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用于研究泛素系统的质谱技术。

Mass spectrometry techniques for studying the ubiquitin system.

作者信息

Heap Rachel E, Gant Megan S, Lamoliatte Frederic, Peltier Julien, Trost Matthias

机构信息

Institute for Cell and Molecular Biosciences, Newcastle University, Framlington Place, Newcastle-upon-Tyne, U.K.

出版信息

Biochem Soc Trans. 2017 Oct 15;45(5):1137-1148. doi: 10.1042/BST20170091. Epub 2017 Sep 22.

Abstract

Post-translational control of proteins through covalent attachment of ubiquitin plays important roles in all eukaryotic cell functions. The ubiquitin system in humans consists of 2 E1, 35 E2 and >600 E3 ubiquitin ligases as well as hundreds of deubiquitylases, which reverse ubiquitin attachment. Moreover, there are hundreds of proteins with ubiquitin-binding domains that bind one of the eight possible polyubiquitin chains. Dysfunction of the ubiquitin system is associated with many diseases such as cancer, autoimmunity and neurodegeneration, demonstrating the importance of ubiquitylation. Therefore, enzymes of the ubiquitin system are considered highly attractive drug targets. In recent years, mass spectrometry (MS)-based techniques have become increasingly important in the deciphering of the ubiquitin system. This short review addresses the state-of-the-art MS techniques for the identification of ubiquitylated proteins and their ubiquitylation sites. We also discuss the identification and quantitation of ubiquitin chain topologies and highlight how the activity of enzymes in the ubiquitin pathway can be measured. Finally, we present current MS tools that can be used for drug discovery in the ubiquitin space.

摘要

通过泛素的共价连接对蛋白质进行的翻译后调控在所有真核细胞功能中都起着重要作用。人类的泛素系统由2种E1、35种E2和超过600种E3泛素连接酶以及数百种去泛素化酶组成,后者可逆转泛素的连接。此外,还有数百种具有泛素结合结构域的蛋白质,它们可结合8种可能的多聚泛素链中的一种。泛素系统功能失调与许多疾病相关,如癌症、自身免疫和神经退行性疾病,这表明了泛素化的重要性。因此,泛素系统的酶被认为是极具吸引力的药物靶点。近年来,基于质谱(MS)的技术在泛素系统的解析中变得越来越重要。这篇简短的综述阐述了用于鉴定泛素化蛋白质及其泛素化位点的最新MS技术。我们还讨论了泛素链拓扑结构的鉴定和定量,并强调了如何测量泛素途径中酶的活性。最后,我们介绍了目前可用于泛素领域药物发现的MS工具。

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