og behandles med en opløsning af 4,0 g dicyclohexylamin i 20 ml ethylacetat. Produktet begynder at krystalliseres ud fra opløsningen i løbet af ca. 1 minut. Efter afkøling natten over filtreres det næsten farveløse 25 faste stof og tørres, udbytte 6,7 g, smeltepunkt 175-177°C; [a]^ -55° (c, 1% EtOH). Efter krystallisation ud fra 60 ml acetonitril vejer det næsten farveløse faste dicyclohex-ylaminsalt 5,6 g (41%), smeltepunkt 179-181°C, [a]^ -62° (c,1% i EtOH).The organic phases are combined, dried (MgSO 4), filtered and the solvent is evaporated to give 6.1 g (73%) of (trans) - 1- [D-3- (acetylthio) -2-methyl-1-oxopropyl] -4-methoxy-L-prolin as a pale yellow syrupy residue. This acid is dissolved in 50 ml of ethyl acetate and treated with a solution of 4.0 g of dicyclohexylamine in 20 ml of ethyl acetate. The product begins to crystallize from the solution over approx. 1 minute. After cooling overnight, the almost colorless solid is filtered and dried, yield 6.7 g, mp 175-177 ° C; [α] D -55 ° (c, 1% EtOH). After crystallization from 60 ml of acetonitrile, the almost colorless solid dicyclohex-ylamine salt weighed 5.6 g (41%), m.p. 179-181 ° C, [α] D -62 ° (c, 1% in EtOH).
30 Dicyclohexylaminsaltet omdannes til syren ved at suspendere 5,5 g i 50 ml ethylacetat, afkøle i isbad og behandle med 50 ml 10% kaliumbisulfat. Lagene adskilles, og den vandige del ekstraheres med 50 ml ethylacetat (2 gange).The dicyclohexylamine salt is converted to the acid by suspending 5.5 g in 50 ml of ethyl acetate, cooling in an ice bath and treating with 50 ml of 10% potassium bisulfate. The layers are separated and the aqueous portion is extracted with 50 ml of ethyl acetate (2 times).
De organiske faser forenes, tørres (MgSO^), filtreres, og 35 opløsningsmidlet afdampes, hvilket giver 3,4 g (41%) næsten farveløst (trans)-1-[D-3-(acetylthio)-2-methyl-l-oxopropyl]--4-methoxy-L-prolin som sirup.The organic phases are combined, dried (MgSO 4), filtered and the solvent evaporated to give 3.4 g (41%) of almost colorless (trans) -1- [D-3- (acetylthio) -2-methyl-1 -oxopropyl] -4-methoxy-L-proline as syrup.
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3.43.4
Eksempel 4 (trans)-4-Methoxy-l-(D-3-mercapto-2-methyl-l-oxopropyl)- -L-prolinExample 4 (trans) -4-Methoxy-1- (D-3-mercapto-2-methyl-1-oxopropyl) - -L-proline
Til 3,4 g (trans)-1-[D-e-(acetylthio)-2-methy1-1-5 -oxopropyl]-4-methoxy-L-prolin sættes en kold opløsning af 8 ml koncentreret ammoniak i 20 ml vand. Basen opløses på ca. 10 minutter, og den fremkomne opløsning (under argon) henstår ved stuetemperatur i to timer. Denne opløsning afkøles, ekstraheres med 20 ml ethylacetat (2 gange), skilles 10 i lag med 20 ml ethylacetat og gøres sur med 15 ml 1:1 saltsyre. Denne blanding mættes med natriumchlorid, lagene adskilles, og den vandige fase ekstraheres med 20 ml ethylacetat (3 gange). De organiske faser forenes, tørres (MgSO^), filtreres, og opløsningsmidlet afdampes, hvilket giver 2,9 15 g (100%) næsten farveløst (trans)-4-methoxy-1-(D-3-mercapto--2-methyl-l-oxopropyl)-L-prolin, [a]^ -80° (c, 1% i EtOH);To 3.4 g of (trans) -1- [D-e- (acetylthio) -2-methyl-1-5-oxopropyl] -4-methoxy-L-proline is added a cold solution of 8 ml of concentrated ammonia in 20 ml of water. The base dissolves in approx. 10 minutes and the resulting solution (under argon) is left at room temperature for two hours. This solution is cooled, extracted with 20 ml of ethyl acetate (2 times), separated in layers with 20 ml of ethyl acetate and acidified with 15 ml of 1: 1 hydrochloric acid. This mixture is saturated with sodium chloride, the layers are separated and the aqueous phase is extracted with 20 ml of ethyl acetate (3 times). The organic phases are combined, dried (MgSO 4), filtered and the solvent is evaporated to give 2.9 g (100%) of almost colorless (trans) -4-methoxy-1- (D-3-mercapto-2 methyl-1-oxopropyl) -L-proline, [α] D -80 ° (c, 1% in EtOH);
Rf 0,53 (MeOH på silikagel, fremkaldt med nitroso-ferricyanid som reagens).Rf 0.53 (MeOH on silica gel developed with nitrosoferricyanide as reagent).
Analyse: Beregnet for C^qH^NO^S . 1/4^0: C 47,69, H 6,83, 20 N 5,56, S 12,73Analysis: Calculated for C ^ qH ^NO ^S. 1/4 O: C 47.69, H 6.83, N 5.56, S 12.73
Fundet: C 47,90, H 6,84, N 5,85, S 12,76.Found: C, 47.90; H, 6.84; N, 5.85; S, 12.76.
Eksempel 5 25 (trans)-1-[D-3-(Acetylthio)-2-methyl-l-oxopropyl]-4-ethoxy- -L-prolinExample 5 (trans) -1- [D-3- (Acetylthio) -2-methyl-1-oxopropyl] -4-ethoxy-L-proline
Ved at benytte den i eksempel 3 beskrevne fremgangsmåde, men anvende en ækvivalent mængde trans-4-ethoxy-L-pro-lin (J.Med. Chem., 10, 1161 (1967)) i stedet for (trans)-4-30 -methoxy-L-prolin fås (trans)-1-(D-3-(acetylthio)-2-methy1--1-oxopropyl]-4-ethoxy-L-prolin. Produktet renses som dicy-clohexylaminsaltet, smeltepumpt 170-172°C (krystalliseret ud fra isopropylalkohol) ; -64° (c, 1% i EtOH).Using the procedure described in Example 3, but using an equivalent amount of trans-4-ethoxy-L-protein (J.Med. Chem., 10, 1161 (1967)) instead of (trans) -4- Methoxy-L-proline is obtained (trans) -1- (D-3- (acetylthio) -2-methyl-1-oxopropyl] -4-ethoxy-L-proline. The product is purified as the dicyclohexylamine salt, melt pump 170 -172 ° C (crystallized from isopropyl alcohol); -64 ° (c, 1% in EtOH).
Dette salt (7,75 g) omdannes til den frie syre ved 35 behandling med kaliumbisulfatopløsning som beskrevet i eksempel 4, hvilket giver 4,85 g næsten farveløst (trans)-1-[D-3--(acetylthio)-2-methyl-l-oxopropyl]-4-ethoxy-L-prolin som sirup.This salt (7.75 g) is converted to the free acid by treatment with potassium bisulfate solution as described in Example 4 to give 4.85 g of almost colorless (trans) -1- [D-3 - (acetylthio) -2- methyl 1-oxopropyl] -4-ethoxy-L-proline as syrup.
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Eksempel 6 (trans)-4-Ethoxy-1-(D-3-mercapto-2-methyl-l-oxopropyl)-L- -prolinExample 6 (trans) -4-Ethoxy-1- (D-3-mercapto-2-methyl-1-oxopropyl) -L- -proline
Til materialet fra eksempel 5 (4,85 g) sættes en 5 kold opløsning af 9 ml koncentreret ammoniak i 22 ml vand (under argon). Blandingen behandles på samme måde som i eksempel 4, hvilket giver 4,2 g (100%) næsten farveløst (trans)-4-ethoxy-1-(D-3-mercapto-2-methy1-1-oxopropy1)-L--prolin som sirup, [a]^ -80° (c, 1% i EtOH) , 0,64 (MeOHTo the material of Example 5 (4.85 g) is added a 5 cold solution of 9 ml of concentrated ammonia in 22 ml of water (under argon). The mixture is treated in the same manner as in Example 4 to give 4.2 g (100%) of almost colorless (trans) -4-ethoxy-1- (D-3-mercapto-2-methyl-1-oxopropyl) -L- -proline as syrup, [α] 25 -80 ° (c, 1% in EtOH), 0.64 (MeOH
10 på silicagel, fremkaldt med nitroso-ferricyanid som reagens). Analyse: Beregnet for C-^H^NO^S: C 50,55, H 7,33, N 5,36, S 12,27.10 on silica gel, developed with nitrosoferricyanide as reagent). Analysis: Calculated for C- HH ^NO ^S: C 50.55, H 7.33, N 5.36, S 12.27.
Fundet: C 50,34, H 7,34, N 5,39, S 12,11.Found: C, 50.34; H, 7.34; N, 5.39; S, 12.11.
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Eksempel 7 (cis)-1-[D-3-(Acetylthio)-2-methyl-l-oxopropyl]-4-methoxy- -L-prolin a) N-Carbobenzyloxy-cis-4-hydroxy-L-prolin 20 N-Carbobenzyloxy-4-keto-L-prolin (10 g, 0,038 mol) opløses i 300 ml methanol og reduceres med 5,8 g (0,15 mol) natriumborhydrid i 20 ml vand som beskrevet i JACS, 79, 189 (1957), hvilket giver 8,7 g af et skumagtigt produkt. Dette materiale opløses i 30 ml ethanol, behandles med 3,5 g cy-25 clohexylamin i lidt ethanol og fortyndes til 500 ml med e-ther. Ved podning og gnidning udskilles det krystallinske cyclohexylaminsalt hurtigt og der fås 10,8 g, smeltepunkt 163-165°C. Dette cyclohexylaminsalt behandles derefter med 30 ml 2N HC1 og ekstraheres med ethylacetat (4 x 50 ml), 30 hvilket giver 8 g N-carbobenzyloxy-cis-4-hydroxy-L-prolin som et glaslignende materiale.Example 7 (cis) -1- [D-3- (Acetylthio) -2-methyl-1-oxopropyl] -4-methoxy-L-proline a) N-Carbobenzyloxy-cis-4-hydroxy-L-proline N-Carbobenzyloxy-4-keto-L-proline (10 g, 0.038 mol) is dissolved in 300 ml of methanol and reduced with 5.8 g (0.15 mol) of sodium borohydride in 20 ml of water as described in JACS, 79, 189 ( 1957) to give 8.7 g of a foamy product. This material is dissolved in 30 ml of ethanol, treated with 3.5 g of cyclohexylamine in a little ethanol and diluted to 500 ml with ether. By grafting and rubbing, the crystalline cyclohexylamine salt is rapidly excreted and 10.8 g, mp 163-165 ° C are obtained. This cyclohexylamine salt is then treated with 30 ml of 2N HCl and extracted with ethyl acetate (4 x 50 ml) to give 8 g of N-carbobenzyloxy-cis-4-hydroxy-L-proline as a glass-like material.
b) N-Carbobenzyloxy-cis-4-methoxy-L-prolin-methylester 13,9 g N-carbobenzyloxy-cis-4-hydroxy-L-prolin (0,052 mol) behandles med 40 g sølvoxid og 40 ml methyliodid 35 (2 gange) i acetone (først 100 ml, derefter 120 ml) som be skrevet i eksempel 1(b), hvilket giver 17,5 g (100%) N-carbo-benzyloxy-cis-4-methoxy-L-prolin-methylester som en gul olie.b) N-Carbobenzyloxy-cis-4-methoxy-L-proline methyl ester 13.9 g of N-carbobenzyloxy-cis-4-hydroxy-L-proline (0.052 mol) are treated with 40 g of silver oxide and 40 ml of methyl iodide (2 times) in acetone (first 100 ml, then 120 ml) as described in Example 1 (b) to give 17.5 g (100%) of N-carbo-benzyloxy-cis-4-methoxy-L-proline methyl ester like a yellow oil.
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c) N-Carbobenzyloxv-cis-4-hnethoxy-L-prolinc) N-Carbobenzyloxy-cis-4-methoxy-L-proline
De .-ovennævnte 17,5 g N-carbobenzyloxy-cis-4-meth-oxy-L-prolin-methylester (ca. 0,052 mol) opløses i 135 ml methanol, behandles dråbevis ved -1°C til 4°C med 32 ml 5 (0,064 mol) 2N natriumhydroxid, holdes derefter ved 0°C i en time og ved stuetemperatur natten over. Efter at ca. halvdelen af opløsningsmidlet er fjernet på en roterende fordamper, fortyndes opløsningen med 300 ml vand, vaskes med ether (vaskevæsken kasseres), gøres sur under afkøling med 10 12,5 ml 1:1 saltsyre til pH 2 og ekstraheres med ethylacetat (4 gange 150 ml). Ekstrakterne forenes, tørres (MgSC>4), filtreres, og opløsningsmidlet afdampes, hvilket giver 15 g af en orangegul sirup. Denne opløses i 60 ml ethanol, behandles med 6 g cyclohexylamin i 10 ml ethanol og fortyndes 15 til 900 ml med ether. Ved podning og gnidning udskilles det krystallinske N-carbobenzyloxy-cis-4-methoxy-L-prolin-cy-clohexylaminsalt: vægt efter afkøling natten over 10,2 g, smeltepunkt 148-150°C (s. 144°C), [a]^ -35° (c, 1% i ethan ol) . Efter omkrystallisation ud fra 40 ml acetonitril ve-20 jer det næsten farveløse faste stof 8,8 g, smeltepunkt 150-152°C (s. 145°C) , [cc]^6 -34° (c, 1% i ethanol).The above-mentioned 17.5 g of N-carbobenzyloxy-cis-4-methoxy-L-proline methyl ester (about 0.052 mol) is dissolved in 135 ml of methanol, treated dropwise at -1 ° C to 4 ° C with 32 ml of 5 (0.064 mol) of 2N sodium hydroxide is then kept at 0 ° C for one hour and at room temperature overnight. After approx. half of the solvent was removed on a rotary evaporator, diluted with 300 ml of water, washed with ether (the wash liquid discarded), acidified with cooling with 12.5 ml of 1: 1 hydrochloric acid to pH 2 and extracted with ethyl acetate (4x150). mL). The extracts are combined, dried (MgSC> 4), filtered and the solvent is evaporated to give 15 g of an orange-yellow syrup. This is dissolved in 60 ml of ethanol, treated with 6 g of cyclohexylamine in 10 ml of ethanol and diluted 15 to 900 ml with ether. By grafting and rubbing, the crystalline N-carbobenzyloxy-cis-4-methoxy-L-proline-cyclohexylamine salt is separated: weight after cooling overnight at 10.2 g, mp 148-150 ° C (p. 144 ° C), [ α] -35 ° (c, 1% in ethanol, etc.). After recrystallization from 40 ml of acetonitrile, the nearly colorless solid weighs 8.8 g, m.p. 150-152 ° C (p. 145 ° C), [cc] +6 -34 ° (c, 1% in ethanol ).
