CN104327000B - 苯基取代的三氮唑亚磺酰丙二酸类化合物、其制备方法及用途 - Google Patents
苯基取代的三氮唑亚磺酰丙二酸类化合物、其制备方法及用途 Download PDFInfo
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Classifications
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- C—CHEMISTRY; METALLURGY
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- C07D249/02—Heterocyclic compounds containing five-membered rings having three nitrogen atoms as the only ring hetero atoms not condensed with other rings
- C07D249/08—1,2,4-Triazoles; Hydrogenated 1,2,4-triazoles
- C07D249/10—1,2,4-Triazoles; Hydrogenated 1,2,4-triazoles 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
- C07D249/12—Oxygen or sulfur atoms
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- Chemical & Material Sciences (AREA)
- Organic Chemistry (AREA)
- Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
- Acyclic And Carbocyclic Compounds In Medicinal Compositions (AREA)
Abstract
本发明涉及与高尿酸血症和痛风相关的药物领域。具体而言,本发明涉及一类含苯基取代的三氮唑亚磺酰丙二酸结构的尿酸转运体1抑制剂、其制备方法、及含有它们的药物组合物以及它们在制备糖尿病药物中的应用。
Description
技术领域
本发明涉及治疗高尿酸血症和痛风相关的药物领域。具体而言,本发明涉及对高尿酸血症和痛风有治疗作用的一类苯基取代的三氮唑亚磺酰丙二酸结构的尿酸转运体1(urate transporter 1,URAT1)抑制剂、制备方法、含有它们的药物组合物以及在医药上的用途。
背景技术
痛风是一种慢性代谢性疾病,以高尿酸血症和尿酸单钠盐(MSU)沉积在关节等部位而引起的痛疼为主要特征,主要原因为嘌呤代谢紊乱和/或尿酸排泄障碍。据估计,目前全球痛风患者有2000多万。目前用于治疗痛风的药物包括用于缓解疼痛的抗炎药物(如秋水仙碱等)、抑制尿酸生成药物(以别嘌醇和非布索坦为代表的黄嘌呤氧化酶抑制剂)、粗尿酸排泄药物(以丙磺舒、苯磺唑酮、苯溴马隆和氯沙坦为代表的尿酸排泄药物)和尿酸酶(以pegloticase为代表)。这些药物存在不同的程度的毒副作用,如苯溴马隆有引起爆发性肝炎的危险,别嘌醇有肝脏及骨髓毒性和变态反应等不良反应,等等。
Lesinurad(RDEA 594)是一种由Ardea公司研制的可以抑制肾脏中尿酸转运体(urate transporter 1,URAT1)而通过尿液的途径来排出血液中尿酸的口服药物,目前处于III期临床阶段。Lesinurad最早由Valeant公司研发的抗病毒药物RDEA806发展而来。现在Lesinurad的所有权目前由于Ardea公司被收购而属于Astra Zeneca。
本发明公开了一类含苯基取代的三氮唑亚磺酰丙二酸结构的URAT1抑制剂,这些化合物可用于制备治疗高尿酸血症和痛风的药物。
发明内容
本发明的一个目的是提供一种具有良好活性,具有通式I的一类化合物。
本发明的另一个目的是提供制备具有通式I的化合物的方法。
现结合本发明的目的对本发明内容进行具体描述。
本发明具有通式(I)的化合物具有下述结构式:
其中,R选自卤素取代基。
优选通式(I)的化合物具有以下结构,
更优选通式(I)的化合物具有以下结构,
本发明所述通式(I)化合物通过以下路线合成:
化合物II与α-溴代丙二酸二甲酯在碱存在下反应,得到化合物IV;化合物IV在溴仿中与亚硝酸钠和二氯乙酸反应得到化合物V;化合物V在碱性条件下水解得到化合物VI;化合物VI与1当量氧化剂氧化得到化合物I。
本发明所述通式I化合物具有URAT1的抑制作用,可作为有效成分用于制备高尿酸血症和痛风的治疗药物。本发明所述通式I化合物的活性是通过受体结合试验来验证的。
本发明的通式I化合物在相当宽的剂量范围内是有效的。例如每天服用的剂量约在1mg-500mg/人范围内,分为一次或数次给药。实际服用本发明通式I化合物的剂量可由医生根据有关的情况来决定。
具体实施方式
下面结合实施例对本发明作进一步的说明。需要说明的是,下述实施例仅是用于说明,而并非用于限制本发明。本领域技术人员根据本发明的教导所做出的各种变化均应在本申请权利要求所要求的保护范围之内。
实施例1化合物I-1的合成
A.化合物IV-1的合成
