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Nε-Formylation of lysine is a widespread post-translational modification of nuclear proteins occurring at residues involved in regulation of chromatin function

机译:赖氨酸的Nε-甲酰化是一种广泛的核蛋白翻译后修饰发生在染色质功能调节的残基上

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摘要

Post-translational modification of histones and other chromosomal proteins regulates chromatin conformation and gene activity. Methylation and acetylation of lysyl residues are among the most frequently described modifications in these proteins. Whereas these modifications have been studied in detail, very little is known about a recently discovered chemical modification, the Nε-lysine formylation, in histones and other nuclear proteins. Here we mapped, for the first time, the sites of lysine formylation in histones and several other nuclear proteins. We found that core and linker histones are formylated at multiple lysyl residues located both in the tails and globular domains of histones. In core histones, formylation was found at lysyl residues known to be involved in organization of nucleosomal particles that are frequently acetylated and methylated. In linker histones and high mobility group proteins, multiple formylation sites were mapped to residues with important role in DNA binding. Nε-lysine formylation in chromosomal proteins is relatively abundant, suggesting that it may interfere with epigenetic mechanisms governing chromatin function, which could lead to deregulation of the cell and disease.
机译:组蛋白和其他染色体蛋白的翻译后修饰可调节染色质构象和基因活性。赖氨酰残基的甲基化和乙酰化是这些蛋白质中最常描述的修饰。尽管已经对这些修饰进行了详细的研究,但对最近发现的化学修饰(组蛋白和其他核蛋白中的N ε-赖氨酸甲酰化)知之甚少。在这里,我们首次绘制了组蛋白和其他几种核蛋白中赖氨酸甲酰化的位点。我们发现,核心和接头组蛋白在位于组蛋白尾部和球状结构域中的多个赖氨酰残基处被甲酰化。在核心组蛋白中,甲酰化被发现在赖氨酰残基上,而赖氨酰残基已知与核糖体颗粒的组织有关,这些颗粒通常被乙酰化和甲基化。在接头组蛋白和高迁移率族蛋白中,多个甲酰化位点被定位到在DNA结合中起重要作用的残基。染色体蛋白中N ε-赖氨酸的甲酰化作用相对丰富,表明它可能干扰控制染色质功能的表观遗传机制,从而导致细胞和疾病的失调。

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