Cyclohexylaminsaltet behandles med saltsyre, hvilket giver 6,9 g (48%) N-carbobenzyloxy-cis-4-methoxy-L-pro- 26 o lin som en svagt gul viskos sirup, [a] -32 (c, 1% i ethan- 25 ol).The cyclohexylamine salt is treated with hydrochloric acid to give 6.9 g (48%) of N-carbobenzyloxy-cis-4-methoxy-L-procoline as a pale yellow viscous syrup, [α] 32 (c, 1%). ethanol).
d) cis-4-Methoxy-Ir-prolind) cis-4-Methoxy-Ir-proline
En blanding af 6,8 g N-carbobenzyloxy-cis-4-meth-oxy-L-prolin, 210 ml 2:1 methanol og vand og 2,3 g 5% palladium på kul anbringes i en hydrogenator ved 3 atm hydrogen 30 i fire timer. Blandingen filtreres for at fjerne katalysatoren, og filtratet inddampes, hvilket giver 3,15 g af et gråligt fast stof, smeltepunkt 218-220°C (sønderdeling). En prøve krystalliseres ud fra methanol-ether, hvilket giver farveløst cis-4-methxoy-L-prolin, smeltepunkt 224-226°C (sønderde-35 ling), [α]^5 -42° (c, 1% i methanol).A mixture of 6.8 g of N-carbobenzyloxy-cis-4-methoxy-L-proline, 210 ml of 2: 1 methanol and water and 2.3 g of 5% palladium on charcoal is placed in a hydrogenator at 3 atm hydrogen. for four hours. The mixture is filtered to remove the catalyst and the filtrate is evaporated to give 3.15 g of a greyish solid, mp 218-220 ° C (dec.). A sample is crystallized from methanol-ether to give colorless cis-4-methxoy-L-proline, m.p. 224-226 ° C (dec.), [Α] 5 ~ 42 ° (c, 1% in methanol) ).
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Analyse: Beregnet for CgH^NO^: C 49,64, H 7,64, N 9,65.Analysis: Calculated for CgHH NO NONO: C 49.64, H 7.64, N 9.65.
Pundet: C 49,63. H 7,71, N 9,54.Pound: C 49.63. H, 7.71; N, 9.54.
e) (cis)-1-[D-3-(Acetylthio)-2-methyl-l-oxopropyl]-4-meth-oxy-L-prolln 5 3 g cis-4-'methoxy-L-prolin (0,031 mol) og 4,2 g (0,023 mol) D-3-acetylthio-2-methylpropionylchlorid i 5 ml ether omsættes i 60 ml vand i nærværelse af natriumbicarbo-nat som beskrevet i eksempel 3. Der kræves ca. 20 ml 25% natriumcarbonat (vægt/volumen) for til at begynde med at 10 . bringe pH på 8,5 og for at holde det på 7,5-8,4 under acetyleringen. Det fremkomne rå viskose produkt (6,4 g) opløses i 50 ml ethylacetat og behandles med 3,9 g dicyclohexyl-amin i 20 ml ethylacetat. Produktet krystalliserer ud fra opløsningen og filtreres og tørres, hvilket giver 6,6 g di-15 cyclohexylaminsalt, smeltepunkt 172-174°C (s. 170°C),e) (cis) -1- [D-3- (Acetylthio) -2-methyl-1-oxopropyl] -4-methoxy-L-proline 5 g of cis-4-methoxy-L-proline (0.031 and 4.2 g (0.023 mol) of D-3-acetylthio-2-methylpropionyl chloride in 5 ml of ether are reacted in 60 ml of water in the presence of sodium bicarbonate as described in Example 3. 20 ml of 25% sodium carbonate (w / v) to begin with 10. bring the pH of 8.5 and to keep it at 7.5-8.4 during the acetylation. The resulting crude viscous product (6.4 g) is dissolved in 50 ml of ethyl acetate and treated with 3.9 g of dicyclohexylamine in 20 ml of ethyl acetate. The product crystallizes from the solution and is filtered and dried to give 6.6 g of di-cyclohexylamine salt, mp 172-174 ° C (p. 170 ° C).
2 £ Q2 £ Q
[a] p -60 (c, 1% i ethanol). 6,5 g af dette materiale om krystalliseres ud fra 35 ml acetonitril, hvilket giver 6 g farveløst fast dicyclohexylaminsalt, smeltepunkt 173-175°C (s. 170°C) , [<x]2d6 -60° (c, 1% i ethanol).[a] p -60 (c, 1% in ethanol). 6.5 g of this material is crystallized from 35 ml of acetonitrile to give 6 g of colorless solid dicyclohexylamine salt, mp 173-175 ° C (p. 170 ° C), [<x] 2d6 -60 ° (c, 1% in ethanol).
20 Analyse: Beregnet for Cj2H]_9^0^S.^2^23^5 c 61/24, H 9,00, N 5,95, S 6,81.Analysis: Calculated for C₂2H] _9 ^O S.S. 22. 23.5 61 c 61/24, H 9.00, N 5.95, S 6.81.
Fundet: C 61,16, H 8,81, N 5,95, S 6,67.Found: C 61.16, H 8.81, N 5.95, S 6.67.
Ved at benytte den i eksempel 3 beskrevne frem-25 gangsmåde omdannes dicyclohexylaminsaltet til syren ved at suspendere 5,9 g i 60 ml ethylacetat, afkøle i isbad og behandle med 60 ml 10% kaliumbisulfat. Lagene adskilles, og den vandige fase ekstraheres med 50 ml ethylacetat (4 gange).Using the procedure described in Example 3, the dicyclohexylamine salt is converted to the acid by suspending 5.9 g in 60 ml of ethyl acetate, cooling in an ice bath and treating with 60 ml of 10% potassium bisulfate. The layers are separated and the aqueous phase is extracted with 50 ml of ethyl acetate (4 times).
De organiske faser forenes, tørres (MgSO^), filtreres, og 30 opløsningsmidlet afdampes, hvilket giver 3,5 g (60%) farveløst (cis)-1-[D-3-(acetylthio)-2-methyl-l-oxopropyl]-4-meth-oxy-L-prolin, smeltepunkt 90-92°C (tritureret med ether), [a] -139° (c, 1% i ethanol), Rf 0,63 (methanol på silica- gel) .The organic phases are combined, dried (MgSO 4), filtered and the solvent is evaporated to give 3.5 g (60%) of colorless (cis) -1- [D-3- (acetylthio) -2-methyl-1- oxopropyl] -4-methoxy-L-proline, m.p. 90-92 ° C (triturated with ether), [α] -139 ° (c, 1% in ethanol), Rf 0.63 (methanol on silica gel ).
35 Analyse: Beregnet for C^H-^NO^S: C 49,81, H 6,62, N 4,84.Analysis: Calculated for C ^ HH- ^NO₂S: C 49.81, H 6.62, N 4.84.
Fundet: C 49,85, H 6,66, N 4,97.Found: C 49.85, H 6.66, N 4.97.
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Eksempel 8 (cis)-4-Methoxy-l-(D-3-mercapto-2-methyl-l-oxopropyl)-L- -prolin 2,9 g (cis)-1-[D-3-(acetylthio)-2-methyl-l-oxopro- 5 pyl]-4-methoxy-L-prolin (0,01 mol) hydrolyseres i 15 ml vand indeholdende 6,5 ml koncentreret ammoniak som beskrevet i eksempel 4, hvilket giver 2,3 g (93%) yderst viskos (cis)- -4-methoxy-l-(D-3-mercap to-2-methy1-1“oxopropy1)-L-prolin, 26 o der bliver voksagtigt ved henstand; [a] ^ -88 (c, 1% i e- 10 thanol).Example 8 (cis) -4-Methoxy-1- (D-3-mercapto-2-methyl-1-oxopropyl) -L- -proline 2.9 g (cis) -1- [D-3- (acetylthio) 2-Methyl-1-oxopropyl] -4-methoxy-L-proline (0.01 mol) is hydrolyzed in 15 ml of water containing 6.5 ml of concentrated ammonia as described in Example 4 to give 2.3 g (93%) highly viscous (cis) - -4-methoxy-1- (D-3-mercap to-2-methyl-1-oxopropyl) -L-proline, which becomes waxy upon standing; [α] D -88 (c, 1% in e-thanol).
Eksempel 8a (cis)-4-Methoxy-l-(D-3-mercapto-2-methyl-l-oxopropyl)-L--prolin-l-adamantanaminsalt 15 En opløsning af 0,55 g (0,0022 mol) cis-4-methoxy- -1-(D-3-mercapto-2-methyl-l-oxopropyl)-L-prolin i 15 ml ethyl-acetat behandles under argonatmosfære med en varm opløsning af 0,34 g (0,0022 mol) 1-adamantanamin i 10 ml ethylacetat til udfældning af saltet. Efter tre timer i kulden, fil-20 treres det farveløse faste stof fra under argon (opløsningsmidlet vedholdende), vaskes med noget koldt ethylacetat og tørres i vakuum i 20 timer, hvilket giver 0,7 g (79%) (cis)--4-methoxy-l-(D-3-mercapto-2-methyl-l-oxopropyl)-L-prolin-1--adamantanaminsalt, smeltepunkt 215-217°C (s. 210°C, sønder-25 deling 220°C) , [a]^* -60° (c, 1% i methanol).Example 8a (cis) -4-Methoxy-1- (D-3-mercapto-2-methyl-1-oxopropyl) -L-proline-1-adamantanamine salt A solution of 0.55 g (0.0022 mol) cis-4-methoxy--1- (D-3-mercapto-2-methyl-1-oxopropyl) -L-proline in 15 ml of ethyl acetate is treated under an argon atmosphere with a hot solution of 0.34 g (0.0022 mole) 1-adamantanamine in 10 ml of ethyl acetate to precipitate the salt. After three hours in the cold, the colorless solid is filtered off under argon (the solvent is persistent), washed with some cold ethyl acetate and dried in vacuo for 20 hours to give 0.7 g (79%) (cis) - 4-Methoxy-1- (D-3-mercapto-2-methyl-1-oxopropyl) -L-proline-1-adamantanamine salt, mp 215-217 ° C (p. 210 ° C, decomposition 220 ° C), [α] D -60 ° (c, 1% in methanol).
Eksempel 9 (trans)-1-[D-3-Acetylthio)-2-methyl-1-oxopropyl]-4-propoxy-30 -L-prolin a) N-acetyl-trans-4-propoxy-L-prolin-propylesterExample 9 (trans) -1- [D-3-Acetylthio) -2-methyl-1-oxopropyl] -4-propoxy-30-L-proline a) N-acetyl-trans-4-propoxy-L-proline propylester
Omsætning af 30 g N-acetyl-trans-4-hydroxy-L-pro-lin fra eksempel 1(a) med 110 g sølvoxid og 110 ml propylio-did i 300 ml acetone som beskrevet ved fremgangsmåden i ek-35 sempel 1(b) giver 19,6 g (41%) svagt gul-orange N-acetyl-Reaction of 30 g of N-acetyl-trans-4-hydroxy-L-proline from Example 1 (a) with 110 g of silver oxide and 110 ml of propyliodide in 300 ml of acetone as described by the procedure of Example 1 ( b) gives 19.6 g (41%) of pale yellow-orange N-acetyl acid;
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-trans-4-propoxy-L-prolin-propylester, kogepunkt 155-165°C (0,2 mm).-trans-4-propoxy-L-proline propyl ester, bp 155-165 ° C (0.2 mm).
b) N-Acetyl-trans-4-propoxy-L-prolinb) N-Acetyl-trans-4-propoxy-L-proline
En opløsning af 6 g (0,15 mol) natriumhydroxid i 5 150 ml vand sættes til 19,4 g (0,075 mol) N-acetyl-trans-4- -propoxy-L-prolin-propylester, hvilket giver en svagt orange opløsning. Efter henstand natten over ved stuetemperatur ekstraheres opløsningen med 60 ml ethylacetat (vaskevæsken kasseres), gøres derefter sur med 1:1 saltsyre, mættes der-10 · efter med natriumchlorid og ekstraheres med 50 ml chloroform (3 gange), De organiske faser forenes, tørres, (MgSO^), filtreres, og opløsningsmidlet afdampes, hvilket giver 12,6 g af en brun olie. Denne opløses i 80 ml ethylacetat og béhandles med en opløsning af 10,7 g dicyclohexylamin i 15 20 ml ethylacetat. Saltet krystalliserer ved stuetempera tur. Efter henstand natten ovér under køling filtreres dicy clohexylaminsaltet og vaskes med koldt ethylacetat, hvilket giver 17,3 g næsten farveløst fast dicyclohexylaminsalt, smeltepunkt 148-153°C. Omkrystallisation af dette materi-20 ale ud fra 125 ml ethylacetat giver 14,5 g farveløst dicyclohexylaminsalt, smeltepunkt 157-159°C [a]^ -30° (c, 1% i ethanol).A solution of 6 g (0.15 mole) of sodium hydroxide in 5 150 ml of water is added to 19.4 g (0.075 mole) of N-acetyl-trans-4-propoxy-L-proline propyl ester to give a slightly orange solution . After standing overnight at room temperature, the solution is extracted with 60 ml of ethyl acetate (the wash liquid is discarded), then acidified with 1: 1 hydrochloric acid, then saturated with sodium chloride and extracted with 50 ml of chloroform (3 times), dried, (MgSO 4), filtered and the solvent evaporated to give 12.6 g of a brown oil. This is dissolved in 80 ml of ethyl acetate and treated with a solution of 10.7 g of dicyclohexylamine in 15 ml of ethyl acetate. The salt crystallizes at room temperature. After standing overnight during cooling, the dicy clohexylamine salt is filtered and washed with cold ethyl acetate to give 17.3 g of almost colorless solid dicyclohexylamine salt, mp 148-153 ° C. Recrystallization of this material from 125 ml of ethyl acetate gives 14.5 g of colorless dicyclohexylamine salt, mp 157-159 ° C [α] D -30 ° (c, 1% in ethanol).
Analyse: Beregnet for C]_oH17N04 * C12H23^: ^ ^6/63, H 10,17, N 7,07.Analysis: Calculated for C ]oH17NO4 * C12H23H: δ 6/63, H 10.17, N 7.07.
25 Fundet: C 66,47, H 10,22, N 7,06.Found: C 66.47, H 10.22, N 7.06.
De 14,4 g dicyclohexylaminsalt omdannes til den fri syre ved at pulverisere dette, suspendere i 100 ml ethylacetat og behandle opslæmningen portionsvis med 100 ml 10% ka-30 liumbisulfat. Den organiske fase skilles fra, og den van dige fase ekstraheres med 100 ml ethylacetat (2 gange). De organiske faser forenes, tørres, (MgSO^), filtreres, og opløsningsmidlet afdampes, hvilket giver 6,7 g (41%) N-acetyl--trans-4-propoxy-L-prolin som en svagt brun væske.The 14.4 g of dicyclohexylamine salt is converted to the free acid by pulverizing it, suspending in 100 ml of ethyl acetate and treating the slurry portionwise with 100 ml of 10% potassium bisulfate. The organic phase is separated and the aqueous phase is extracted with 100 ml of ethyl acetate (2 times). The organic phases are combined, dried, (MgSO 4), filtered and the solvent is evaporated to give 6.7 g (41%) of N-acetyl-trans-4-propoxy-L-proline as a slightly brown liquid.
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c) (trans)-1-[D-3-(Acetylthio)-2-methyl-l-oxopropyl]-4-pro-poxy-Ii-prolin 6,4 g N-acetyl-trans-4-propoxy-L-prolin (0,03 mol) behandles med en opløsning af 10 g koncentreret svovlsyre i 5 100 ml vand, og den fremkomne opløsning omrøres og tilbage svales i tre timer. Derefter afkøles opløsningen til 15°C, behandles portionsvis med 12 g natriumcarbonat for at bringe pH på 8,0 og behandles derefter med en opløsning af 5,4 g (0,03 mol) D-3-acetylthio-2-methylpropionylchlorid i 5 ml 10 ether i løbet af 10 minutter, medens der tilsættes 7 g natriumcarbonat for at holde pH på ca. 8,0. Derefter omrøres blandingen i isbad i 30 minutter og ved stuetemperatur i en time. Produktet isoleres derpå og renses som et dicyclohexylamin-salt ved fremgangsmåden ifølge eksempel 3, hvilket giver 6,3 15 g dicyclohexylaminsalt, smeltepunkt 165-167°C (ud fra aceto-nitril) , [a]^5 -56°C (c, 1% i ethanol).c) (trans) -1- [D-3- (Acetylthio) -2-methyl-1-oxopropyl] -4-propoxy-1-proline 6.4 g N-acetyl-trans-4-propoxy-L -proline (0.03 mol) is treated with a solution of 10 g of concentrated sulfuric acid in 5 100 ml of water and the resulting solution is stirred and refluxed for three hours. Then the solution is cooled to 15 ° C, treated portionwise with 12 g of sodium carbonate to bring the pH to 8.0, and then treated with a solution of 5.4 g (0.03 mole) of D-3-acetylthio-2-methylpropionyl chloride in 5 10 ml of ether over 10 minutes, while adding 7 g of sodium carbonate to maintain the pH of approx. 8.0. Then the mixture is stirred in an ice bath for 30 minutes and at room temperature for one hour. The product is then isolated and purified as a dicyclohexylamine salt by the procedure of Example 3 to give 6.3 g of dicyclohexylamine salt, mp 165-167 ° C (from acetonitrile), [α] 5 -56 ° C (c , 1% in ethanol).
