Reversible Covalent Inhibition─Desired Covalent Adduct Formation by Mass Action

共价键 加合物 化学 组合化学 非共价相互作用 立体化学 有机化学 分子 氢键
作者
Disha Patel,Zil E Huma,Dustin Duncan
出处
期刊:ACS Chemical Biology [American Chemical Society]
卷期号:19 (4): 824-838 被引量:4
标识
DOI:10.1021/acschembio.3c00805
摘要

Covalent inhibition has seen a resurgence in the last several years. Although long-plagued by concerns of off-target effects due to nonspecific reactions leading to covalent adducts, there has been success in developing covalent inhibitors, especially within the field of anticancer therapy. Covalent inhibitors can have an advantage over noncovalent inhibitors since the formation of a covalent adduct may serve as an additional mode of selectivity due to the intrinsic reactivity of the target protein that is absent in many other proteins. Unfortunately, many covalent inhibitors form irreversible adducts with off-target proteins, which can lead to considerable side-effects. By designing the inhibitor to form reversible covalent adducts, one can leverage competing on/off kinetics in complex formation by taking advantage of the law of mass action. Although covalent adducts do form with off-target proteins, the reversible nature of inhibition prevents accumulation of the off-target adduct, thus limiting side-effects. In this perspective, we outline important characteristics of reversible covalent inhibitors, including examples and a guide for inhibitor development.
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