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首页> 外文期刊>Bioorganic and medicinal chemistry >ACE inhibitors hypothesis generation for selective design, synthesis and biological evaluation of 3-mercapto-2-methyl-propanoyl-pyrrolidine-3-imine derivatives as antihypertensive agents.
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ACE inhibitors hypothesis generation for selective design, synthesis and biological evaluation of 3-mercapto-2-methyl-propanoyl-pyrrolidine-3-imine derivatives as antihypertensive agents.

机译:ACE抑制剂假说的产生,可作为抗高血压药的3-巯基-2-甲基丙酰基-吡咯烷-3-亚胺衍生物的选择性设计,合成和生物学评估。

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摘要

A series of new 3-mercapto-2-methyl-propanoyl-pyrrolidine derivatives (V, VIa-e) were designed. A new validated ACE inhibitors pharmacophore model (hypothesis) was generated for the first time in this research from the biologically active (frozen) conformation of Lisinopril-Human ACE complex that was downloaded from PDB, using stepwise technique of CATALYST modules. The molecular modeling compare-fit study of the designed molecules (V, VIa-e), with such ACE inhibitors hypothesis was fulfilled, and several compounds showed significant high simulation fit values. The compounds with high fit values were synthesized and biologically evaluated in vivo as hypotensive agents. It appears that the in vivo hypotensive activity of compounds V, VIa, VIb, and VIe was consistent with their molecular modeling results, and compound VIe showed the highest activity in comparison to Captopril.
机译:设计了一系列新的3-巯基-2-甲基-丙酰基-吡咯烷衍生物(V,VIa-e)。在这项研究中,首次使用从PDB下载的Lisinopril-Human ACE复合物的生物活性(冻结)构象,使用CATALYST模块的逐步技术,生成了一个新的经过验证的ACE抑制剂药效团模型(假设)。使用这种ACE抑制剂的假设,对设计分子(V,VIa-e)进行了分子建模比较拟合研究,并且几种化合物显示出很高的模拟拟合值。合成具有高拟合值的化合物,并在体内作为降压药进行生物学评估。似乎化合物V,VIa,VIb和VIe的体内降压活性与其分子建模结果一致,并且与卡托普利相比,化合物VIe表现出最高的活性。

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