Analyse: Beregnet for . Cj_2®23^: C 62,62, H 9,30, N 5,61, S 6,43.Analysis: Calculated for. C 21 F 23: C 62.62, H 9.30, N 5.61, S 6.43.
Fundet: C 62,35, H 9,48, 20 N 5,88, S 6,45.Found: C, 62.35; H, 9.48; N, 5.88; S, 6.45.
De 6,1 g dicyclohexylaminsalt omdannes til den fri syre ved at blive suspenderet i 60 ml ethylacetat, afkølet i isbad og behandles med 60 ml 10% kaliumbisulfat. Lagene adskilles, og den vandige fase ekstraheres med 60 ml ethylace-25 tat (2 gange). De organiske faser forenes, tørres (MgSO^), filtreres, og opløsningsmidlet afdampes, hvilket giver 4,0 g (42%) (trans)-1-[D-3-(acetylthio)-2-methyl-l-oxopropyl]-4--propoxy-L-prolin som en næsten farveløs sirup.The 6.1 g of dicyclohexylamine salt is converted to the free acid by being suspended in 60 ml of ethyl acetate, cooled in an ice bath and treated with 60 ml of 10% potassium bisulfate. The layers are separated and the aqueous phase is extracted with 60 ml of ethyl acetate (2 times). The organic phases are combined, dried (MgSO 4), filtered and the solvent is evaporated to give 4.0 g (42%) of (trans) -1- [D-3- (acetylthio) -2-methyl-1-oxopropyl] -4 - propoxy-L-proline as an almost colorless syrup.
30 Eksempel 10 L-(D-3-Mercapto-2-methyl-l-oxopropyl)-trans-4-propoxy-L-prolinExample 10 L- (D-3-Mercapto-2-methyl-1-oxopropyl) -trans-4-propoxy-L-proline
Hydrolyse af 4,0 g (trans)-1-[D-3-(acetylthio)-2--methyl-l-oxopropyl]-4-propoxy-L-prolin med 8 ml koncentreret ammoniak i 20 ml vand under argon efter den i eksempel 4 an-35 givne fremgangsmåde giver 3,42 g (97%) 1-(D-3-mercapto-2-meth- 21Hydrolysis of 4.0 g of (trans) -1- [D-3- (acetylthio) -2-methyl-1-oxopropyl] -4-propoxy-L-proline with 8 ml of concentrated ammonia in 20 ml of water under argon after The procedure given in Example 4 gives 3.42 g (97%) of 1- (D-3-mercapto-2-meth-21
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yl-l-oxopropyl)-trans-4-propoxy-L-prolin som en næsten farveløs sirup, [a]^ -72° (c, 1% i ethanol).1-yl-1-oxopropyl) -trans-4-propoxy-L-proline as an almost colorless syrup, [α] D -72 ° (c, 1% in ethanol).
Analyse: Beregnet for · 1/4 H^O: C 51,49, H 9,74, N 5,05, S 11,46.Analysis: Calculated for 1/4 H 2 O: C 51.49, H 9.74, N 5.05, S 11.46.
5 Fundet: C 51,66, H 7,76, N 5,94, S 10,51.Found: C, 51.66; H, 7.76; N, 5.94; S, 10.51.
Eksempel HExample H
(cis)-4-(4-Fluorphenoxy)-!-(D-3-mercapto-2-methyl-l-oxopropyl)-10 -L-prolin a) (cis)-4-(4-Fluorphenoxy)-L-prolin(cis) -4- (4-Fluorophenoxy) -1- (D-3-mercapto-2-methyl-1-oxopropyl) -10-L-proline a) (cis) -4- (4-Fluorophenoxy) -L proline
Til en opløsning af 8,4 g (0,024 mol) N-carbobenz-oxy-trans-4-hydroxy-L-prolin-benzylester (Baer m.fl., Can. J. Biochem. & Phys., 37, 583 (1959)), 4,0 g (0,036 mol) 4-fluor-15 phenol og 9,27 g (0,036 mol) triphenylphosphin i 75 ml tør tetrahydrofuran sættes dråbevis i løbet af en time 6,2 g (0,036 mol) diethylazodicarboxylat i 25 ml tetrahydrofuran. Opløsningen henstår under omrøring natten over ved stuetemperatur. Blandingen inddampes til tørhed, og der tilsættes 20 100 ml ether til remanensen. Et bundfald af triphenylphoshin og diethylazodicarboxylat filtreres fra. Søjlechromatrografi (silicagel) fraskiller 8,1 g af en blanding indholdende ca.To a solution of 8.4 g (0.024 mole) of N-carbobenzoxy-trans-4-hydroxy-L-proline benzyl ester (Baer et al., Can. J. Biochem. & Phys., 37, 583 ( 1959), 4.0 g (0.036 mole) of 4-fluoro-phenol and 9.27 g (0.036 mole) of triphenylphosphine in 75 ml of dry tetrahydrofuran are added dropwise over one hour to 6.2 g (0.036 mole) of diethyl azodicarboxylate. 25 ml of tetrahydrofuran. The solution is left to stir overnight at room temperature. The mixture is evaporated to dryness and 20 ml of ether is added to the residue. A precipitate of triphenylphoshine and diethyl azodicarboxylate is filtered off. Column chromatography (silica gel) separates 8.1 g of a mixture containing approx.
70% N-carbobenzoxy-cis-4-(4-fluorphenoxy)-L-prolin-benzylester. En opløsning af 7,5 g af ovennævnte benzylester-25 holdige blanding hydrogeneres ved 1 atm (stuetemperatur) med 0,8 g 10% pd/C. Der dannes et hvidt bundfald under reaktionen. Efter at hydrogenoptagelsen er ophørt, filtreres blandingen, og filterkagen udvaskes med tre 125 ml-portioner varm methanol. Methanolopløsningen inddampes til tørhed, hvilket 30 giver 3,2 g cis-4-(4-fluorphenoxy)-L-prolin, smeltepunkt 235-236°C.70% N-carbobenzoxy-cis-4- (4-fluorophenoxy) -L-proline-benzyl ester. A solution of 7.5 g of the above-mentioned benzyl ester-containing mixture is hydrogenated at 1 atm (room temperature) with 0.8 g of 10% pd / C. A white precipitate forms during the reaction. After the hydrogen uptake has ceased, the mixture is filtered and the filter cake washed out with three 125 ml portions of hot methanol. The methanol solution is evaporated to dryness to give 3.2 g of cis-4- (4-fluorophenoxy) -L-proline, mp 235-236 ° C.
Analyse: Beregnet for C^H^FNO^. 1/3 E^O: C 57,14, H 5,48, N 6,06, F 8,22.Analysis: Calculated for C ^H ^FNO ^. 1/3 E + O: C 57.14, H 5.48, N 6.06, F 8.22.
Fundet: C 56,94, H 5,19, N 5,94, F 7,97.Found: C 56.94, H 5.19, N 5.94, F 7.97.
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b) I-[D-3-(Acetylthio)-2-methyl-l-oxopropyl]-cis-4-(4-fluor-phenoxy)-L-prolinb) 1- [D-3- (Acetylthio) -2-methyl-1-oxopropyl] -cis-4- (4-fluoro-phenoxy) -L-proline
Til en suspension af 2,25 g (0,01 mol) cis-4-(4--fluorphenoxy)-L-prolin i 125 ml tør pyridin ved stuetempera-5 tur sættes 1,0 g (0,01 mol) triethylamin og 2 g (0,011 mol) ... D-3-(acetylthio)-2-methylpropionylchlorid. Efter omrøring natten over ved stuetemperatur inddampes blandingen til tørhed. Remanensen tages op i vand, dækkes med ether og gøres sur med 10% saltsyre. Vandlaget ekstraheres gentagne gange 10 med ether, etherlagene forenes, vaskes med vand, tørres (Na2SO^) og inddampes til tørhed, hvilket giver 3,9 g remanens. Remanensen chromatograferes på 250 ml silicagel med ether, hvilket giver en fraktion indeholdende det ønskede produkt. Søjlen vaskes med methanol, og methanolvaskevæsken 15 rechromatograferes på en kort søjle af silicagel, hvilket giver yderligerere produkt. Denne proces gentages endnu engang, hvilket ialt giver 1,2 g rent 1-[D-3-(acetylthio)-2-me-thyl-l-oxopropyl]-cis-4-(4-fluorphenoxy)-L-prolin.To a suspension of 2.25 g (0.01 mole) of cis-4- (4-fluorophenoxy) -L-proline in 125 ml of dry pyridine at room temperature is added 1.0 g (0.01 mole) of triethylamine. and 2 g (0.011 mole) of D-3- (acetylthio) -2-methylpropionyl chloride. After stirring overnight at room temperature, the mixture is evaporated to dryness. The residue is taken up in water, covered with ether and acidified with 10% hydrochloric acid. The water layer is repeatedly extracted with ether, the ether layers are combined, washed with water, dried (Na 2 SO 4) and evaporated to dryness to give 3.9 g of residue. The residue is chromatographed on 250 ml of silica gel with ether to give a fraction containing the desired product. The column is washed with methanol and the methanol wash liquid is rechromatographed on a short column of silica gel to give further product. This process is repeated again, giving a total of 1.2 g of pure 1- [D-3- (acetylthio) -2-methyl-1-oxopropyl] -cis-4- (4-fluorophenoxy) -L-proline.
c) (cis)-4-(4-Fluorphenoxy)-1-(D-3-mercapto-2-methyl-l-oxo-20 propyl)-L-prolin 1,2 g 1-[D-3-(acetylthio)-2-methyl-l-oxopropyl]--cis-4-(4-fluorphenoxy)-L-prolin opløses i 25 ml methanol og behandles med 5 ml koncentreret ammoniak under argon i 40 minutter. De flygtige stoffer fjernes, og remanensen dækkes 25 med ethylacetat. Vandlaget gøres surt med 10% saltsyre.c) (cis) -4- (4-Fluorophenoxy) -1- (D-3-mercapto-2-methyl-1-oxo-propyl) -L-proline 1.2 g 1- [D-3- ( acetylthio) -2-methyl-1-oxopropyl] - cis-4- (4-fluorophenoxy) -L-proline is dissolved in 25 ml of methanol and treated with 5 ml of concentrated ammonia under argon for 40 minutes. The volatiles are removed and the residue is covered with ethyl acetate. The water layer is acidified with 10% hydrochloric acid.
Lagene skilles, og det sure lag vaskes med ethylacetat. De forenede organiske lag befries med vand (2 gange, mættet natriumchloridopløsning (2 gange) og tørres (Na2SO^). Opløsningsmidlet afdampes, hvilket giver 1,1 g af en fast skum-30 remanens bestående af cis-4-(4-fluorphenoxy)-1-(D-3-mercapto--2-methyl-1-oxopropy1)-L-prolin.The layers are separated and the acidic layer is washed with ethyl acetate. The combined organic layers are liberated with water (2 times, saturated sodium chloride solution (2 times) and dried (Na 2 SO 4)). The solvent is evaporated to give 1.1 g of a solid foam residue consisting of cis-4- (4-fluorophenoxy) ) -1- (D-3-mercapto - 2-methyl-1-oxopropy1) -L-proline.
Analyse: Beregnet for C-^H^gFNO . 1/3 E^O: C 54,04, H 5,70, N 4,20, F 5,70, S 9,60.Analysis: Calculated for C- HH ^ gFNO. 1/3 E + O: C 54.04, H 5.70, N 4.20, F 5.70, S 9.60.
Fundet: C 54,04, H 5,71, N 4,05, F 5,40, S 9,61.Found: C, 54.04; H, 5.71; N, 4.05; F, 5.40; S, 9.61.
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Tyndtlagschromatografi viser produktet ved 0,30 'som påvist ved UV-lys, SH-reagens (gul plet) og vanillin (gul plet), [a]^ -80° (c, 1% i chloroform), 5 Eksempel 12 (cis)-4-(4-Fluorphenylthio)-1-(D-3-mercapto-2-methyl-l—oxo- propyl)-L-prolinThin layer chromatography shows the product at 0.30 'as detected by UV light, SH reagent (yellow spot) and vanillin (yellow spot), [α] D -80 ° (c, 1% in chloroform), Example 12 (cis ) -4- (4-Fluorophenylthio) -1- (D-3-mercapto-2-methyl-1-oxopropyl) -L-proline
Ved anvendelse af den i eksempel 11 anførte fremgangsmåde med ved i stedet for 4-fluorphenolen i del (a) at 10 anvende en ækvivalent mængde 4-fluorphenylmercaptan fås (cis)-4-(4-fluorphenylthio)-l-(D-3-mercapto-2-methy1-1-oxo-propyl)-L-prolin, smp. 242-243° (sønderdeling) som adamam— tanaminsalt efter omkrystallisation fra (1:1) chloroform/me- 25 o thanolblanding fortyndet med ether. [α] -51,8 (c = 0,5% i ·Using the procedure of Example 11 by using an equivalent amount of 4-fluorophenyl mercaptan instead of the 4-fluorophenol in part (a), (cis) -4- (4-fluorophenylthio) -1- (D-3) is obtained. -mercapto-2-methyl-1-oxo-propyl) -L-proline, m.p. 242-243 ° (dec.) As adamam-tanamine salt after recrystallization from (1: 1) chloroform / methanol mixture diluted with ether. [α] -51.8 (c = 0.5% i
pr Dper D
15 methanol). Fri syre [α]β -42,5 (c = 1%'absolut ethanol,) .(Methanol). Free acid [α] β -42.5 (c = 1% absolute ethanol).
