胃(H+/K+)- atp酶抑制剂的定量构效关系研究。

Drug design and delivery Pub Date : 1991-04-01
P Singh, R C Sharma, T N Ojha
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引用次数: 0

摘要

发现奥美拉唑类似物(图1)和1-芳基-4-甲基-2,3-二氢吡罗[3,2-c]喹啉(图2)的(H+/K+)- atp酶抑制活性与控制分子碱度的电子(sigma)或pKa参数显著相关。前者是不可逆阻滞剂的代表,后者是可逆阻滞剂的代表。包含疏水(pi)和/或位阻(Es)参数有时会导致相关性的改善,这表明这些参数可能在环状中间体的形成中起作用。推导出的显著相关方程有力地支持了Lindberg等人首先提出的涉及这种循环中间体的作用机制。
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Quantitative structure-activity relationship studies of inhibitors of gastric (H+/K+)-ATPase.

The (H+/K+)-ATPase enzyme inhibitory activity of omeprazole analogues (Figure 1) and 1-aryl-4-methyl-2,3-dihydropyrrolo[3,2-c]quinolines (Figure 2) was found to be significantly correlated with electronic (sigma) or pKa parameter that governs the basicity of the molecules. The former compounds are representative of irreversible blockers, and the latter of reversible blockers. Inclusion of hydrophobic (pi) and/or steric (Es) parameters sometimes led to improvement in the correlations, suggesting that these parameters may play a role in the formation of a cyclic intermediate. The derived significant correlation equations strongly support a mechanism of action, first proposed by Lindberg et al., involving such a cyclic intermediate.

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