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活性位点结合物的非竞争性抑制。

Non-competitive inhibition by active site binders.

机构信息

Department of Mechanistic Biochemistry, Bristol-Myers Squibb Company, Rt. 206 and Provinceline Rd., Princeton, NJ 08543, USA.

出版信息

Chem Biol Drug Des. 2010 Jun;75(6):535-40. doi: 10.1111/j.1747-0285.2010.00972.x. Epub 2010 Mar 30.

Abstract

Classical enzymology has been used for generations to understand the interactions of inhibitors with their enzyme targets. Enzymology tools enabled prediction of the biological impact of inhibitors as well as the development of novel, more potent, ones. Experiments designed to examine the competition between the tested inhibitor and the enzyme substrate(s) are the tool of choice to identify inhibitors that bind in the active site. Competition between an inhibitor and a substrate is considered a strong evidence for binding of the inhibitor in the active site, while the lack of competition suggests binding to an alternative site. Nevertheless, exceptions to this notion do exist. Active site-binding inhibitors can display non-competitive inhibition patterns. This unusual behavior has been observed with enzymes utilizing an exosite for substrate binding, isomechanism enzymes, enzymes with multiple substrates and/or products and two-step binding inhibitors. In many of these cases, the mechanisms underlying the lack of competition between the substrate and the inhibitor are well understood. Tools like alternative substrates, testing the enzyme reaction in the reverse direction and monitoring inhibition time dependence can be applied to enable distinction between 'badly behaving' active site binders and true exosite inhibitors.

摘要

经典酶学已经被使用了几代人,用于了解抑制剂与酶靶标的相互作用。酶学工具使我们能够预测抑制剂的生物学影响,并开发出更有效、更具潜力的新型抑制剂。设计用于检查测试抑制剂与酶底物之间竞争的实验是识别抑制剂结合在活性部位的首选工具。抑制剂与底物之间的竞争被认为是抑制剂结合在活性部位的有力证据,而缺乏竞争则表明结合在替代部位。然而,这种观点也存在例外。活性部位结合抑制剂可能显示非竞争性抑制模式。这种不寻常的行为已经在利用变构部位结合底物的酶、同工酶、具有多个底物和/或产物的酶以及两步结合抑制剂中观察到。在许多情况下,缺乏底物和抑制剂之间竞争的机制已经得到很好的理解。可以应用替代底物等工具,测试酶反应的逆方向,并监测抑制时间依赖性,以区分“行为不良”的活性部位结合物和真正的变构抑制剂。

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