Eksempel 13 1-(D-3-Mercapto-2-methyl-l-oxopropyl)-cis-4-phenylthio-L- -prolin 20 a) N-Carbobenzyloxy-cis-4-phenylthio-L-prolin-methylester 0,85 g natriummetal (©-,037 mol) ‘opløses i 40 ml absolut ethanol. Hertil sættes under omrøring 3,7 ml (0,036 mol) thiophenol efterfulgt af 7,5 g (0,017 mol) N--carbobenzyloxy-trans-4-tosyloxy-L-prolin-methylester (J„ 25 Am. Chem. Soc., 79, 191 (1957)). Sidstnævnte forbindelse går gradvis i opløsning, men snart efter fraskilles et fast produkt. Efter omrøring i 4 timer og henstand natten over ved stuetemperatur fjernes størstedelen af ethanolen i em roterende fordamper. Den hovedsagelig faste remanens ©m-30 røres med 120 ml diehlormethan ©g 60 ml vand. Lagene adskilles (noget methanol tilsættes for at fremme nedbrydningen af emulsioner), og den vandige fase ekstraheres med y-derligere diehlormethan (2 x 60 ml). De forenede organiske faser vaskes med 100 ml mættet matriumchloridopløsning, 35 tørres (MgSO^), og opløsningsmidlet afdampes, hvilket giverExample 13 1- (D-3-Mercapto-2-methyl-1-oxopropyl) -cis-4-phenylthio-L-proline a) N-Carbobenzyloxy-cis-4-phenylthio-L-proline methyl ester 0, Dissolve 85 g of sodium metal (© - 037 mol) in 40 ml of absolute ethanol. To this is added 3.7 ml (0.036 mol) of thiophenol, followed by 7.5 g (0.017 mol) of N - carbobenzyloxy-trans-4-tosyloxy-L-proline methyl ester (J. Am. Chem. Soc. 79, 191 (1957)). The latter compound gradually dissolves, but soon after a solid product is separated. After stirring for 4 hours and standing overnight at room temperature, most of the ethanol in the rotary evaporator is removed. The essentially solid residue © m-30 is stirred with 120 ml of Diehlormethane © g of 60 ml of water. The layers are separated (some methanol is added to promote the decomposition of emulsions) and the aqueous phase is extracted with additional dichloromethane (2 x 60 ml). The combined organic phases are washed with 100 ml of saturated sodium chloride solution, dried (MgSO 4) and the solvent evaporated to give
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6.5 g (100%) N-carbobenzyloxy-cis-4-phenylthio-L-prolin--methylester som en svagt gul viskos olie.6.5 g (100%) of N-carbobenzyloxy-cis-4-phenylthio-L-proline - methyl ester as a pale yellow viscous oil.
b) N-Carbobenzyloxy-cis-4-phenylthio-L-prolinb) N-Carbobenzyloxy-cis-4-phenylthio-L-proline
Methylesterproduktet fra del (a) (6,5 g, 0,017 5 mol) opløses i 55 ml methanol, behandles portionsvis ved -1 til 4°C med 13 ml (0,026 mol) 2N natriumhydroxid, omrøres ved 0°C i en time og holdes ved stuetemperatur i ca. 16 timer. Efter af ca. halvdelen af opløsningsmidlet er fjernet på en roterende fordamper,fortyndes den afkølede opløsning 10 med 100 ml vand, vaskes med 60 ml ether (vaskevæsken kasseres), et lag af 70 ml ethylacetat hældes over, omrøres, afkøles og gøres sur med 4,8 ml 1:1 saltsyre. Efter adskillelse ekstraheres den vandige fase med yderligere ethylacetat (3 x 40 ml), og de forenede organiske lag tørres (MgS04) 15 og inddampes, hvilket giver 5,9 g af en lys gul viskos olie.The methyl ester product of part (a) (6.5 g, 0.017 mol) is dissolved in 55 ml of methanol, treated portionwise at -1 to 4 ° C with 13 ml (0.026 mol) of 2N sodium hydroxide, stirred at 0 ° C for one hour and kept at room temperature for approx. 16 hours. After of approx. half of the solvent is removed on a rotary evaporator, dilute the cooled solution 10 with 100 ml of water, wash with 60 ml of ether (discard the wash liquid), pour a layer of 70 ml of ethyl acetate, stir, cool and acidify with 4.8 ml 1: 1 hydrochloric acid. After separation, the aqueous phase is extracted with additional ethyl acetate (3 x 40 ml) and the combined organic layers are dried (MgSO 4) and evaporated to give 5.9 g of a light yellow viscous oil.
Denne opløses i 30 ml ethanol, behandles med 1,9 g cyclohexyl-amin i 3 ml ethanol og fortyndes til 330 ml med ether. Efter podning fraskilles det krystallinske cyclohexylaminsalt.This is dissolved in 30 ml of ethanol, treated with 1.9 g of cyclohexylamine in 3 ml of ethanol and diluted to 330 ml with ether. After grafting, the crystalline cyclohexylamine salt is separated.
Dette vejer efter afkøling i ca. 16 timer 5,3 g, smelte-20 punkt 148-151°C (s. 135°C). Dette materiale forenes med 1.5 g identisk produkt fra et tidligere eksperiment, omrøres med 200 ml kogende acetonitril og afkøles, hvilket giver 6,3 g farveløst cyclohexylaminsalt, smeltepunkt 152-155°C (s. 137°C); [a]^6 -24° (c, 1% i ethanol).This weighs after cooling for approx. 16 hours 5.3 g, m.p. 148-151 ° C (p. 135 ° C). This material is combined with 1.5 g of identical product from a previous experiment, stirred with 200 ml of boiling acetonitrile and cooled to give 6.3 g of colorless cyclohexylamine salt, mp 152-155 ° C (p. 137 ° C); [.alpha.] @ 6 -24 ° (c, 1% in ethanol).
25 Dette cyclohexylaminsalt suspenderes i 25 ml e- thylacetat, omrøres og behandles med 25 ml N saltsyre.This cyclohexylamine salt is suspended in 25 ml of ethyl acetate, stirred and treated with 25 ml of N hydrochloric acid.
Når der er opnået to klare lag, adskilles de, og den vandige fase ekstraheres med yderligere ethylacetat ( 3 x 25 ml). De forenede organiske lag tørres (MgS04), og op-30 løsningsmidlet afdampes, hvilket giver 5,0 g (65%) N-car-bobenzyloxy-cis-4-phenylthio-L-prolin som en næsten farveløs, meget viskos sirup.When two clear layers are obtained, they are separated and the aqueous phase is extracted with additional ethyl acetate (3 x 25 ml). The combined organic layers are dried (MgSO 4) and the solvent is evaporated to give 5.0 g (65%) of N-carbobenzyloxy-cis-4-phenylthio-L-proline as an almost colorless, highly viscous syrup.
c) (cis)-4-Phenylthio-L-prolin-hydrochlorid 4,9 g N-carbobenzyloxy-cis-4-phenylthio-L-prolin 35 (0,014 mol) behandles med 25 ml hydrogenbromid i eddikesy-c) (cis) -4-Phenylthio-L-proline hydrochloride 4.9 g of N-carbobenzyloxy-cis-4-phenylthio-L-proline (0.014 mol) are treated with 25 ml of hydrogen bromide in acetic acid.
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re (30-32%), tilproppes løst og omrøres magnetisk. Efter 1 time fortyndes den orangegule opløsning til 250 ml med ether, for at udfælde produktet som en tung olie, der gradvis krystallisere efter podning, gnidning og afkøling. Ef-5 ter omrøring i isbad i en time filtreres materialet under nitrogen, vaskes med ether,.suspenderes i frisk ether, afkøles i ca. 16 timer og filtreres igen, hvilket giver 3,2 g (77%) farveløst fast (cis)-4-phenylthio-L-prolin-hydrdb.ro-mid, smeltepunkt 106-109°C (s. 99°C), [a]^* "3° (c, 1% i 10 methanol).re (30-32%), loosely plugged and magnetically stirred. After 1 hour, the orange-yellow solution is diluted to 250 ml with ether to precipitate the product as a heavy oil which gradually crystallizes after grafting, rubbing and cooling. After stirring in an ice bath for one hour, the material is filtered under nitrogen, washed with ether, suspended in fresh ether, cooled for approx. 16 hours and filtered again to give 3.2 g (77%) of colorless solid (cis) -4-phenylthio-L-proline hydrobromide, mp 106-109 ° C (p. 99 ° C), [α] D 20 ° (c, 1% in methanol).
d) 1-[D-3-(Acetylthio)-2-methyl-l-oxopropyl]-cis-4-phenyl·-thio-L-prolind) 1- [D-3- (Acetylthio) -2-methyl-1-oxopropyl] -cis-4-phenyl · -thio-L-proline
Omsætning af 3,0 g (0,0094 mol) (cis)-4-phenylthio--L-prolin-hydrobromid og 2,0 g (0,011 mol) D-3-acetylthio-2-15 -methylpropionylchlorid i 25 ml vand som beskrevet i eksempel 1(d) (under anvendelse af ca. 15 ml 20% natriumcarbonat-opløsning for at holde pH på 8,0-8,4) giver 3,8 g af en svagt gul viskos olie. Dicyclohexylaminsaltet (fremstillet i 30 ml ethylacetat under anvendelse af 1,8 g dicyclohexylamin) 2o vejer 2,9 g (isoleret i to udbytter), smeltepunkt 184-188°C (s. 180°C). Efter triturering med 15 ml acetonitil fås 2,4 g farveløst fast dicyclohexylaminsalt, smeltepunkt 184-186°C (s. 180°C) , [a]p6 -75° (c, 1% i ethanol).Reaction of 3.0 g (0.0094 mol) (cis) -4-phenylthio - L-proline hydrobromide and 2.0 g (0.011 mol) of D-3-acetylthio-2-15-methylpropionyl chloride in 25 ml of water as described in Example 1 (d) (using about 15 ml of 20% sodium carbonate solution to maintain the pH of 8.0-8.4) gives 3.8 g of a pale yellow viscous oil. The dicyclohexylamine salt (prepared in 30 ml of ethyl acetate using 1.8 g of dicyclohexylamine) 20o weighs 2.9 g (isolated in two yields), mp 184-188 ° C (p. 180 ° C). After trituration with 15 ml of acetonitil, 2.4 g of colorless solid dicyclohexylamine salt, m.p. 184-186 ° C (p. 180 ° C), [a] p6 -75 ° (c, 1% in ethanol) is obtained.
Dette cieyclohexylaminsalt behandles med 30 .ml 10% 25 kaliumbisulfat og ekstraheres i ethylacetat som beskrevet i eksempel 1, hvilket giver 2,0 g (59%) glaslignende 1-ID-3-- (acetylthio) -2-methyl-l-oxopropyl] -cis-4-phenylthio-L-pro-ling.This cieyclohexylamine salt is treated with 30 ml of 10% potassium bisulfate and extracted into ethyl acetate as described in Example 1 to give 2.0 g (59%) of glass-like 1-ID-3- (acetylthio) -2-methyl-1-oxopropyl ] -cis-4-phenylthio-L-pro-ling.
e) 1- (D-3-Mercapto-2-methyl-l-oxopropyl) -cis-4-phenyli:hiD-30 -L-prolin 1- [D-3- (Acetylthio) -2-methyl-l-oxopropyl] -ciLs-4--phenylthio-L-prolinet (2,0 g, 0,0042 mol) behandles med 3,5 ml koncentreret ammoniak i 8,5 ml vand ved anvendelse af den i eksempel 2 anførte fremgangsmåde (det faste ammoniumsalt 35 af produktet skilles fra reaktionsblandingen), hvilket gi- 26e) 1- (D-3-Mercapto-2-methyl-1-oxopropyl) -cis-4-phenyl: hiD-30-L-proline 1- [D-3- (Acetylthio) -2-methyl-1- The oxopropyl] -CiLs-4-phenylthio-L-proline (2.0 g, 0.0042 mol) is treated with 3.5 ml of concentrated ammonia in 8.5 ml of water using the procedure described in Example 2 (the solid ammonium salt (35 of the product is separated from the reaction mixture), giving 26
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o ver 1,35 g (100%) viskos sirupsagtigt 1-(D-3-mercapto-2-meth-- yl-l-oxopropyl)-cis-4-phenylthio-L-prolin, [a]^6 -43° (c, 1% i ethanol) 5 Eksempel 14 1-(D-3-Mercapto-2-methyl-l-oxopropyl)-cis-4-(4-chlorphenyl- thio)-L-prolinover 1.35 g (100%) of viscous syrupy 1- (D-3-mercapto-2-methyl-1-oxopropyl) -cis-4-phenylthio-L-proline, [α] 6 -43 ° (c, 1% in ethanol) Example 14 1- (D-3-Mercapto-2-methyl-1-oxopropyl) -cis-4- (4-chlorophenylthio) -L-proline
Ved anvendelse af den i eksempel 13 anførte fremgangsmåde, men ved i stedet for thiophenolen i del (a) at an-10 vende en ækvivalent mængde 4-chlorphenylmercaptan fås 1-(D--3-mercapto-2-methyl-l-oxopropyl)-cis-4-(4-chlorphenylthio)--L-prolin, smp. 241-242°C (sønderdeling) som adamantanamin- salt efter omkrystallisation fra (1:1) chloroform/methanol- 25 o blanding fortyndet med ether. [α]η -55,4 (c = 0,5% i methanol). 25 o - 15 Fri syre [a]D - 38,1 (c = 1% i absolut ethanol).Using the procedure of Example 13, but using the equivalent of 4-chlorophenylmercaptan instead of the thiophenol in part (a), 1- (D-3-mercapto-2-methyl-1-oxopropyl) is obtained. ) -cis-4- (4-chlorophenylthio) - L-proline, m.p. 241-242 ° C (dec.) As adamantanamine salt after recrystallization from (1: 1) chloroform / methanol-o mixture diluted with ether. [α] η -55.4 (c = 0.5% in methanol). 25 - 15 Free Acid [a] D - 38.1 (c = 1% in absolute ethanol).
Eksempel 15 (trans) -1- (3-Mercapto-l-o'xopropyl)-3-methylthio-D,L-prolin a) 1,2-Dehydroprolin-t-butylester 20 Til en omrørt opløsning af 34,2 g (0,20 mol) pro- lin-t-butylester i 600 ml ether ved -5 til 0°C sættes dråbevis i løbet af 10 minutter 21,7 g (23,9 ml, 0,20 mol) frisk fremstillet t-butylhypochlorit (Org. Syn., Coll. bd. V, 184 (1973)]. Under tilsætningen holdes temperaturen på -5 til 25 0°C. Efter at tilsætningen er tilendebragt omrøres opløs ningen ved denne temperatur i yderligere fem minutter.Example 15 (trans) -1- (3-Mercapto-1-oxopropyl) -3-methylthio-D, L-proline a) 1,2-Dehydroproline t-butyl ester To a stirred solution of 34.2 g (0.20 mole) of proline t-butyl ester in 600 ml of ether at -5 to 0 ° C is added dropwise over 10 minutes to 21.7 g (23.9 ml, 0.20 mole) of freshly prepared t butyl hypochlorite (Org. Syn., Coll. bd. V, 184 (1973)]. During the addition, the temperature is maintained at -5 to 25 ° C. After completion of the addition, the solution is stirred at this temperature for an additional five minutes.
Til den kraftigt omrørte opløsning sættes hurtigt ( oj 3-5 minutter) en opløsning af 7,8 g (0,20 mol) kalium i frisk destilleret tør (Cal^) t-butanol. Efter tilsætningen 30 ligger reaktionsblandingens temperatur omkring 18°C. Reaktionsbeholderen fjernes fra kølebadet og omrøres i 30 minutter. Reaktionsblandingen filtreres gennem "Celite" (diatoméjord), og filtratet inddampes i vakuum. Remanensen tages op i ether og vaskes med flere portioner vand. Etheropløs-35 ningen tørres og inddampes i vakuum til 31,6 g gul væske.To the vigorously stirred solution, a solution of 7.8 g (0.20 mol) of potassium in freshly distilled dry (Cal After addition 30, the temperature of the reaction mixture is about 18 ° C. The reaction vessel is removed from the cooling bath and stirred for 30 minutes. The reaction mixture is filtered through "Celite" (diatomaceous earth) and the filtrate is evaporated in vacuo. The residue is taken up in ether and washed with several portions of water. The ether solution is dried and evaporated in vacuo to 31.6 g of yellow liquid.
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Der tilsættes spor af hydroquinon, og det rå produkt destilleres, hvilket giver 22,4 g 1,2-dehydroprolin-t-butylester (66%), kogepunkt 60-62°C/0,l mm.Traces of hydroquinone are added and the crude product distilled to give 22.4 g of 1,2-dehydroproline t-butyl ester (66%), boiling point 60-62 ° C / 0.1 mm.
b) l-Benzyloxycarbonyl-4,5-dihydro-IH-pyrrol-2-carboxylsyre-5 -t-butylesterb) 1-Benzyloxycarbonyl-4,5-dihydro-1H-pyrrole-2-carboxylic acid 5-t-butyl ester
En opløsning af 16,9 g (0,1 mol) 1,2-dehydroprol.in--t-butylester i 70 ml dichlormethan afkøles til -10°C under argon. En opløsning af frisk destilleret benzylchlorformiat (14,2 ml, 0,1 mol, kogepunkt 62-64°C/0,4 mm) i 70 ml dicblor-10 methan tilsættes dråbevis i løbet af 30 minutter. Efter omrøring i kulde i yderligere 30 minutter tilsættes en opløsning af 15,22 g (0,1 mol) l,5-d±azabicyclo[5,4,0]undec-5-en i 70 ml dichlormethan i løbet af 20 minutter. Derefter fjernes kølebadet, og blandingen omrøres ved stuetemperatur i 15 en time. Efter to gange vask med kold fortyndet saltsyre og én gang med mættet natriumcarbonatopløsning tørres opløsningen i vakuum, hvilket giver 18,2 g (60%) 1-benzyloxycar-bonyl-4,5-dihydro-lH-pyrrol-2-carboxylsyre-t-butylester som en svagt gul olie.A solution of 16.9 g (0.1 mole) of 1,2-dehydroproline-t-butyl ester in 70 ml of dichloromethane is cooled to -10 ° C under argon. A solution of freshly distilled benzyl chloroformate (14.2 ml, 0.1 mol, boiling point 62-64 ° C / 0.4 mm) in 70 ml of dicloro-10-methane is added dropwise over 30 minutes. After stirring in the cold for an additional 30 minutes, a solution of 15.22 g (0.1 mole) of 1,5-d ± azabicyclo [5.4.0] undec-5ene in 70 ml of dichloromethane is added over 20 minutes. . Then, the cooling bath is removed and the mixture is stirred at room temperature for 15 hours. After twice washing with cold dilute hydrochloric acid and once with saturated sodium carbonate solution, the solution is dried in vacuo to give 18.2 g (60%) of 1-benzyloxycarbonyl-4,5-dihydro-1H-pyrrole-2-carboxylic acid. butyl ester as a pale yellow oil.
