泛素样蛋白修饰级联反应中的曲折。

Twists and turns in ubiquitin-like protein conjugation cascades.

机构信息

Department of Structural Biology and Tumor Cell Biology and Howard Hughes Medical Institute, St. Jude Children's Research Hospital, Memphis, Tennessee 38105, USA.

出版信息

Protein Sci. 2011 Dec;20(12):1941-54. doi: 10.1002/pro.750. Epub 2011 Nov 9.

DOI:10.1002/pro.750

PMID:22012881

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3302639/

Abstract

Post-translational modification by ubiquitin-like proteins (UBLs) is a predominant eukaryotic regulatory mechanism. The vast reach of this form of regulation extends to virtually all eukaryotic processes that involve proteins. UBL modifications play critical roles in controlling the cell cycle, transcription, DNA repair, stress responses, signaling, immunity, plant growth, embryogenesis, circadian rhythms, and a plethora of other pathways. UBLs dynamically modulate target protein properties including enzymatic activity, conformation, half-life, subcellular localization, and intermolecular interactions. Moreover, the enzymatic process of UBL ligation to proteins is itself dynamic, with the UBL moving between multiple enzyme active sites and ultimately to a target. This review highlights our work on how the dynamic conformations of selected enzymes catalyzing UBL ligation help mediate this fascinating form of protein regulation.

摘要

泛素样蛋白（UBLs）的翻译后修饰是真核生物的主要调控机制。这种调控形式的广泛作用几乎涉及到所有涉及蛋白质的真核生物过程。UBL 修饰在控制细胞周期、转录、DNA 修复、应激反应、信号转导、免疫、植物生长、胚胎发生、昼夜节律等多种途径中发挥着关键作用。UBL 动态调节靶蛋白的特性，包括酶活性、构象、半衰期、亚细胞定位和分子间相互作用。此外，UBL 与蛋白质连接的酶促过程本身也是动态的，UBL 在多个酶活性位点之间移动，最终到达靶标。本综述重点介绍了我们在研究催化 UBL 连接的选定酶的动态构象如何帮助介导这种迷人的蛋白质调控形式方面的工作。

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