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Site-Specific and Regiospecific Installation of Methylarginine Analogues into Recombinant Histones and Insights into Effector Protein Binding

机译:位点特异性和甲基精氨酸类似物的区域专一安装到重组组蛋白和洞察效应蛋白结合

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摘要

Arginine methylation has emerged as a widespread post-translational modification with influence over myriad cellular processes. However, the molecular mechanisms underlying such methylarginine-dependent phenomena remain unclear. To aid in this research, a facile method was developed to install methylarginine analogues on recombinant protein for use in biochemical, biophysical, and structural studies. Through chemical conjugation of novel α,β-unsaturated amidine precursors with proteins, methylarginine mimics can be displayed with control of methylation site, extent, and regiospecificity. Analogue installation into histones using this strategy produced modified proteins that were recognized by antibodies specific to endogenous methylarginine, and these histones retained the capacity to form mononucleosomes. Moreover, a native methylarginine-specific binding domain was shown to interact with methylarginine analogue-modified substrates. This chemical conjugation method for installing methylarginine analogues provides an efficient route to produce homogeneous modified proteins for subsequent investigations of methylarginine-dependent processes.
机译:精氨酸甲基化已作为一种广泛的翻译后修饰而出现,其影响了无数的细胞过程。但是,这种甲基精氨酸依赖性现象的分子机制仍不清楚。为了帮助这项研究,开发了一种简便的方法来在重组蛋白上安装甲基精氨酸类似物,以用于生物化学,生物物理和结构研究。通过新型α,β-不饱和am前体与蛋白质的化学结合,可以控制甲基化位点,程度和区域特异性来显示甲基精氨酸模拟物。使用这种策略将类似物安装到组蛋白中会产生修饰的蛋白,这些蛋白可以被内源性甲基精氨酸特异的抗体识别,这些组蛋白保留了形成单核小体的能力。此外,天然甲基精氨酸特异性结合域显示出与甲基精氨酸类似物修饰的底物相互作用。这种用于安装甲基精氨酸类似物的化学偶联方法为生产均质的修饰蛋白提供了一条有效途径,用于后续研究甲基精氨酸依赖性过程。

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