20 c) (trans)-l-Benzyloxycarbonyl-3-methylthio-D,L-prolin-t-bu-tylesterC) (trans) -1-Benzyloxycarbonyl-3-methylthio-D, L-proline t-butyl ester
En opløsning af 18,2 g (0,06 mol) 1-benzyloxycar-bonyl-4,5-dihydro-lH-pyrrol-2-carboxylsyre-t-butylester i 180 ml tør methanol behandles med 3,24 g (0,06 mol) natrium-25 methoxid og afkøles i isbad. Methanthiol bobles langsomt ind i opløsningen i 30 minutter. Blandingen omrøres natten over under argon ved stuetemperatur. Der tilsættes fortyndet vandig eddikesyre, indtil opløsningen er let sur. Der bobles argon gennem opløsningen 1 en time, før den inddamp-30 es til næsten tørhed i vakuum. Der tilsættes ethylacetat, og opløsningen vaskes to gange med mættet natriumcarbonatopløsning, tørres og befries for opløsningsmiddel i vakuum, hvilket giver 17 g gul olie. Denne olie chromatograferes under anvendelse af 300 g silicagel og petroleumether: ether 35 (4:1), hvilket giver 11,1 g (trans)-l-benzyloxycarbonyJL-l- -methylthio-D,L-prolin som en farveløs olie.A solution of 18.2 g (0.06 mol) of 1-benzyloxycarbonyl-4,5-dihydro-1H-pyrrole-2-carboxylic acid t-butyl ester in 180 ml of dry methanol is treated with 3.24 g (0, (6 mol) sodium methoxide and cool in an ice bath. Methanthiol is slowly bubbled into the solution for 30 minutes. The mixture is stirred overnight under argon at room temperature. Dilute aqueous acetic acid is added until the solution is slightly acidic. Argon is bubbled through the solution for 1 hour before evaporating to near dryness in vacuo. Ethyl acetate is added and the solution is washed twice with saturated sodium carbonate solution, dried and free of solvent in vacuo to give 17 g of yellow oil. This oil is chromatographed using 300 g of silica gel and petroleum ether: ether 35 (4: 1) to give 11.1 g of (trans) -1-benzyloxycarbonyJL-1-methylthio-D, L-proline as a colorless oil.
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d) (trans)-3-Methylthio-D,L-prolin 8.4 g (0,024 mol) (trans)-1-benzyloxycarbony1-3--methylthio-D,L-prolin behandles med 45 ml 4N hydrobromsyre i eddikesyre. Efter omrøring i en time ved stuetemperatur 5 tørres opløsningen i vakuum. Der tilsættes en lille smule vand, og dette vaskes to gange med ether. Den vandige opløsning påføres en søjle med 300 ml ion-bytterharpiks, og der ledes vand igennem, indtil eluatet ikke mere er stærkt surt. Derefter elueres produktet med pH 6,5 (vandig pyridinacetat) 10 puffer. Fraktioner, der er positive over for ninhydrin, forenes og lyophiliseres, hvilket giver 3,4 g (88%) hvide fnug.d) (trans) -3-Methylthio-D, L-proline 8.4 g (0.024 mol) (trans) -1-benzyloxycarbonyl-3-methylthio-D, L-proline are treated with 45 ml of 4N hydrobromic acid in acetic acid. After stirring for one hour at room temperature, the solution is dried in vacuo. A small amount of water is added and this is washed twice with ether. The aqueous solution is applied to a column of 300 ml ion exchange resin and water is passed through until the eluate is no longer strongly acidic. The product is then eluted with pH 6.5 (aqueous pyridine acetate) 10 buffer. Ninhydrin positive fractions are combined and lyophilized to give 3.4 g (88%) of white lilacs.
En lille prøve af dette materiale krystalliseres ud fra methanol, hvilket giver (trans)-3-(methylthio-D,L-prolin, smeltepunkt 196-200°C, sønderdeling (s. 192°C).A small sample of this material is crystallized from methanol to give (trans) -3- (methylthio-D, L-proline, m.p. 196-200 ° C, decomp. (P. 192 ° C).
15 Analyse: Beregnet for CgH^C^NS: C 44,70, H 6,88, N 8,69, S 19,89.Analysis: Calculated for CgHH₂ ^N₂: C 44.70, H 6.88, N 8.69, S 19.89.
Fundet: C 44,53, H 7,10, N 8,61, S 19,95.Found: C 44.53, H 7.10, N 8.61, S 19.95.
e) (trans)-1-[3-(Acetylthio)-1-oxopropyl]-3-methylthio-D,L-20 -prolin 3.05 g (0,019 mol) (trans)-3-methylthio-D,L-pro-lin opløses i 19 ml IN natriumcarbonat og fortyndes med 10 ml vand. Opløsningen afkøles i isbad, og under hurtig omrøring tilsættes en opløsning af 3-acetylthiopropionylchlo- 25 rid i 20 ml ether. pH holdes på 8 ved tilsætning af IN natriumcarbonat. Efter 30 minutters forløb holdes pH konstant, og der er tilsat 45 ml natriumcarbonatopløsning. Lagene adskilles, og det vandige lag vaskes én gang med ether.e) (trans) -1- [3- (Acetylthio) -1-oxopropyl] -3-methylthio-D, L-20-proline 3.05 g (0.019 mol) (trans) -3-methylthio-D, L-pro -lin dissolve in 19 ml 1N sodium carbonate and dilute with 10 ml water. The solution is cooled in an ice bath and, with rapid stirring, a solution of 3-acetylthiopropionyl chloride in 20 ml of ether is added. The pH is maintained at 8 by the addition of 1N sodium carbonate. After 30 minutes, the pH is kept constant and 45 ml of sodium carbonate solution is added. The layers are separated and the aqueous layer is washed once with ether.
Det vandige lag gøres derefter surt med 10% kaliumbisulfat-30 opløsning, og produktet ekstraheres i ethylacetat, tørres og befries for opløsningsmiddel i vakuum, hvilket giver 5,2 g olie. Dette materiale chromatograferes på 150 g silicagel under anvendelse af ethylacetat til eluering. 3,85 g af en noget rå (trans)-1-(3-(acetylthio)-1-oxopropyl]-3-methyl-35 thio-D,L-prolin opnås.The aqueous layer is then acidified with 10% potassium bisulfate solution and the product is extracted into ethyl acetate, dried and free of solvent in vacuo to give 5.2 g of oil. This material is chromatographed on 150 g of silica gel using ethyl acetate for elution. 3.85 g of a somewhat crude (trans) -1- (3- (acetylthio) -1-oxopropyl] -3-methyl-thio-D, L-proline is obtained.
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En lille prøve opløses i ether og omdannes til di-cyclohexylaminsaltet, der derefter omkrystalliseres ud fra ethylacetat, hvilket giver (trans)-1-[3-(acetylthio)-1-oxo-propyl]-3-methylthio-D,L-prolin-dicyclohexylaminsalt, smel-5 tepunkt 153-157°C.A small sample is dissolved in ether and converted to the di-cyclohexylamine salt which is then recrystallized from ethyl acetate to give (trans) -1- [3- (acetylthio) -1-oxo-propyl] -3-methylthio-D, L proline-dicyclohexylamine salt, mp 153-157 ° C.
Analyse: Beregnet for C^H^O^NS . (CgH^^NH: C 58,44, H 8,53, N 5,83, S 13,57.Analysis: Calculated for C (CgHH₂ NHNH: C 58.44, H 8.53, N 5.83, S 13.57.
Fundet: C 58,77, H 8,57, N 5,68, S 13,74.Found: C, 58.77; H, 8.57; N, 5.68; S, 13.74.
f) (trans) -1- (3-Mercapto-l-oxopropyl) -3-methylthio-D,L-pro- 10 lin 2,05 g (0,007 mol) (trans)-l-[3-(acetylthio)-1— -oxopropyl]-3-methylthio-D,L-prolin afkøles i isbad under argon og behandles med en kold argon-mættet blanding af 7 ml vand og 7 ml koncentreret ammoniak. Efter omrøring i 30 15 minutter ved 0°C gøres opløsningen sur med saltsyre. Produktet ekstraheres i ethylacetat, tørres og befries for opløsningsmiddel i vakuum, hvilket giver 1,85 g materiale, der bliver delvis krystallinsk ved henstand. Triturering .med ether giver 1,0 g (57%) hvidt krystallinsk produkt. Omkry-20 stallisation ud fra 5 ml ethylacetat giver 0,85 g (trans)--1-(3-mercapto-l-oxopropyl)-3-methylthio-D,L-prolin, smeltepunkt 89-93°C.f) (trans) -1- (3-Mercapto-1-oxopropyl) -3-methylthio-D, L-protein 2.05 g (0.007 mol) (trans) -1- [3- (acetylthio) -1- -oxopropyl] -3-methylthio-D, L-proline is cooled in an ice bath under argon and treated with a cold argon-saturated mixture of 7 ml of water and 7 ml of concentrated ammonia. After stirring for 30 minutes at 0 ° C, the solution is acidified with hydrochloric acid. The product is extracted into ethyl acetate, dried and free from solvent in vacuo to give 1.85 g of material which becomes partially crystalline upon standing. Trituration with ether gives 1.0 g (57%) of white crystalline product. Recrystallization from 5 ml of ethyl acetate gives 0.85 g of (trans) - 1- (3-mercapto-1-oxopropyl) -3-methylthio-D, L-proline, mp 89-93 ° C.
Analyse: Beregnet for CgH^^O^NS : C 43,35, H 6,06, N 5,62, S 25,72.Analysis: Calculated for CgHH₂ ONO: C 43.35, H 6.06, N 5.62, S 25.72.
25 Fundet: G 43,35, H 6,27, N 5,54, S 25,91.Found: G 43.35, H 6.27, N 5.54, S 25.91.
30 35 0 3030 35 0 30
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Eksempel 16 (cis) -4- <ly 1-Dimethylethoxv) -1- (D-3-mercaoto-2-methyl-l-oxo- propyl)-L-prolin (a) N-Carbobenzyloxy-cis-4-(1,1-dimethylethoxy)-L-prolin-methyl-5 esterExample 16 (cis) -4- (1-Dimethylethoxy) -1- (D-3-mercaoto-2-methyl-1-oxopropyl) -L-proline (a) N-Carbobenzyloxy-cis-4- ( 1,1-dimethylethoxy) -L-proline-methyl ester
En opløsning af 6,0 g (0,021 mol) N-carbobenzyloxy--cis-4-hydroxy-L-prolin-methylester i 60 ml methylenchlorid anbringes i en Parr-apparat, omrøres magnetisk, afkøles i et bad af tøris/isopropanol og behandles med ca. 40 ml flydendegjort 10 isobutylen efterfulgt af 0,75 ml koncentreret svovlsyre. Appara-tet lukkes, og reaktionsblandingen får lov at varne op til stuetemperatur under fortsat omrøring. Der forekommer ingen målelig trykstigning. Efter omrøring ved stuetemperatur i 4 dage, åbnes apparatet, og opløsningen (80 ml) fortyndes med 120 ml me-15 thylenchlorid og vaskes med 5 g natriumbicarbonat i 100 ml vand.A solution of 6.0 g (0.021 mol) of N-carbobenzyloxy - cis-4-hydroxy-L-proline methyl ester in 60 ml of methylene chloride is placed in a Parr apparatus, magnetically stirred, cooled in a dry ice / isopropanol bath and treated with approx. 40 ml of liquefied 10 isobutylene followed by 0.75 ml of concentrated sulfuric acid. The apparatus is closed and the reaction mixture is allowed to warm to room temperature with continued stirring. There is no measurable increase in pressure. After stirring at room temperature for 4 days, the apparatus is opened and the solution (80 ml) is diluted with 120 ml of methylene chloride and washed with 5 g of sodium bicarbonate in 100 ml of water.
Den vandige fase returekstraheres med 50 ml methylenchlorid, de organiske lag kombineres og tørres (MgS04), og opløsningsmidlet afdampes, hvilket giver 7,5 g N-carbobenzyloxy-cis-4-(l,l-dimethyl-ethoxv)-L-prolin-methylester som en bleggul olie.The aqueous phase is back extracted with 50 ml of methylene chloride, the organic layers are combined and dried (MgSO 4) and the solvent is evaporated to give 7.5 g of N-carbobenzyloxy-cis-4- (1,1-dimethylethoxy) -L-proline methyl ester as a pale yellow oil.
20 [a]^ ="46° (c, 1% i chloroform).[Α] D = 46 ° (c, 1% in chloroform).
TLC (på silicagel): 0,62 (ethylacetat), 0,43 (7:1 benzen/eddikesyre)TLC (on silica gel): 0.62 (ethyl acetate), 0.43 (7: 1 benzene / acetic acid)
Synliggjort UV, n^-damp.Visible UV, n 2 vapor.
b) N-Carbobenzyloxy-cis-4-(1,1-dimethylethoxy)-L-prolin 25 En omrørt opløsning af methylesterproduktet fra af snit (a) (7,2 g, 0,02 mol) i 15 ml ether afkøles i isvand og behandles portionsvis med 42 ml (0,042 mol) iskoldt N natriumhydroxid. Efter omrøring og afkøling i ialt 6 timer fjernes kølebadet, og omrøringen fortsættes natten over ved stuetemperatur.b) N-Carbobenzyloxy-cis-4- (1,1-dimethylethoxy) -L-proline A stirred solution of the methyl ester product of section (a) (7.2 g, 0.02 mol) in 15 ml of ether is cooled in ice water and treated portionwise with 42 ml (0.042 mol) of ice-cold N sodium hydroxide. After stirring and cooling for a total of 6 hours, the cooling bath is removed and stirring is continued overnight at room temperature.
30 Den klare opløsning vaskes med. 40 ml ether (vask kasseres), der anbringes et lag af 40 ml ethylacetat, omrøres, afkøles og syr-nes med 8 ml 6N saltsyre. Efter adskillelse ekstraheres den vandige fase med yderligere ethylacetat (3 x 40 ml), de organiske lag kombineres og tørres (MgS04), og opløsningsmidlet af-35 dampes,' hvilket giver 6,8 g bleggul viskos olie. Denne olie opløses i 50 ml acetonitril og behandles med en varm opløsning af 3,2 g 1-adamantanamin i 20 ml acetonitril. Det faste adamantan-30 Wash the clear solution with. 40 ml of ether (wash is discarded), a layer of 40 ml of ethyl acetate is stirred, cooled and acidified with 8 ml of 6N hydrochloric acid. After separation, the aqueous phase is extracted with additional ethyl acetate (3 x 40 ml), the organic layers are combined and dried (MgSO 4) and the solvent is evaporated to give 6.8 g of pale yellow viscous oil. This oil is dissolved in 50 ml of acetonitrile and treated with a warm solution of 3.2 g of 1-adamantanamine in 20 ml of acetonitrile. The solid adamantane
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aminsalt udskilles hurtigt. Efter afkøling natten.over filtreres det farveløse salt under nitrogen, vaskes xaed kold aeetoni-tril og ether og tørres i vakuum, hvilket giver 8,8 g N-carbo-benzyloxy-cis-4-(1,1-dimethylethoxy)-L-prolin-adamantanaminsalt, 5 smeltepunkt 228-230°C (sønderdeling), begynder 215°C.amine salt is rapidly excreted. After cooling overnight, the colorless salt is filtered under nitrogen, washed with cold ethyl acetate and ether and dried in vacuo to give 8.8 g of N-carbo-benzyloxy-cis-4- (1,1-dimethylethoxy) -L -proline adamantanamine salt, m.p. 228-230 ° C (decomposition), starts at 215 ° C.
