醛糖还原酶抑制螺喹唑啉酮类药物的3d药效团分析。

Drug design and discovery Pub Date : 1999-08-01
K Nakao, M Asao, H Shirai, R Shimizu
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引用次数: 0

摘要

为了更好地设计新型醛糖还原酶抑制剂,我们通过比较分子场分析和酶抑制剂复合物的分子建模,分析了螺喹唑啉酮类化合物的结构与其对兔醛糖还原酶的抑制活性之间的关系。结果表明,以下相互作用对抑制活性的增强起作用;1)喹唑啉酮6′和7′位置取代基与Trp20、Val47、Tyr48、Tyr121和Phe122等疏水残基之间的疏水相互作用;2) 6′位电负性取代基与Gln49侧链之间形成静电相互作用;3)空间小的6′取代基与活性位点的互补配合。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
3D-pharmacophore analyses of aldose reductase inhibitory spiroquinazolinones.

In order to get an insight for designing novel inhibitors of aldose reductase, we analyzed relationships between structures of spiroquinazolinones and their inhibitory activities against rabbit aldose reductase by comparative molecular field analysis and molecular modeling of the enzyme-inhibitor complex. It was revealed that the following interactions were operative for the enhancement of inhibitory activity; 1) the hydrophobic interaction between substituents at the 6'- and 7'-position of quinazolinone and the hydrophobic residues such as Trp20, Val47, Tyr48, Tyr121 and Phe122; 2) the electrostatic interaction formed between electronegative substituents at the 6'-position and the side chain of Gln49; 3) the complementary fit of sterically small 6'-substituents to the active site.

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