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蛋白质组规模的蛋白质磷酸化分析。

Analysis of protein phosphorylation on a proteome-scale.

作者信息

Collins Mark O, Yu Lu, Choudhary Jyoti S

机构信息

Proteomic Mass Spectrometry, Wellcome Trust Sanger Institute, Hinxton, Cambridge, UK.

出版信息

Proteomics. 2007 Aug;7(16):2751-68. doi: 10.1002/pmic.200700145.

Abstract

Phosphorylation, the most intensively studied and common PTM on proteins, is a complex biological phenomenon. Its complexity manifests itself in the large numbers of proteins that attach it, remove it and recognise it as a protein code. Since the first report of protein phosphorylation on vitellin 100 years ago, a wide variety of biochemical and analytical chemical approaches have been developed to enrich and detect protein phosphorylation. The last 5 years have witnessed a renaissance in methodologies capable of characterising protein phosphorylation on a proteome-scale. These technological advances have allowed identification of hundreds to thousands of phosphorylation sites in a proteome and have resulted in a profound paradigm shift. For the first time, using quantitative MS, the topology and significance of global phosphorylation networks may be investigated, marking a new era of cell signalling research. This review addresses recent technological advances in the purification of phosphorylated proteins and peptides and current MS-based strategies used to qualitatively and quantitatively probe these enriched phosphoproteomes. In addition, we review the application of complementary array-based technologies to derive signalling networks from kinase-substrate interactions and discuss future challenges in the field.

摘要

磷酸化是蛋白质上研究最为深入且常见的一种翻译后修饰(PTM),是一种复杂的生物学现象。其复杂性体现在大量能添加、去除磷酸化修饰并将其识别为蛋白质编码的蛋白质上。自100年前首次报道卵黄磷蛋白的蛋白质磷酸化以来,人们已开发出各种各样的生化和分析化学方法来富集和检测蛋白质磷酸化。在过去5年中,能够在蛋白质组规模上表征蛋白质磷酸化的方法迎来了复兴。这些技术进步使得在一个蛋白质组中能够鉴定出成百上千个磷酸化位点,并导致了深刻的范式转变。首次利用定量质谱技术,可以研究全局磷酸化网络的拓扑结构和重要性,标志着细胞信号研究进入了一个新时代。本综述阐述了磷酸化蛋白质和肽段纯化方面的最新技术进展,以及当前用于定性和定量探测这些富集的磷酸化蛋白质组的基于质谱的策略。此外,我们还综述了基于互补阵列技术从激酶-底物相互作用推导信号网络的应用,并讨论了该领域未来面临的挑战。

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