Interfacial inhibitors of protein-nucleic acid interactions.

Current medicinal chemistry. Anti-cancer agents Pub Date : 2005-07-01 DOI:10.2174/1568011054222337

Yves Pommier, Christophe Marchand

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引用次数: 69

Abstract

This essay develops the paradigm of "Interfacial Inhibitors" (Pommier and Cherfils, TiPS, 2005, 28: 136) for inhibitory drugs beside orthosteric (competitive or non-competitive) and allosteric inhibitors. Interfacial inhibitors bind with high selectivity to a binding site involving two or more macromolecules within macromolecular complexes undergoing conformational changes. Interfacial binding traps (generally reversibly) a transition state of the complex, resulting in kinetic inactivation. The exemplary case of interfacial inhibitor of protein-DNA interface is camptothecin and its clinical derivatives. We will also provide examples generalizing the interfacial inhibitor concept to inhibitors of topoisomerase II (anthracyclines, ellipticines, epipodophyllotoxins), gyrase (quinolones, ciprofloxacin, norfloxacin), RNA polymerases (alpha-amanitin and actinomycin D), and ribosomes (antibiotics such as streptomycin, hygromycin B, tetracycline, kirromycin, fusidic acid, thiostrepton, and possibly cycloheximide). We discuss the implications of the interfacial inhibitor concept for drug discovery.

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蛋白质-核酸相互作用的界面抑制剂。

本文发展了“界面抑制剂”范式(Pommier和Cherfils, TiPS, 2005, 28: 136)，用于抑制药物，除了orthosteric(竞争性或非竞争性)和变构抑制剂。界面抑制剂与发生构象变化的大分子复合物中涉及两个或多个大分子的结合位点具有高选择性结合。界面结合陷阱(通常是可逆的)是复合物的过渡状态，导致动力学失活。蛋白质- dna界面抑制剂的典型例子是喜树碱及其临床衍生物。我们还将提供一些例子，将界面抑制剂的概念推广到拓扑异构酶II(蒽环类药物、椭圆类药物、表观卟啉毒素)、回旋酶(喹诺酮类药物、环丙沙星、诺氟沙星)、RNA聚合酶(α -amanitin和放线菌素D)和核糖体(抗生素，如链霉素、红霉素B、四环素、克罗霉素、氟西地酸、硫链霉素，可能还有环己亚胺)的抑制剂。我们讨论了界面抑制剂概念对药物发现的意义。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Current medicinal chemistry. Anti-cancer agents

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