化合物II参照专利文献WO2011085009制备。5.96g(20mmol)化合物II-1和4.22g(20mmol)化合物III溶于100mL干燥的DMF中,室温下搅拌,加入8.29g(60mmol)固体K2CO3,而后反应混合物在室温下搅拌,直到TLC跟踪发现反应完成(一般12h以内)。反应混合物倾倒入400mL冰水中,搅拌,使用100mL×3的CH2Cl2萃取,合并萃取相,使用100mL 5%的盐水洗涤,无水硫酸钠干燥。抽滤除去干燥剂,滤液在旋转蒸发仪上蒸干,得到的残余物使用柱层析纯化,得到化合物IV-1,白色固体,ESI-MS,m/z=551([M+Na]+)。
B.化合物V-1的合成
6.33g(12mmol)化合物IV-1溶于30mL溴仿中,室温下搅拌,加入3.45g(50mmol)NaNO2和3.00g苄基三乙基溴化铵,而后加入6.45g(50mmol)二氯乙酸。所得混合物在室温下搅拌,直到TLC跟踪发现反应完成(一般12h以内)。反应混合物倾倒入300mL冰水中,搅拌,使用100mL×3的CH2Cl2萃取,合并萃取相,依次使用100mL 2%的Na2S2O3溶液和100mL 5%的盐水洗涤,无水硫酸钠干燥。抽滤除去干燥剂,滤液在旋转蒸发仪上蒸干,得到的残余物使用柱层析纯化,得到化合物V-1,白色固体,ESI-MS,m/z=613([M+Na]+)。
C.化合物VI-1的合成
4.72g(8mmol)化合物V-1溶于30mL甲醇中,室温下搅拌,加入3mL10%的LiOH溶液,所得混合物室温下搅拌,直到TLC跟踪发现反应完成(一般3h以内)。反应混合物倾倒入200mL冰水中,搅拌,使用浓盐酸调节pH=2-3,100mL×3的CH2Cl2萃取,合并萃取相,使用100mL 5%的盐水洗涤,无水硫酸钠干燥。抽滤除去干燥剂,滤液在旋转蒸发仪上蒸干,得到的残余物使用柱层析纯化,得到化合物VI-1,白色固体,ESI-MS,m/z=562,564,560([M-H]-)。
D.化合物I-1的合成
3.38g(6mmol)化合物VI-1溶于10mL CH2Cl2中,搅拌,加入1.20g(7.0mmol)间氯过氧苯甲酸(mCPBA),室温下搅拌5h小时。反应混合物倾倒入200mL冰水中,搅拌,100mL×3的CH2Cl2萃取,合并萃取相,依次使用100mL 2%Na2S2O3溶液、100mL饱和NaHCO3和100mL 5%的盐水洗涤,无水硫酸钠干燥。抽滤除去干燥剂,滤液在旋转蒸发仪上蒸干,得到的残余物使用柱层析纯化,得到化合物I-1,黄白色固体,ESI-MS,m/z=578,580,576([M-H]-)。
实施例2-8
参照实施例1操作步骤,合成了下表所列化合物。
实施例9
本发明所述的化合物及相关化合物对URAT1抑制的IC50值按照文献记载的类似的方法测定(US2014/0005136中实施例12)。
构建稳定表达人源化URAT1转运体的细胞株:将人源化URAT1基因(SLC22A112)从质粒pCMV6-XL-5(Origene)亚克隆到真核表达的质粒pCMV6/neo(Origene)上。基因测序证实了人源化URAT1与基因库中记录的信息一致(NM_144585.2)。HEK293人胚胎肾细胞(ATCC#CRL-1573)在EMEM组织培养液中在5%的CO2和95%的空气气氛中培养。使用L2000型转染剂(Invitrogene)将pCMV6/Neo/URAT1转染到HEK293细胞上。24小时后,将被转染的细胞分到直径为10cm的组织培养皿中,继续生长一天,而后将培养基更换为含有0.5mg/mL G418(Gibco)的新鲜的培养基。8天后,选择并收集耐药性菌落,并用其测试对14C-标记的尿酸的转运活性。将HEK293/URAT1细胞以75,000/孔的密度种植于聚D-赖氨酸覆盖的96孔板上。
这些细胞在培养箱中37℃下生长过夜,而后冷却到室温下,其中的培养液使用250μL/孔的清洗液洗涤一次(125mM葡萄糖酸钠、pH=7.3的10mMHEPES)。将待测化合物或者空白对照加到含有40μM的14C-标记尿酸(54mCi/mmol)的缓冲液中,所述缓冲液含有125mM葡萄糖酸钠、4.8mM葡萄糖酸钾、1.2mM磷酸二氢钾、1.2mM硫酸镁、1.3mM葡萄糖酸钙、5.6mM葡萄糖、25mM HEPES,最终pH=7.3。96孔板在室温下培养10分钟,接着依次用50μL/孔和250μL/孔的上述清洗液各清洗三次。在96孔板上加入Microscint 20型液闪剂,板子在45℃下培养过夜,而后在TopCount Plate Reader上读数,并据此计算IC50。
结果如下列表所示。
本发明的部分化合物对URAT1的IC50值
| 化合物 | IC50(hURAT1,nM) |
| Lesinurad | 22.4 |
| I-1 | 8.3 |
| I-2 | 28.0 |
| I-3 | 14.7 |
| I-4 | 9.1 |
| I-6 | 35.6 |
| I-7 | 24.2 |
| I-8 | 20.5 |
上述IC50的测定结果表明,本发明化合物为强的URAT1抑制剂,可以用来制备治疗高尿酸血症和痛风的药物。
Claims (3)
1.下列化合物,
2.合成式I化合物的方法:
化合物II与α-溴代丙二酸二甲酯在碱存在下反应,得到化合物IV;化合物IV在溴仿中与亚硝酸钠和二氯乙酸反应得到化合物V;化合物V在碱性条件下水解得到化合物VI;化合物VI与1当量氧化剂氧化得到化合物I;其中R为F、Cl或Br。
3.权利要求1任一所述化合物在制备治疗高尿酸血症和痛风药物方面的用途。
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