[a]p5 =-28° (c, 1% i methanol).[α] p 5 = -28 ° (c, 1% in methanol).
Analyse: Beregnet for h20: C 67,96, H 8,56, N 5,87.Analysis: Calculated for H 2 O: C 67.96, H 8.56, N 5.87.
Fundet: C 67,77, H 8,54, N 5,93.Found: C, 67.77; H, 8.54; N, 5.93.
10 Behandling af ovennævnte adamantanaminsalt (8,5 g) med syre giver 5,5 g N-carbobenzyloxy-cis-4-(1,1-dimethylethoxy)-L--prolin som en næsten farveløs viskos sirup.Treatment of the above adamantanamine salt (8.5 g) with acid gives 5.5 g of N-carbobenzyloxy-cis-4- (1,1-dimethylethoxy) -L-proline as an almost colorless viscous syrup.
TLC: 0,20 (85:15 toluen/eddikesyre på silicagel, fremkaldt I2-damp eller PMA plus varme).TLC: 0.20 (85:15 toluene / acetic acid on silica gel, evoked I2 vapor or PMA plus heat).
15 (c) cis-4-(1,1-Dimethoxyethoxy)-L-prolin N-Carbobenzyloxyproduktet fra afsnit (b) (5,5 g, 0,017 mol) hydrogeneres i 165 ml 2:1 methanol/vand under 3 atm. hydrogen i nærvær af 1,7 g 51's palladium-carbon-katalysator, hvilket giver 3,2 g af en klæbrigt delvis fast produkt. Dette materia-20 le suspenderes i 30 ml acetonitril, gnides og afkøles natten o-ver, hvilket giver 1,35 g cis-4-(1,1-dimethylethoxy)-L-prolin som et farveløs faststof, smeltepuntk 240-242°C (sønderdeling), forudgående gradvis mørkfarvning og sintring.(C) cis-4- (1,1-Dimethoxyethoxy) -L-proline The N-Carbobenzyloxy product of section (b) (5.5 g, 0.017 mol) is hydrogenated in 165 ml of 2: 1 methanol / water under 3 atm. hydrogen in the presence of 1.7 g of 51 palladium carbon catalyst to give 3.2 g of a sticky partially solid product. This material is suspended in 30 ml of acetonitrile, rubbed and cooled overnight to give 1.35 g of cis-4- (1,1-dimethylethoxy) -L-proline as a colorless solid, m.p. 240-242 ° C (decomposition), prior gradual darkening and sintering.
25 o [a] D = -36 (c, 0,5% i methanol).[Α] D = -36 (c, 0.5% in methanol).
25 Analyse: Beregnet for CgH^N03.0,25 H20: C 56,37, Έ 9,20, N 7,31.Analysis: Calculated for CgH ^NO3.0.25 H₂O: C 56.37, Έ 9.20, N 7.31.
Fundet: C 56,26, H 9,27, N 7,26.Found: C 56.26, H 9.27, N 7.26.
(d) 1- [D-3- (Acetylthio) -2-methyl-l-oxopropyl] -cis-4- (.1,1—dime-thylethoxy)-L-prolin 30 cis-4-(1,1-Dimethylethoxy)-L-prolinet fra afsnit (c) (1,3 g, 0,0069 mol) omsættes med 1,4 g (0,0078 mol) D-5-acetyl- thio-2-methylpropionylchlorid i 20 ml vand i nærvær af natrium- bicarbonat som beskrevet i eksempel 3, hvilket giver 2,2 g af en næsten farveløs viskos olie. Det fremkomne råprodukt ©pløses i 35 50 ml ethylacetat og behandles med 1,3 g dicyclohexylamin i 20 ml ethylacetat. Produktet krystalliserer ud fra opløsningen og filtreres og tørres, hvilket giver 2,65 g dicyclohexvlaminsalt,(d) 1- [D-3- (Acetylthio) -2-methyl-1-oxopropyl] -cis-4- (1,1,1-dimethylethoxy) -L-proline cis-4- (1,1 The dimethylethoxy) -L-proline from section (c) (1.3 g, 0.0069 mol) is reacted with 1.4 g (0.0078 mol) of D-5-acetylthio-2-methylpropionyl chloride in 20 ml of water in the presence of sodium bicarbonate as described in Example 3 to give 2.2 g of an almost colorless viscous oil. The resulting crude product is dissolved in 50 ml of ethyl acetate and treated with 1.3 g of dicyclohexylamine in 20 ml of ethyl acetate. The product crystallizes from the solution and is filtered and dried to give 2.65 g of dicyclohexvlamine salt,
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smeltepunkt 181-183°C, begynder-ved 170°C.mp 181-183 ° C, starting at 170 ° C.
[a]^ = -62° (c, 1% i ethanol).[α] D = -62 ° (c, 1% in ethanol).
Udrivning med 15 ml varm acetonitril efterfulgt af afkøling giver 2,4 g farveløst fast dicvclohexylaminsalt, smelte-5 punkt 183-185°C, begynder ved 175°.Pouring out with 15 ml of hot acetonitrile followed by cooling gives 2.4 g of colorless solid dicyclohexylamine salt, melting point 183-185 ° C, starts at 175 °.
[a] ^ = -65° (c, 1% i ethanol).[α] D = -65 ° (c, 1% in ethanol).
Analyse: Beregnet for ci5H25N05S* C 63,24, H 9,44, N 5,46, S 6,25 Fundet: C 63,22, H 9,61, N 5,41, S 6,02.Analysis: Calculated for C 15 H 25 NO 5 S * C 63.24, H 9.44, N 5.46, S 6.25 Found: C 63.22, H 9.61, N 5.41, S 6.02.
10 Ved at benytte fremgangsmåden i eksempel 3 omdannes de 2,4 g dicyclohexylaminsalt til syren ved at suspendere i e-thylacetat, afkøle i isbad og behandle med 30 ml 10%'s kaliumbi-sulfat. Lagene adskilles, og den vandige fase ekstraheres med 25 ml ethylacetat (4 gange). Efter fjernelse af opløsningsmid-15 let gnides materialet, der bliver delvis krystallinsk ved henstand, under 10 ml ether for at fuldende krystallisationen, fortyndes med 20 ml hexan, gnides og afkøles, hvilket giver 1,3 g 1-[D-3-(acetylthio)-2-methyl-l-oxopropyl]-cis-4-(1,1-dimethyl-ethoxy)-L-prolin som et farveløst faststof, smeltepunkt 96-98°C, 20 begynder ved 93°C.Using the procedure of Example 3, the 2.4 g of dicyclohexylamine salt is converted to the acid by suspending in ethyl acetate, cooling in an ice bath and treating with 30 ml of 10% potassium bisulfate. The layers are separated and the aqueous phase is extracted with 25 ml of ethyl acetate (4 times). After removal of the solvent, the material, which becomes partially crystalline upon standing, is rubbed under 10 ml of ether to complete the crystallization, diluted with 20 ml of hexane, rubbed and cooled to give 1.3 g of 1- [D-3- ( acetylthio) -2-methyl-1-oxopropyl] -cis-4- (1,1-dimethyl-ethoxy) -L-proline as a colorless solid, m.p. 96-98 ° C, starting at 93 ° C.
[ct]^ = -109° (c, 1% i ethanol).[α] D = -109 ° (c, 1% in ethanol).
Analyse: Beregnet for C-^I^NO^S: C 54,36, H 7,60, N 4,23, S 9,68.Analysis: Calculated for C- IH NO ^N₂S: C 54.36, H 7.60, N 4.23, S 9.68.
Fundet: C 53,92, H 7,73, N 4,30, S 9,29.Found: C, 53.92; H, 7.73; N, 4.30; S, 9.29.
(e) cis-4-(1,l-Dimethylethoxy)-1-(D-3-mercapto-2-methyl-l-oxo-25 propyl)-L-prolin 1-[D-3-(acetylthio)-2-methyl-l-oxopropyl]-cis-4-(1,1- -dimethylethoxy)-L-prolinen fra afsnit (d) (1,3 g, 0,0039 mol) hydrolyseres med 2,6 ml koncentreret ammoniakhydroxid i 6 ml vand, hvilket giver 1,1 g af en glaslignende remanens. Ved hen-30 stand fremkommer podekrystaller i produktet. Dette materiale dæk-kes med 8 ml ether, podes og gnides. Efterhånden som glasset går i opløsning, udskilles gradvis et krystallisk faststof. Efter 2 timer ved stuetemperatur tilsættes 20 ml hexan, og blandingen afkøles natten over under argon. Opløsningsmidlet fjer-35 nes, hvilket giver 1,0 g farveløs fast cis-4-(1,1-dimethylethoxy)--1-(D-3-mercapto-2-methyl-l-oxo-propyl)-L-prolin, smeltepunkt 106-108°C (begynder ved 103°C).(e) cis-4- (1,1-Dimethylethoxy) -1- (D-3-mercapto-2-methyl-1-oxo-propyl) -L-proline 1- [D-3- (acetylthio) - 2-Methyl-1-oxopropyl] -cis-4- (1,1- -dimethylethoxy) -L-proline from section (d) (1.3 g, 0.0039 mol) is hydrolyzed with 2.6 ml of concentrated ammonia hydroxide in 6 ml of water to give 1.1 g of a glass-like residue. Upon standing, seed crystals appear in the product. This material is covered with 8 ml of ether, seeded and rubbed. As the glass dissolves, a crystalline solid is gradually separated. After 2 hours at room temperature, 20 ml of hexane is added and the mixture is cooled overnight under argon. The solvent is removed to give 1.0 g of colorless solid cis-4- (1,1-dimethylethoxy) -1- (D-3-mercapto-2-methyl-1-oxo-propyl) -L-proline , mp 106-108 ° C (starts at 103 ° C).
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[a]^ = -78° (c, 1% ± methanol).[α] D = -78 ° (c, 1% ± methanol).
Analyse: Beregnet for C]_3H23N°4S·0'25 H20: C 53,12, H 8,06, N 4,77, S 10,91.Analysis: Calculated for C 13 H 23 N 4 O · 25 H 2 O: C 53.12, H 8.06, N 4.77, S 10.91.
Fundet: C 53,30, H 8,28, N 4,76, S 10,70.Found: C 53.30, H 8.28, N 4.76, S 10.70.
55
Eksempel 17 (cis)-1-[D-3-(Benzovlthio)-2~methyl-l-oxopropyl3-4-(phenylthio)- -L-prolin 9,9 g (0,031 mol) cis-4-phenylthio-L-prolin snspen-10 deres i 100 ml vand (pH 5,6), og pH justeres til 10,2 ved tilsætning af ca. 20 ml 10%'s natriumbicarbonat, så at der fås en klar opløsning. pH justeres derpå til 9,5 ved tilsætning af ca.Example 17 (cis) -1- [D-3- (Benzoylthio) -2-methyl-1-oxopropyl3-4- (phenylthio) -L-proline 9.9 g (0.031 mol) of cis-4-phenylthio-L -proline snowflake in 100 ml of water (pH 5.6), and the pH is adjusted to 10.2 by adding approx. 20 ml of 10% sodium bicarbonate to give a clear solution. The pH is then adjusted to 9.5 by the addition of ca.
4,5 ml koncentreret HC1. Opløsningen holdes ved 30°C, medens der tilsættes 8,1 g (0,033 mol) (D)-3-(benzoylthio)-2-methylpropan-15 syre-chlorid i 30 ml toluen samtidig med 100 ml 10%'s natriumbicarbonat for at holde pH på 9,3. Efter at ca. en fjerdedel af svrechloridet er tilsat, begynder et slimet bundfald .at dannes, hvilket holder sig under hele reaktionen. Efter omrøring af reaktionsblandingen ved pH 9,3 i 2,5 timer gøres denne stærkt 20 sur ved tilsætning af 20%'s HCl i nærvær af ethylacetat. Det vandige lag ekstraheres to gange med 350 ml-portioner ethylace-tat, og de forenede organiske lag vaskes med 300 ml mættet saltvandsopløsning og tørres (MgSO^,) . Opløsningsmidlet fjernes, hvilket giver 11,8 g skumagtigt fast råprodukt.4.5 ml of concentrated HCl. The solution is kept at 30 ° C while adding 8.1 g (0.033 mol) of (D) -3- (benzoylthio) -2-methylpropanoic acid chloride in 30 ml of toluene simultaneously with 100 ml of 10% sodium bicarbonate keeping the pH at 9.3. After approx. a quarter of the hydrochloric acid is added, a slimy precipitate begins to form, which stays throughout the reaction. After stirring the reaction mixture at pH 9.3 for 2.5 hours, this is strongly acidified by the addition of 20% HCl in the presence of ethyl acetate. The aqueous layer is extracted twice with 350 ml portions of ethyl acetate and the combined organic layers are washed with 300 ml of saturated brine and dried (MgSO 4). The solvent is removed to give 11.8 g of foamy solid crude product.
25 Til en opløsning af disse 11,8 g (0,027 mol.) skumag tigt faststof i 70 ml acetonitril tilsættes der ca. 6 g dicyclo-hexylamin i 25 ml ether. Der da‘nnes straks et hvidt .krystallinsk bundfald. Efter henstand natten over i kølerum filtreres faststoffet fra og vaskes med ether, hvilket giver (cis)-1-[D-3-30 -(benzoylthio)-2-methyl-l-oxopropyl]-4-(phenylthio)-L-nrolin-di- cyclohexylaminsalt (1:1).To a solution of these 11.8 g (0.027 mol.) Foamy solid in 70 ml of acetonitrile is added approx. 6 g of dicyclohexylamine in 25 ml of ether. A white crystalline precipitate is formed immediately. After standing overnight in cold rooms, the solid is filtered off and washed with ether to give (cis) -1- [D-3-30 - (benzoylthio) -2-methyl-1-oxopropyl] -4- (phenylthio) -L- nroline di-cyclohexylamine salt (1: 1).
Analyse: Beregnet for C22H23N04S2’C12H23N: C 66,85, H 7,59, N 4,59.Analysis: Calculated for C 22 H 23 NO 4 S 2 C 12 H 23 N: C 66.85, H 7.59, N 4.59.
Fundet: C 66,33, Έ. 7,30, N 4,48.Found: C, 66.33, Έ. 7.30, N 4.48.
35 Det let fugtige dicyelohexylaminsalt omrøres i 2,5 ti mer i en blanding af 300 ml ethylacetat og 200 ml 10%!' s ’kalium-bisulfat. Der dannes to klare lag. Det vandige lag ekstraheresThe slightly moist dicyelohexylamine salt is stirred for 2.5 hours in a mixture of 300 ml of ethyl acetate and 200 ml of 10%! s of potassium bisulfate. Two clear layers are formed. The aqueous layer is extracted
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med to 200 ml-portioner ethvlacetat, og de kombinerede organiske lag tørres (MgSO^). Opløsningsmidlet fjernes, hvilket giver et udbytte på 10,1 g skumagtigt fast (cis)-1-[D-3-(benzoyl-thio)-2-methyl-l-oxopropyl]-4-(phenylthio)-L-prolin, smeltepunkt 5 42-44°C.with two 200 ml portions of ethyl acetate and the combined organic layers are dried (MgSO4). The solvent is removed, yielding 10.1 g of foamy solid (cis) -1- [D-3- (benzoyl-thio) -2-methyl-1-oxopropyl] -4- (phenylthio) -L-proline, m.p. 42-44 ° C.
