3-Ethoxy-3-(3-methoxy-2-methyl-phenylimino)-propionic acid ethyl ester | 874124-78-4
中文名称
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中文别名
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英文名称
3-Ethoxy-3-(3-methoxy-2-methyl-phenylimino)-propionic acid ethyl ester
英文别名
ethyl 3-ethoxy-3-(3-methoxy-2-methylphenyl)iminopropanoate
CAS
874124-78-4
化学式
C15H21NO4
mdl
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分子量
279.336
InChiKey
NCDILZNMVZRXSZ-UHFFFAOYSA-N
BEILSTEIN
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EINECS
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物化性质
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计算性质
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ADMET
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安全信息
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SDS
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制备方法与用途
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上下游信息
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文献信息
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表征谱图
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同类化合物
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相关功能分类
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相关结构分类
计算性质
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辛醇/水分配系数(LogP):3
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重原子数:20
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可旋转键数:8
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环数:1.0
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sp3杂化的碳原子比例:0.47
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拓扑面积:57.1
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氢给体数:0
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氢受体数:5
反应信息
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作为反应物:描述:3-Ethoxy-3-(3-methoxy-2-methyl-phenylimino)-propionic acid ethyl ester 在 盐酸 、 caesium carbonate 、 三乙胺 、 sodium hydroxide 、 lithium hexamethyldisilazane 作用下, 以 四氢呋喃 、 1,4-二氧六环 、 N-甲基吡咯烷酮 、 甲醇 、 二苯醚 、 二氯甲烷 为溶剂, 反应 10.8h, 生成参考文献:名称:Discovery of Hepatitis C Virus NS3-4A Protease Inhibitors with Improved Barrier to Resistance and Favorable Liver Distribution摘要:Given the emergence of resistance observed for the current clinical-stage hepatitis C virus (HCV) NS3 protease inhibitors, there is a need for new inhibitors with a higher barrier to resistance. We recently reported our rational approach to the discovery of macrocyclic acylsulfonamides as HCV protease inhibitors addressing potency against clinically relevant resistant variants. Using X-ray crystallography of HCV protease variant/inhibitor complexes, we shed light on the complex structural mechanisms by which the D168V and R155K residue mutations confer resistance to NS3 protease inhibitors. Here, we disclose SAR investigation and ADME/PK optimization leading to the identification of inhibitors with significantly Unproved potency against the key resistant variants and with increased liver partitioning.DOI:10.1021/jm400121t
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作为产物:描述:参考文献:名称:Discovery of Hepatitis C Virus NS3-4A Protease Inhibitors with Improved Barrier to Resistance and Favorable Liver Distribution摘要:Given the emergence of resistance observed for the current clinical-stage hepatitis C virus (HCV) NS3 protease inhibitors, there is a need for new inhibitors with a higher barrier to resistance. We recently reported our rational approach to the discovery of macrocyclic acylsulfonamides as HCV protease inhibitors addressing potency against clinically relevant resistant variants. Using X-ray crystallography of HCV protease variant/inhibitor complexes, we shed light on the complex structural mechanisms by which the D168V and R155K residue mutations confer resistance to NS3 protease inhibitors. Here, we disclose SAR investigation and ADME/PK optimization leading to the identification of inhibitors with significantly Unproved potency against the key resistant variants and with increased liver partitioning.DOI:10.1021/jm400121t
文献信息
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ANTIVIRAL COMPOUNDS申请人:Cottell Jeromy J.公开号:US20140051626A1公开(公告)日:2014-02-20The invention is related to anti-viral compounds, compositions containing such compounds, and therapeutic methods that include the administration of such compounds, as well as to processes and intermediates useful for preparing such compounds.该发明涉及抗病毒化合物、含有这种化合物的组合物、包括给予这种化合物的治疗方法,以及用于制备这种化合物的过程和中间体。
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Antiviral compounds申请人:Gilead Sciences, Inc.公开号:US08809267B2公开(公告)日:2014-08-19The invention is related to anti-viral compounds, compositions containing such compounds, and therapeutic methods that include the administration of such compounds, as well as to processes and intermediates useful for preparing such compounds.这项发明涉及抗病毒化合物,包含这种化合物的组合物,以及包括给予这种化合物的治疗方法,还涉及用于制备这种化合物的过程和中间体。
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Discovery of Hepatitis C Virus NS3-4A Protease Inhibitors with Improved Barrier to Resistance and Favorable Liver Distribution作者:Benoît Moreau、Jeff A. O’Meara、Josée Bordeleau、Michel Garneau、Cedrickx Godbout、Vida Gorys、Mélissa Leblanc、Elisia Villemure、Peter W. White、Montse Llinàs-BrunetDOI:10.1021/jm400121t日期:2014.3.13Given the emergence of resistance observed for the current clinical-stage hepatitis C virus (HCV) NS3 protease inhibitors, there is a need for new inhibitors with a higher barrier to resistance. We recently reported our rational approach to the discovery of macrocyclic acylsulfonamides as HCV protease inhibitors addressing potency against clinically relevant resistant variants. Using X-ray crystallography of HCV protease variant/inhibitor complexes, we shed light on the complex structural mechanisms by which the D168V and R155K residue mutations confer resistance to NS3 protease inhibitors. Here, we disclose SAR investigation and ADME/PK optimization leading to the identification of inhibitors with significantly Unproved potency against the key resistant variants and with increased liver partitioning.
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