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人类蛋白质组中赖氨酸反应性和配体结合能力的全局分析。

Global profiling of lysine reactivity and ligandability in the human proteome.

机构信息

Department of Chemical Physiology, The Scripps Research Institute, La Jolla, California 92307, USA.

Department of Integrative Structural and Computational Biology, The Scripps Research Institute, La Jolla, California 92307, USA.

出版信息

Nat Chem. 2017 Dec;9(12):1181-1190. doi: 10.1038/nchem.2826. Epub 2017 Jul 31.

Abstract

Nucleophilic amino acids make important contributions to protein function, including performing key roles in catalysis and serving as sites for post-translational modification. Electrophilic groups that target amino-acid nucleophiles have been used to create covalent ligands and drugs, but have, so far, been mainly limited to cysteine and serine. Here, we report a chemical proteomic platform for the global and quantitative analysis of lysine residues in native biological systems. We have quantified, in total, more than 9,000 lysines in human cell proteomes and have identified several hundred residues with heightened reactivity that are enriched at protein functional sites and can frequently be targeted by electrophilic small molecules. We have also discovered lysine-reactive fragment electrophiles that inhibit enzymes by active site and allosteric mechanisms, as well as disrupt protein-protein interactions in transcriptional regulatory complexes, emphasizing the broad potential and diverse functional consequences of liganding lysine residues throughout the human proteome.

摘要

亲核氨基酸对蛋白质功能有重要贡献,包括在催化中发挥关键作用,以及作为翻译后修饰的位点。靶向氨基酸亲核试剂的亲电基团已被用于构建共价配体和药物,但迄今为止,主要限于半胱氨酸和丝氨酸。在这里,我们报告了一个用于在天然生物系统中全局和定量分析赖氨酸残基的化学蛋白质组学平台。我们总共定量了人类细胞蛋白质组中超过 9000 个赖氨酸,并鉴定了数百个反应性增强的残基,这些残基富集在蛋白质功能位点,并且可以经常被亲电子小分子靶向。我们还发现了通过活性位点和别构机制抑制酶的赖氨酸反应性片段亲电试剂,以及破坏转录调节复合物中的蛋白质-蛋白质相互作用,强调了在整个人类蛋白质组中配体赖氨酸残基的广泛潜力和多样化功能后果。

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