[a]^ = -36,5° (c = 1, methanol).[α] D = -36.5 ° (c = 1, methanol).
Analyse: Beregnet for ^22Η23Ν04δ2: C 60,87, H 5,46, N 3,23.Analysis: Calculated for ^22Η23Ν04δ2: C 60.87, H 5.46, N 3.23.
Fundet: C 60,75, H 5,35, N 3,17.Found: C, 60.75; H, 5.35; N, 3.17.
10 Eksempel 18 (cis) -1- (D-3-Mercapto-2-!-methyl-l-oxopropyl) -3-phenoxy-D,L-prolin (a) 3-Phenoxy-l,2-dehydroprolin-l-butylesterExample 18 (cis) -1- (D-3-Mercapto-2-methyl-1-oxopropyl) -3-phenoxy-D, L-proline (a) 3-Phenoxy-1,2-dehydroproline-1 butyl ester
En blanding af 9,25 g (50 mmol) 1,2-dehydroproplin-l--butylester i 70 ml toluen opvarmes sammen med 8,9 g (50 mmol) 15 n-bromsuccinimid ved tilbagesvaling, medens det udsættes for en sollampe (ca. 5 cm's afstand) i en time. I dette tidsrum produceres succinimid, og reaktionen afkøles til stuetemperatur. Suc-cinimidet fjernes ved filtrering, og filtratet inddampes til tørhed. Remanensen destilleres ved 80°C, hvilket som udbytte giver 20 3,5 g rå 3-brom-l,2-dehydroprolin-l-butylester.A mixture of 9.25 g (50 mmol) of 1,2-dehydroproplin-1-butyl ester in 70 ml of toluene is heated at reflux with 8.9 g (50 mmol) of 15 n-bromosuccinimide while being exposed to a solar lamp ( about 5 cm distance) for one hour. During this time succinimide is produced and the reaction is cooled to room temperature. The succinimide is removed by filtration and the filtrate is evaporated to dryness. The residue is distilled at 80 ° C to yield 20 3.5 g of crude 3-bromo-1,2-dehydroproline-1-butyl ester.
En blanding af denne rå 3-brom-l,2-dehydroprolin-l-bu-tylester og 3,9 g (13 mmol) thalliumphenoxid i 30 ml tørt dime-thvlformamid omrøres ved stuetemperatur under argon i 24 timer. Opløsningsmidlet fjernes under vakuum, og remanensen fortyndes 25 med ether til udfældning af thalliumbromid, der fjernes ved filtrering. Filtratet inddampes, hvilket giver en olie, der renses ved detstillation. Efter to timer ved 0,005 mm og 80°C er der 1,48 g 3-phenoxy-l,2-dehydroprolin-l-butvlester tilbage i destillationskolben .A mixture of this crude 3-bromo-1,2-dehydroproline-1-butyl ester and 3.9 g (13 mmol) of thallium phenoxide in 30 ml of dry dimethylformamide is stirred at room temperature under argon for 24 hours. The solvent is removed in vacuo and the residue is diluted with ether to precipitate thallium bromide which is removed by filtration. The filtrate is evaporated to give an oil which is purified by distillation. After two hours at 0.005 mm and 80 ° C, 1.48 g of 3-phenoxy-1,2-dehydroproline-1-butyl ester is left in the distillation flask.
30 (b) (cis)-3-Phenoxy-D,L-prolin.(B) (cis) -3-Phenoxy-D, L-proline.
En blanding af de 1,48 g 3-phenoxy-l,2-dehydroprolin--1-butylester, 5 ml IN natriumhydroxid og 20 ml 80%'s dioxan/vand omrøres ved stuetemperatur i 4 timer. Opløsningsmidlerne fjernes i vakuum, og remanensen opløses i 25 ml vand og behandles med 35 168 mg hatriumborhydrid i et tidsrum på en time ved stuetempera tur. Blandingen svrnes til pH 6 ved tilsætning af 2N HC1, og opløsningen holdes på 0°C i 16 timer, hvorefter der udfældes kry-A mixture of the 1.48 g of 3-phenoxy-1,2-dehydroproline-1-butyl ester, 5 ml of 1 N sodium hydroxide and 20 ml of 80% dioxane / water is stirred at room temperature for 4 hours. The solvents are removed in vacuo and the residue is dissolved in 25 ml of water and treated with 168 168 mg of sodium borohydride for a period of one hour at room temperature. The mixture is turned to pH 6 by the addition of 2N HCl and the solution is kept at 0 ° C for 16 hours, after which time the precipitate is precipitated.
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staller (ca. 25 mg) af (trans)-3-phenoxy-D,L-prolin. Disse fjernes ved filtrering, og filtratet afsaltes ved at blive ført gennem en "Dowex1® 50 W x 8 kolonne (2,5 x 30 cm), idet der anvendes IN ammoniumhydroxid som elueringsmiddel. De UV-aktive 5 fraktioner kombineres og inddampes, hvilket giver 616 mg fast (cis)-3-phenoxy--D,L-prolin.stalls (about 25 mg) of (trans) -3-phenoxy-D, L-proline. These are removed by filtration and the filtrate is desalted by passing through a Dowex1® 50 W x 8 column (2.5 x 30 cm) using 1N ammonium hydroxide as the eluant. The UV-active fractions are combined and evaporated, gives 616 mg of solid (cis) -3-phenoxy - D, L-proline.
(c) (cis)-1-[D-3-(Acetylthio)-2-methyl-l-oxopropyl]-3-phenoxy--D,L-prolin(c) (cis) -1- [D-3- (Acetylthio) -2-methyl-1-oxopropyl] -3-phenoxy - D, L-proline
De 616 mg (cis)-3-phenoxy-D,L-prolin opslæmmes 1 20 10 ml vand ved 5°C, og pH indstilles til 8,0 med fast natriumcarbo-nat. En opløsning af 550 mg (2,5 mmol) D-3-acetvlthio-2—methvl-propanoyl-syrechlorid i 1 ml ether tilsættes, og reaktiomsblandingens pH holdes mellem 7,3 og 8,2 i den næste 1,5 time ved tilsætning af natriumcarbonat. Blandingen vaskes med ethylacetat 15 (2 x 20 ml), syrnes til pH 2 ved tilsætning af 10% HC1 og ekstra- heres med ethylacetat (3 x 50 ml). Ekstrakterne forenes, tørres (MgSO^) og inddampes, hvilket som udbytte giver 810 mg af en olie. Denne olie renses ved lynchromatografi på silicagel (LP-1, 300 ml), idet der anvendes 10-20%’s eddikesyre/toluenblandinger som 20 elueringsmidler, og udbyttet er 530 mg (cis)-1-[D-3-(acetylthio)--2-methy1-1-oxopropy1]-3-phenoxy-D,L-prolin.The 616 mg (cis) -3-phenoxy-D, L-proline is slurried in 10 ml of water at 5 ° C and the pH is adjusted to 8.0 with solid sodium carbonate. A solution of 550 mg (2.5 mmol) of D-3-acetylthio-2-methyl-propanoyl acid chloride in 1 ml of ether is added and the pH of the reaction mixture is maintained between 7.3 and 8.2 for the next 1.5 hours at addition of sodium carbonate. The mixture is washed with ethyl acetate 15 (2 x 20 ml), acidified to pH 2 by the addition of 10% HCl and extracted with ethyl acetate (3 x 50 ml). The extracts are combined, dried (MgSO 4) and evaporated to yield 810 mg of an oil. This oil is purified by flash chromatography on silica gel (LP-1, 300 ml) using 10-20% acetic acid / toluene mixtures as eluents and the yield is 530 mg (cis) -1- [D-3- (acetylthio ) - 2-methy1-1-oxopropy1] -3-phenoxy-D, L-proline.
(d) (cis)-1-(D-3-Mercapto-2-methyl-l-oxopropyl)-3-phenoxy-D,L--prolin(d) (cis) -1- (D-3-Mercapto-2-methyl-1-oxopropyl) -3-phenoxy-D, L-proline
De 530 mg (cis)-1-[D-3-(acetylthio)-2-methyl-1-oxopro-25 pyl]-3-phenoxy-D,L-prolin opløses i 50:50 koncentreret ammoniak/ vand (afgasset ved at boble argon gennem opløsningen i 15 minutter) under argon og omrøres ved stuetemperatur i 1,5 time. Den let uklare opløsning justeres til pH 6,5 med koncentreret HC1 (nogen varme forekommer) og ekstraheres med methylenchlorid 30 (2 x 25 ml). Derpå indstilles pH til 1, og opløsningen ekstrahe- res igen med methylenchlorid (3x50 ml). Ekstrakterne kombineres, tørres (MgSO^) og inddampes, hvilket som udbytte giwer 410 mg af en glasagtig forbindelse. Udrivning med chlorførm resulterer i krystallisation. Faststoffet omkrystalliseres ud fra 35 ethylacetat/hexan, hvilket som udbytte giver 261 mg ('c.is))—l-(D-3--mercapto-2-methyl-l-oxopropylf~3-phenoxy-D,L-prolin, smeltepunkt 134-135°C.The 530 mg (cis) -1- [D-3- (acetylthio) -2-methyl-1-oxopropyl] -3-phenoxy-D, L-proline is dissolved in 50:50 concentrated ammonia / water (degassed) by bubbling argon through the solution for 15 minutes) under argon and stirring at room temperature for 1.5 hours. The slightly cloudy solution is adjusted to pH 6.5 with concentrated HCl (no heat is present) and extracted with methylene chloride 30 (2 x 25 ml). The pH is then adjusted to 1 and the solution is extracted again with methylene chloride (3x50 ml). The extracts are combined, dried (MgSO4) and evaporated to yield 410 mg of a glassy compound. Chlorine depletion results in crystallization. The solid is recrystallized from ethyl acetate / hexane to yield 261 mg ('c.is)) - 1- (D-3-mercapto-2-methyl-1-oxopropylph-3-phenoxy-D, L-proline , mp 134-135 ° C.
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Analyse: Beregnet for C^H^NO^S: C 58,23, H 6,19, N 4,53, S 10,36.Analysis: Calculated for C ^ HH ^NO ^S: C 58.23, H 6.19, N 4.53, S 10.36.
Fundet: C 58,07,' H 6,18, N 4,45, S 10,16.Found: C, 58.07; H, 6.18; N, 4.45; S, 10.16.
5 Biologisk afprøvning5 Biological testing
Et af de systemer, som regulerer (forøger) blodtryk hos mennesker, er systemet renin/angiotensin/aldoste-ron. Renin er et enzym, der frembringes i myoepitheliecel-lerne i nyrernes juxtaglomerulære apparat, og som frigives 10 derfra. Mekanismen, der styrer sekretionen af renin, synes primært at reguleres ved blodets salt- og vandindhold og ved det tryk, ved hvilket blodet pumpes gennem nyren. Når disse faktorer sænkes, sendes renin direkte ud i blodet.One of the systems that regulate (increase) blood pressure in humans is the system renin / angiotensin / aldosteroon. Renin is an enzyme produced in the myoepithelial cells of the kidney juxtaglomerular apparatus and released therefrom. The mechanism that controls the secretion of renin appears to be primarily regulated by the salt and water content of the blood and by the pressure at which the blood is pumped through the kidney. When these factors are lowered, renin is sent directly into the bloodstream.
Der møder det som substrat et -globulin, angiotensinogen 15 (et inaktivt proteinstof). Renin spalter angiotensinogen i to ligeledes inaktive komponenter, et tetrapeptid og et de-capeptid kaldet angiotensin I (forkortet til A-I). Når A-I cirkulerer gennem kapillærerne (primært lungens kapillærer), møder det det angiotensinomdannende enzym (forkortet til ACE), 20 der er lokaliseret i kapillærernes endothelieceller. ACE spalter A-I i et dipeptid og et octapeptid, angiotensin II (forkortet til A-II), som er det stærkeste kendte blodtryksforøgende stof i menneskelegemet. A-II1s blodtryksforøgende virkning finder sted både lokalt i muskulaturen og centralt.There it encounters as a substrate a -globulin, angiotensinogen 15 (an inactive protein). Renin cleaves angiotensinogen into two equally inactive components, a tetrapeptide and a decapeptide called angiotensin I (abbreviated to A-I). As A-I circulates through the capillaries (primarily the capillaries of the lung), it encounters the angiotensin-converting enzyme (abbreviated to ACE) 20 located in the endothelial cells of the capillaries. ACE cleaves A-I into a dipeptide and an octapeptide, angiotensin II (abbreviated to A-II), which is the strongest known blood pressure enhancer in the human body. A-II1's blood pressure boosting action takes place both locally in the musculature and centrally.
25 Efter stimulering ved hjælp af A-II udsender postremaområdet i hjernen til resten af kroppen impulser, som fremkalder blodtryksforøgelse. Derudover frembringer A-II endnu en virkning, nemlig den fysiologiske stimulering af sekretionen fra binyrebarken af aldosteron, et mineralcorticoid. Aldosteron 30 forøger resorptionen af natriumioner fra nyrerørene, hvorved det effektive blodrumfang forøges, således at blodtrykket hæves yderligere ved hjælp af denne sekundære mekanisme.25 After stimulation by A-II, the postrema region of the brain sends impulses to the rest of the body that induce blood pressure increase. In addition, A-II produces another effect, namely the physiological stimulation of the secretion from the adrenal cortex of aldosterone, a mineral corticoid. Aldosterone 30 increases the resorption of sodium ions from the renal tubes, thereby increasing the effective blood volume, thus raising the blood pressure further by this secondary mechanism.
Foruden omdannelsen af A-I til A-II har ACE endnu en yderligere virkning. Blod indeholder et octapeptid, bra-35 dykinin', som har vasodi later ende egenskaber. ACE transforme-In addition to the conversion of A-I to A-II, ACE has yet another effect. Blood contains an octapeptide, bra-dykinin ', which has vasodi later end properties. ACE transformer
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bradykinin til inaktive komponenter. Med hensyn til denne funktion betegnes ACE til tider som kininase II.bradykinin for inactive components. For this function, ACE is sometimes referred to as kininase II.
Renin-angiotensin-aldosteronsystemet er i uorden hos hypertensive personer og bidrager således afgørende til 5 patientens høje blodtryk. Et lægemiddel, som således inhlbe-rer ACE, er altså i stand til at frembringe følgende virkninger : 1. Inhibering af dannelsen af A-II og dermed: a) direkte inhibering af vasoconstriktion og 10 b) inhibering af udsendelsen af aldosteron Æra binyrebarken (dvs. inhibering af overskydende vand- og saltresorption), samt 2. som resultat af ACE-inhibitionen fås en inhibering af bradykinins spaltning, således at dets vasodilatxeren- 15 de virkning (blodtrykssænkende) bibeholdes.The renin-angiotensin-aldosterone system is disordered in hypertensive individuals and thus contributes significantly to the patient's high blood pressure. Thus, a drug thus involving ACE is capable of producing the following effects: 1. Inhibition of the formation of A-II and thus: a) direct inhibition of vasoconstriction and b) inhibition of the release of aldosterone era adrenal cortex ( i.e., inhibition of excess water and salt resorption), and 2. as a result of the ACE inhibition, an inhibition of bradykinin cleavage is obtained so that its vasodilate-reducing (blood pressure lowering) effect is maintained.
Ingen af de almindelige antihypertensive midler virker som ACE-inhibitor.None of the usual antihypertensive agents act as an ACE inhibitor.
