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串联质谱技术在磷酸化蛋白质组学分析中的应用。

Tandem mass spectrometry strategies for phosphoproteome analysis.

机构信息

Department of Chemistry, Michigan State University, East Lansing, USA.

出版信息

Mass Spectrom Rev. 2011 Jul-Aug;30(4):600-25. doi: 10.1002/mas.20310. Epub 2011 Feb 3.

Abstract

Protein phosphorylation is involved in nearly all essential biochemical pathways and the deregulation of phosphorylation events has been associated with the onset of numerous diseases. A multitude of tandem mass spectrometry (MS/MS) and multistage MS/MS (i.e., MS(n) ) strategies have been developed in recent years and have been applied toward comprehensive phosphoproteomic analysis, based on the interrogation of proteolytically derived phosphopeptides. However, the utility of each of these MS/MS and MS(n) approaches for phosphopeptide identification and characterization, including phosphorylation site localization, is critically dependant on the properties of the precursor ion (e.g., polarity and charge state), the specific ion activation method that is employed, and the underlying gas-phase ion chemistries, mechanisms and other factors that influence the gas-phase fragmentation behavior of phosphopeptide ions. This review therefore provides an overview of recent studies aimed at developing an improved understanding of these issues, and highlights the advantages and limitations of both established (e.g., CID) and newly maturing (e.g., ECD, ETD, photodissociation, etc.) yet complementary, ion activation techniques. This understanding is expected to facilitate the continued refinement of existing MS/MS strategies, and the development of novel MS/MS techniques for phosphopeptide analysis, with great promise in providing new insights into the role of protein phosphorylation on normal biological function, and in the onset and progression of disease. © 2011 Wiley Periodicals, Inc., Mass Spec Rev 30:600-625, 2011.

摘要

蛋白质磷酸化几乎涉及所有基本的生化途径,磷酸化事件的失调与许多疾病的发生有关。近年来,已经开发出了多种串联质谱(MS/MS)和多级 MS/MS(即 MS(n))策略,并应用于基于对酶解衍生的磷酸肽进行分析的全面磷酸蛋白质组学分析。然而,这些 MS/MS 和 MS(n) 方法中的每一种在用于磷酸肽鉴定和表征(包括磷酸化位点定位)中的用途,都取决于前体离子(例如极性和电荷状态)、所采用的特定离子活化方法以及基础气相离子化学、机制和其他影响磷酸肽离子气相碎片化行为的因素的特性。因此,本综述提供了对这些问题的最新研究的概述,并强调了成熟的(例如 ECD、ETD、光解离等)和新兴的(例如 CID)离子活化技术的优势和局限性。这种理解有望促进现有 MS/MS 策略的不断改进,以及用于磷酸肽分析的新型 MS/MS 技术的开发,这将为深入了解蛋白质磷酸化在正常生物学功能中的作用以及疾病的发生和发展提供新的见解。© 2011 年 Wiley 期刊,质谱评论 30:600-625,2011 年。

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