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首页> 外文期刊>Cell Reports >Proteome-wide Prediction of Lysine Methylation Leads to Identification of H2BK43 Methylation and Outlines the Potential Methyllysine Proteome
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Proteome-wide Prediction of Lysine Methylation Leads to Identification of H2BK43 Methylation and Outlines the Potential Methyllysine Proteome

机译:丙氨酸甲基化的蛋白质组预测导致H2BK43甲基化的鉴定,并概述了潜在的甲基氰基蛋白质

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Protein Lys methylation plays a critical role in numerous cellular processes, but it is challenging to identify Lys methylation in a systematic manner. Here we present an approach combining in silico prediction with targeted mass spectrometry (MS) to identify Lys methylation (Kme) sites at the proteome level. We develop MethylSight, a program that predicts Kme events solely on the physicochemical properties of residues surrounding the putative methylation sites, which then requires validation by targeted MS. Using this approach, we identify 70 new histone Kme marks with a 90% validation rate. H2BK43me2, which undergoes dynamic changes during stem cell differentiation, is found to be a substrate of KDM5b. Furthermore, MethylSight predicts that Lys methylation is a prevalent post-translational modification in the human proteome. Our work provides a useful resource for guiding systematic exploration of the role of Lys methylation in human health and disease.
机译:蛋白质Lys甲基化在许多细胞过程中起着关键作用,但以系统的方式鉴定Lys甲基化是挑战性的。在这里,我们提出了一种在靶标质谱(MS)中的硅预测中的方法,以鉴定蛋白质组水平的Lys甲基化(KME)位点。我们开发Methylsight,该程序仅预测了KME事件,仅仅是围绕推定甲基化位点周围的残留物的物理化学性质,然后通过靶向MS进行验证。使用这种方法,我们识别70个具有90%的验证率的新组代码标记。在干细胞分化期间经过动态变化的H2BK43ME2是KDM5B的基材。此外,甲基岩预测Lys甲基化是人蛋白质组中普遍的翻译后修饰。我们的工作提供了指导系统探索Lys甲基化在人体健康和疾病中的作用的有用资源。

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