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Regulation of DNA Methylation Patterns by CK2-Mediated Phosphorylation of Dnmt3a

机译:CK2介导的Dnmt3a磷酸化对DNA甲基化模式的调控

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DNA methylation is a central epigenetic modification that is established by de novo DNA methyltransferases. The mechanisms underlying the generation of genomic methylation patterns are still poorly understood. Using mass spectrometry and a phosphospecific Dnmt3a antibody, we demonstrate that CK2 phosphorylates endogenous Dnmt3a at two key residues located near its PWWP domain, thereby downregulating the ability of Dnmt3a to methylate DNA. Genome-wide DNA methylation analysis shows that CK2 primarily modulates CpG methylation of several repeats, most notably of Alu SINEs. This modulation can be directly attributed to CK2-mediated phosphorylation of Dnmt3a. We also find that CK2-mediated phosphorylation is required for localization of Dnmt3a to heterochromatin. By revealing phosphorylation as a mode of regulation of de novo DNA methyltransferase function and by uncovering a mechanism for the regulation of methylation at repetitive elements, our results shed light on the origin of DNA methylation patterns.
机译:DNA甲基化是由从头DNA甲基转移酶建立的主要表观遗传修饰。基因组甲基化模式产生的机制仍知之甚少。使用质谱和磷酸特异性Dnmt3a抗体,我们证明CK2在位于其PWWP域附近的两个关键残基处磷酸化内源性Dnmt3a,从而下调Dnmt3a甲基化DNA的能力。全基因组DNA甲基化分析表明CK2主要调节几个重复序列(尤其是Alu SINE)的CpG甲基化。这种调节可直接归因于CK2介导的Dnmt3a磷酸化。我们还发现CK2介导的磷酸化是Dnmt3a定位于异染色质所必需的。通过揭示磷酸化作用作为从头调控DNA甲基转移酶功能的一种方式,并揭示出一种在重复元件上调控甲基化的机制,我们的研究结果揭示了DNA甲基化模式的起源。

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