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泛素结合蛋白:解码泛素介导的细胞功能。

Ubiquitin-binding proteins: decoders of ubiquitin-mediated cellular functions.

机构信息

Institute of Biochemistry II, School of Medicine, Goethe University, 60590 Frankfurt am Main, Germany.

出版信息

Annu Rev Biochem. 2012;81:291-322. doi: 10.1146/annurev-biochem-051810-094654. Epub 2012 Apr 5.

Abstract

Ubiquitin acts as a versatile cellular signal that controls a wide range of biological processes including protein degradation, DNA repair, endocytosis, autophagy, transcription, immunity, and inflammation. The specificity of ubiquitin signaling is achieved by alternative conjugation signals (monoubiquitin and ubiquitin chains) and interactions with ubiquitin-binding proteins (known as ubiquitin receptors) that decode ubiquitinated target signals into biochemical cascades in the cell. Herein, we review the current knowledge pertaining to the structural and functional features of ubiquitin-binding proteins and the mechanisms by which they recognize various types of ubiquitin topologies. The combinatorial use of diverse ubiquitin-binding domains (UBDs) in full-length proteins, selective recognition of chains with distinct linkages and length, and posttranslational modifications of ubiquitin receptors or multivalent interactions within protein complexes illustrate a few mechanisms by which a circuitry of signaling networks can be rewired by ubiquitin-binding proteins to control cellular functions in vivo.

摘要

泛素作为一种通用的细胞信号,控制着包括蛋白质降解、DNA 修复、内吞作用、自噬、转录、免疫和炎症在内的广泛的生物学过程。泛素信号的特异性是通过替代的连接信号(单泛素和泛素链)和与泛素结合蛋白(称为泛素受体)的相互作用来实现的,这些泛素受体将泛素化靶信号解码为细胞内的生化级联反应。在此,我们综述了有关泛素结合蛋白的结构和功能特征以及它们识别各种类型泛素拓扑结构的机制的现有知识。全长蛋白中不同泛素结合结构域(UBD)的组合使用、对具有不同连接和长度的链的选择性识别以及泛素受体或蛋白质复合物内多价相互作用的翻译后修饰,说明了泛素结合蛋白通过控制体内细胞功能来重新布线信号网络的电路的几种机制。

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