溴尿嘧啶
赖氨酸
乙酰化
乙酰转移酶
组蛋白
蛋白质组学
组蛋白乙酰转移酶
计算生物学
蛋白质组
乙酰转移酶
生物
生物化学
化学
氨基酸
基因
作者
Orlando Morales-Tarré,Ramiro Alonso-Bastida,Bolívar Arcos-Encarnación,Leonor Pérez-Martı́nez,Sergio Encarnación
标识
DOI:10.1080/14789450.2021.2007766
摘要
Introduction Lysine acetylation is a reversible post-translational modification (PTM) regulated through the action of specific types of enzymes: lysine acetyltransferases (KATs) and lysine deacetylases (HDACs), in addition to bromodomains, which are a group of conserved domains which identify acetylated lysine residues, several of the players in the process of protein acetylation, including enzymes and bromodomain-containing proteins, have been related to the progression of several diseases. The combination of high-resolution mass spectrometry-based proteomics, and immunoprecipitation to enrich acetylated peptides has contributed in recent years to expand the knowledge about this PTM described initially in histones and nuclear proteins, and is currently reported in more than 5000 human proteins, that are regulated by this PTM.Areas Covered This review presents an overview of the main participant elements, the scenario in the development of protein lysine acetylation, and its role in different human pathologies.Expert opinion Acetylation targets are practically all cellular processes in eukaryotes and prokaryotes organisms. Consequently, this modification has been linked to many pathologies like cancer, viral infection, obesity, diabetes, cardiovascular, and nervous system-associated diseases, to mention a few relevant examples. Accordingly, some intermediate mediators in the acetylation process have been projected as therapeutic targets.
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