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通过丹磺酰氯串联质谱碎裂选择性检测和鉴定磷酸肽

Selective detection and identification of phosphopeptides by dansyl MS/MS/MS fragmentation.

作者信息

Amoresano Angela, Monti Gianluca, Cirulli Claudia, Marino Gennaro

机构信息

Department of Organic Chemistry and Biochemistry, Federico II University of Naples, Naples, Italy.

出版信息

Rapid Commun Mass Spectrom. 2006;20(9):1400-4. doi: 10.1002/rcm.2461.

Abstract

Protein phosphorylation regulates many cellular processes and pathways, such as cell cycle progression, signal transduction cascades and gene expression. Selective detection of phosphopeptides from proteolytic digests is a challenging and highly relevant task in many proteomics applications. Often phosphopeptides are present in small amounts and need selective isolation or enrichment before identification. Here we report a novel approach to label selectively phospho-Ser/-Thr residues by exploiting the features of a novel linear ion trap mass spectrometer. Using dansyl labelling and MS3 fragmentation, we developed a method useful for the large-scale proteomic profiling of phosphorylation sites. The new residues in the sequence were stable and easily identifiable under general conditions for tandem mass spectrometric sequencing.

摘要

蛋白质磷酸化调节许多细胞过程和信号通路,如细胞周期进程、信号转导级联反应和基因表达。在许多蛋白质组学应用中,从蛋白水解消化物中选择性检测磷酸肽是一项具有挑战性且高度相关的任务。通常,磷酸肽含量较少,在鉴定前需要进行选择性分离或富集。在此,我们报告了一种利用新型线性离子阱质谱仪的特性来选择性标记磷酸化丝氨酸/苏氨酸残基的新方法。通过丹磺酰氯标记和MS3碎片化,我们开发了一种可用于磷酸化位点大规模蛋白质组学分析的方法。在串联质谱测序的一般条件下,序列中的新残基稳定且易于识别。

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