Forbindelserne med den ovenstående almene formel I er derimod stærke ACE-inhibitorer. De inhiberer omdannelsen 20 af decapeptidet angiotensin I til angiotensin II og minimerer eller eliminerer således hypertension fremkaldt ved hjælp af angiotensin II. Forbindelserne fremstillet ved fremgangsmåden ifølge opfindelsen griber ind i omdannelsesprocessen for an-giotensinogen (renin) -^angiotensin I-^angiotensin II ved at blo-25 kere ACE og således minimere eller eliminere dannelsen af angiotensin II, hvilken forbindelse er ansvarlig for forøgelsen i blodtrykket. Det effektive ingrebssted eller virkningssted for forbindelserne med den almene formel I er fuldstændig forskelligt fra det, som kendes for et hvilket som helst af de 30 almindeligvis anvendte antihypertensive lægemidler. Forbandelserne fremstillet ved fremgangsmåden ifølge opfindelsen gør det muligt - i modsætning til de almindelige antihypefteansi-ver - at opnå et indgreb i de årsags fremkaldende faktorer til hypertension.The compounds of the above general formula I, on the other hand, are potent ACE inhibitors. They inhibit the conversion 20 of the decapeptide angiotensin I to angiotensin II and thus minimize or eliminate hypertension induced by angiotensin II. The compounds produced by the process of the invention interfere with the conversion process of angiotensinogen (renin) - angiotensin I- ^ angiotensin II by blocking ACE and thus minimizing or eliminating the formation of angiotensin II, which compound is responsible for the increase in blood pressure. . The effective site of action or site of action of the compounds of general formula I is completely different from that known for any of the commonly used antihypertensive drugs. The dressings made by the method of the invention make it possible, unlike the usual antihypertensive agents, to interfere with the causes of hypertension.
35 Således er den farmakologiske anvendelighed af for-35 Thus, the pharmacological utility of the
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bindeiserne med formlen I baseret på deres evne til at inhi-- bere det angiotensinomdannende enzyms virkning. Denne inhi-bering er bestemt på in vitro-basis ved måling af virkningen på det angiotensinomdannende enzym ekstraheret fra kaninlun-5 ge og ved at bestemme den inhiberende aktivitet på angiotensin I-fremkaldte kontraktioner af marsvinetyktarm. Disse prøver er standardiserede og anvendes som sådanne inden for dette område af medicinen, og de er i Øvrigt nærmere beskrevet nedenfor.the binders of formula I based on their ability to inhibit the action of the angiotensin converting enzyme. This inhibition is determined on an in vitro basis by measuring the effect on the angiotensin converting enzyme extracted from rabbit lung and by determining the inhibitory activity on angiotensin I-induced contractions of guinea pig intestine. These tests are standardized and used as such in this field of medicine and are further described below.
1010
Inhibition af angiotensin-omdannende enzym isoleret fra kaninlungeInhibition of angiotensin-converting enzyme isolated from rabbit lung
Aktiviteten hos det angiotensinomdannende enzym fra kaninlunge i cellefri ekstrakt måles ved spektrofotometrisk 15 bestemmelse af hippursyre frigivet ved indvirkning af ensymet på hippuryl-L-histidyl-L-leucin (HHL) således som beskrevet af Cushman og Cheung i Biochem. Pharmacol., 20, 1637 (1971), jfr. nedenstående reaktionsskema.The activity of the rabbit lung angiotensin converting enzyme in cell-free extract is measured by spectrophotometric determination of hippuric acid released by the action of the enzyme on hippuryl-L-histidyl-L-leucine (HHL) as described by Cushman and Cheung in Biochem. Pharmacol., 20, 1637 (1971), cf. the reaction scheme below.
-Gly-His-Leu —“Gly + His-Leu HHL hippursyre 25 Måling af det angiotensinomdannende enzyms inhibi tion under anvendelse af denne spektrofotometriske biologiske afprøvning kræver inkubation af blandinger af følgende * komponenter ved 37°C i et rumfang på 0,25 ml: 100 mM phosphatpuffer (pH 8,3) 30 300 mM natriumchlorid 0,001-1000 jig/ml inhibitor eller eventuelt ingen inhibitor 5-10 millienheder enzym.-Gly-His-Leu - "Gly + His-Leu HHL Hippuric Acid 25 Measurement of the inhibition of the angiotensin converting enzyme using this spectrophotometric biological assay requires incubation of mixtures of the following * components at 37 ° C in a volume of 0.25 ml : 100 mM phosphate buffer (pH 8.3) 300 mM sodium chloride 0.001-1000 µg / ml inhibitor or optionally no inhibitor 5-10 milligrams of enzyme.
Efter ovennævnte blandingers inkubation ved forskel-35 lige inhibitorkoncentrationer eller i fraværelse af inhibito-Following the incubation of the above mixtures at various inhibitor concentrations or in the absence of inhibitory
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rer i 30 minutter standses enzymreaktionen ved tilsætning af 0,25 ml 1 H saltsyre. Det er også nødvendigt at køre kontrolforsøg, hvor enzymet inaktiveres ved tidspunktet 0 ved tilsætning af syren før enzymet. 1,5 ml ethylacetat sættes til 5 hvert reagensglas for at ekstrahere den ved hjælp af enzymet dannede hippursyre. Efter 20 sekunders kraftig blanding ((i hvirvelstrøm) og fraskillelse af ethylacetatlaget ved centrifugering udtages fra hvert reagensglas 1,0 ml af opløsningsmidlet og inddampes til tørhed ved 100°C, og hippursyren «genio opløses i 1,0 ml vand, og dens mængde bedømmes ved hjælp af opløsningens basorptionsevne ved bølgelængden 228 nm.For 30 minutes, the enzyme reaction is stopped by the addition of 0.25 ml of 1 H hydrochloric acid. It is also necessary to run control experiments where the enzyme is inactivated at time 0 upon addition of the acid before the enzyme. 1.5 ml of ethyl acetate are added to each test tube to extract the hippuric acid formed by the enzyme. After 20 seconds vigorous mixing ((in vortex flow) and separation of the ethyl acetate layer by centrifugation, remove from each tube 1.0 ml of the solvent and evaporate to dryness at 100 ° C and dissolve the hippuric acid in 1.0 ml of water and its amount is judged by the basor absorption capacity of the solution at the wavelength of 228 nm.
Kraften som inhibitorer for det angiotensinomdannen-de enzym udtrykkes som I50 -værdien, der er den mængde inhibitor i pg/ml eller mikromolært, som kræves for at inhibere 15 det angiotensinomdannende enzyms aktivitet med 50% således som målt ved den spektrofotornetriske biologiske afprøvningsmetode. Denne værdi opnås ved grafisk at afsætte den procentvise inhibition, som frembringes ved inhibitorkoncentrationer varierende fra to gange til tre gange den -foregående over et· interval fra 20 0,001 pg/ml til 1000 pg/ml. En sådan procentvis inhibition be regnes ifølge nedenstående udtryk: procentvis inhibition = —^ A -------- ^ (A-A°) 25 hvor A betegner hippursyres absorptionsevne ved en 30 minutters biologisk afprøvning uden inhibitor, A° betegner Jbag-grundsabsorptionsevnen ved en biologisk afprøvning inkuberet i 0 minutter, B betegner hippursyres absorptionsevne ved en 30 minutters biologisk afprøvning ved den afprøvede inhibi-30 torkoncentration, og B° betegner baggrundabsorptionen ved biologisk afprøvning indeholdende inhibitoren, men kun inkuberet i 0 minutter.The force as inhibitors of the angiotensin converting enzyme is expressed as the I50 value, which is the amount of inhibitor in pg / ml or micromolar required to inhibit the activity of the angiotensin converting enzyme by 50% as measured by the spectrophotometric biological assay method. This value is obtained by graphically plotting the percentage inhibition produced by inhibitor concentrations varying from twice to three times the preceding over a range of from 0.001 µg / ml to 1000 µg / ml. Such a percentage inhibition is calculated according to the following terms: percentage inhibition = - ^ A -------- ^ (AA °) where A denotes the absorbency of hippuric acid in a 30 minute biological test without inhibitor, A ° denotes the Jbag basic absorbency in a biological test incubated for 0 minutes, B represents the absorbency of hippuric acid at a 30 minute biological test at the inhibitor concentration tested, and B ° represents the background absorption by biological test containing the inhibitor, but only incubated for 0 minutes.
35 0 4035 0 40
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Procedure ved afprøvning af den inhibitoriske aktivitet på • det angiotensin I-omdannende enzym (ACE) på marsvinetyktarm in vitroProcedure for testing the inhibitory activity of the angiotensin I converting enzyme (ACE) on guinea pig intestine in vitro
Denne procedure anvendes til at bestemme, hvorvidt 5 en forbindelse udgør en inhibitor for angiotensin I-omdannende enzym baseret på dens aktivitet afsat som funktion af måleresultater for angiotensin I-fremkaldte kontraktioner af marsvinetyktarm. ACE-inhibitorer inhiberer typisk angiotensin I-fremkaldte kontraktioner.This procedure is used to determine whether a compound is an inhibitor of angiotensin I converting enzyme based on its activity set aside as a function of measurement results for angiotensin I-induced contractions of guinea pig colon. ACE inhibitors typically inhibit angiotensin I-induced contractions.
10 Marsvin af begge køn af stamme Hartley, som ikke har fastet, og som vejer fra ca. 300 til ca. 400 g, dræbes ved et slag mod hovedet. Tyktarmen udtages, og 2-3 cm afsnit præpareres ifølge Vane's metode, jfr. nedenstående litteratursted 1. Hver tyktarmsstrimmel suspenderes derpå i et 10 ml's 15 vævsbad fyldt med Krebs's opløsning, jfr. nedenstående litteraturlisten nr. 2, og holdes ved 37°C og luftes ved 95% O2 og 5% COj· Muskelaktiviteten registreres isotonisk under en belastning på 1 g målt ved hjælp af Harvard nr. 356 spændingsmåler (transducer) for hjertemuskulator/glatmuskulator for- 20 bundet med en Beckman type R dynograf.10 Guinea pigs of both species of Hartley that have not fasted and weigh from approx. 300 to approx. 400 g, killed in a blow to the head. The colon is removed and 2-3 cm sections are prepared according to Vane's method, cf. The following literature site 1. Each colon strip is then suspended in a 10 ml 15 tissue bath filled with Krebs's solution, cf. The following list of references is No. 2, and is maintained at 37 ° C and vented at 95% O2 and 5% CO 2. 20 bound with a Beckman type R dynograph.
Efter at vævene har opnået ligevægtsindstilling efter ca. 90 minutter, opnås 2 minutters kontrolrespons med intervaller på 10 minutter ved hjælp af følgende agonist..After the tissues have reached equilibrium position after approx. 90 minutes, a 2 minute control response is achieved at 10 minute intervals using the following agonist.
25 angiotensin I (A-I) 0,025 mikrogram/ml FBC (endelig bladkoncentration)Angiotensin I (A-I) 0.025 micrograms / ml FBC (final leaf concentration)
Kontraktionerne, som frembringes ved denne koncentration af A-I, repræsenterer fra 50 til 75% af de maksimale.The contractions produced at this concentration of A-I represent from 50 to 75% of the maximum.
30 Prøveforbindelsen opløses sædvanligvis i vandig el ler vandig saltholdig opløsning, og der fremstilles tifoldige fortyndinger i H20. Agonisten' forbehandles i 2 minutter med prøveforbindelsen, og den procentvise ændring i kontraktions-responset beregnes . Specifikt aktive forbindelser, dvs.The test compound is usually dissolved in aqueous or aqueous saline solution and ten-fold dilutions are prepared in H2 O. The agonist 'is pretreated for 2 minutes with the test compound and the percentage change in contraction response calculated. Specifically active compounds, i.e.
35 forbindelser, som sandsynligvis vil være ACE-inhibitorer, in-35 compounds, which are likely to be ACE inhibitors, include
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hiberer typisk angiotensin I-fremkaldte kontraktioner.typically inhibits angiotensin I-induced contractions.
A—BA-B
Procentvis inhibition = —x 100 5 hvor A betegner kontraktionen imms) forårsaget af A-I før tilsætning af prøveforbindelse, og B betegner kontraktionen (mms) forårsaget af A-I efter tilsætning af prøveforbindelsen.Percent inhibition = -x 100 5 where A denotes the contraction imms) caused by A-I before addition of test compound, and B denotes the contraction (mms) caused by A-I after addition of the test compound.
10 EC50 (koncentrationen af prøveforbindelse, som frembringer 50%'s inhibition af A-I*s kontraktive virkning) udregnes grafisk eller biometrisk. Nogle få koncentrationer af prøve-forbindelsen anvendes typisk til at konstruere kurven- over inhibitorisk respons som funktion af koncentrationen.EC50 (the concentration of test compound which produces 50% inhibition of the contractile action of A-I *) is calculated graphically or biometrically. Typically, a few concentrations of the sample compound are used to construct the curve of inhibitory response as a function of concentration.
1515
Under anvendelse af ovenstående teknik er der opnået følgende 1^ og EC^q data for ’"Captopril" og en forbindelse fremstillet ved fremgangsmåden ifølge opfindelsen; 20 Aktivitet ' AktivitetUsing the above technique, the following 1 µ and EC 2 q data for "Captopril" and a compound prepared by the method of the invention have been obtained; 20 Activity 'Activity
MarevineMare Vineyards
Kaninlunge ACE ileum Forb._Struktur_150 mM_ECgp xnMRabbit lung ACE ileum Ref_Structure_150 mM_ECgp xnM
Kendt sammlign. ,3 Γ I on On "Captopril" HSCH^CHCO-N_l-CCØH 20 20 25 S-CfiH,-Known compare. , 3 Γ I on On "Captopril" HSCH ^ CHCO-N_l-CCØH 20 20 25 S-CfiH, -
Fremst. JLMfr. JL
iflg· opf. I I o eks. 13 HSCH2CHCO-N_l-COOH 0 30 35according to In Example 13 HSCH2CHCO-N_l-COOH 0 30 35
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- 1979-08-09 CS CS795462A patent/CS228118B2/en unknown
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- 1979-08-10 DK DK335879A patent/DK154553C/en not_active IP Right Cessation
- 1979-08-10 NL NL7906120A patent/NL193374C/en active Protection Beyond IP Right Term
- 1979-08-10 LU LU81593A patent/LU81593A1/en active Protection Beyond IP Right Term
- 1979-08-10 BE BE0/196688A patent/BE878191A/en not_active IP Right Cessation
- 1979-08-10 SU SU792800304A patent/SU1066460A3/en active
- 1979-08-10 AR AR277678A patent/AR229081A1/en active
- 1979-08-10 IE IE1544/79A patent/IE48802B1/en active Protection Beyond IP Right Term
- 1979-08-10 SE SE7906722A patent/SE447477B/en active Protection Beyond IP Right Term
- 1979-08-10 KR KR1019790002731A patent/KR830002450B1/en active
- 1979-08-10 CH CH737579A patent/CH642064A5/en not_active IP Right Cessation
- 1979-08-10 GB GB7927867A patent/GB2028327B/en not_active Expired
- 1979-08-10 PT PT70049A patent/PT70049A/en unknown
- 1979-08-10 RO RO98428A patent/RO78870B/en unknown
- 1979-08-10 FI FI792498A patent/FI69834C/en not_active IP Right Cessation
- 1979-08-10 ES ES483311A patent/ES483311A1/en not_active Expired
- 1979-08-10 JP JP10272279A patent/JPS5527199A/en active Granted
-
1988
- 1988-12-21 JP JP63323204A patent/JPH01287069A/en active Pending
-
1999
- 1999-06-04 LU LU90403C patent/LU90403I2/en unknown
- 1999-08-04 NL NL990024C patent/NL990024I1/en unknown
Patent Citations (1)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
DE2703828A1 (en) * | 1976-02-13 | 1977-08-18 | Squibb & Sons Inc | PROLINDER DERIVATIVES AND RELATED COMPOUNDS, METHODS FOR THEIR MANUFACTURING AND THEIR USE AS A MEDICINAL PRODUCT |
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Legal Events
Date | Code | Title | Description |
---|---|---|---|
CTFF | Application for supplementary protection certificate (spc) filed |
Free format text: CA 1999 00011, 19990507, EXPIRES: 20040810 |
|
PUP | Patent expired |