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解读非经典泛素信号传导:生物学与方法学

Deciphering non-canonical ubiquitin signaling: biology and methodology.

作者信息

van Overbeek Nila K, Aguirre Tim, van der Heden van Noort Gerbrand J, Blagoev Blagoy, Vertegaal Alfred C O

机构信息

Department of Cell and Chemical Biology, Leiden University Medical Center, Leiden, Netherlands.

Department of Biochemistry and Molecular Biology, University of Southern Denmark, Odense, Denmark.

出版信息

Front Mol Biosci. 2024 Feb 13;10:1332872. doi: 10.3389/fmolb.2023.1332872. eCollection 2023.

Abstract

Ubiquitination is a dynamic post-translational modification that regulates virtually all cellular processes by modulating function, localization, interactions and turnover of thousands of substrates. Canonical ubiquitination involves the enzymatic cascade of E1, E2 and E3 enzymes that conjugate ubiquitin to lysine residues giving rise to monomeric ubiquitination and polymeric ubiquitination. Emerging research has established expansion of the ubiquitin code by non-canonical ubiquitination of N-termini and cysteine, serine and threonine residues. Generic methods for identifying ubiquitin substrates using mass spectrometry based proteomics often overlook non-canonical ubiquitinated substrates, suggesting that numerous undiscovered substrates of this modification exist. Moreover, there is a knowledge gap between studies and comprehensive understanding of the functional consequence of non-canonical ubiquitination . Here, we discuss the current knowledge about non-lysine ubiquitination, strategies to map the ubiquitinome and their applicability for studying non-canonical ubiquitination substrates and sites. Furthermore, we elucidate the available chemical biology toolbox and elaborate on missing links required to further unravel this less explored subsection of the ubiquitin system.

摘要

泛素化是一种动态的翻译后修饰,通过调节数千种底物的功能、定位、相互作用和周转来调控几乎所有的细胞过程。典型的泛素化涉及E1、E2和E3酶的酶促级联反应,这些酶将泛素连接到赖氨酸残基上,从而产生单体泛素化和多聚泛素化。新兴研究表明,通过对N端以及半胱氨酸、丝氨酸和苏氨酸残基进行非典型泛素化可扩展泛素密码。使用基于质谱的蛋白质组学来鉴定泛素底物的通用方法常常忽略非典型泛素化的底物,这表明存在许多尚未被发现的这种修饰的底物。此外,在非典型泛素化的功能后果的研究和全面理解之间存在知识空白。在此,我们讨论关于非赖氨酸泛素化的现有知识、绘制泛素组图谱的策略及其在研究非典型泛素化底物和位点方面的适用性。此外,我们阐明了可用的化学生物学工具箱,并详细阐述了进一步揭示泛素系统中这个较少被探索的子部分所需的缺失环节。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/adc6/10897730/7273a356ae3d/fmolb-10-1332872-g001.jpg

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