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一种用于探测蛋白质甲基化的电荷抑制策略。

A charge-suppressing strategy for probing protein methylation.

作者信息

Ning Zhibin, Star Alexandra Therese, Mierzwa Anna, Lanouette Sylvain, Mayne Janice, Couture Jean-Francois, Figeys Daniel

机构信息

Ottawa Institute of Systems Biology, Department of Biochemistry, Immunology and Microbiology, Faculty of Medicine, University of Ottawa, Ontario, Canada.

出版信息

Chem Commun (Camb). 2016 Apr 7;52(31):5474-7. doi: 10.1039/c6cc00814c.

Abstract

Methylation of arginine and lysine (RK) residues play essential roles in epigenetics and the regulation of gene expression. However, research in this area is often hindered by the lack of effective tools for probing the protein methylation. Here, we present an antibody-free strategy to capture protein methylation on RK residues by using chemical reactions to eliminate the charges on un-modified RK residues and peptide N-termini. Peptides containing methylated RK residues remain positively charged and are then enriched by strong cation exchange chromatography, followed by high-resolution mass spectrometry identification.

摘要

精氨酸和赖氨酸(RK)残基的甲基化在表观遗传学和基因表达调控中起着至关重要的作用。然而,该领域的研究常常受到缺乏有效探测蛋白质甲基化工具的阻碍。在此,我们提出一种无抗体策略,通过化学反应消除未修饰的RK残基和肽N端的电荷,以捕获RK残基上的蛋白质甲基化。含有甲基化RK残基的肽仍带正电荷,随后通过强阳离子交换色谱法进行富集,接着进行高分辨率质谱鉴定。

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