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首页> 外文期刊>Nucleic Acids Research >The DNA methyltransferases associate with HP1 and the SUV39H1 histone methyltransferase
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The DNA methyltransferases associate with HP1 and the SUV39H1 histone methyltransferase

机译:DNA甲基转移酶与HP1和SUV39H1组蛋白甲基转移酶相关

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The DNA methyltransferases, Dnmts, are the enzymes responsible for methylating DNA in mammals, which leads to gene silencing. Repression by DNA methylation is mediated partly by recruitment of the methyl-CpG-binding protein MeCP2. Recently, MeCP2 was shown to associate and facilitate histone methylation at Lys9 of H3, which is a key epigenetic modification involved in gene silencing. Here, we show that endogenous Dnmt3a associates primarily with histone H3-K9 methyltransferase activity as well as, to lesser extent, with H3-K4 enzymatic activity. The association with enzymatic activity is mediated by the conserved PHD-like motif of Dnmt3a. The H3-K9 histone methyltransferase that binds Dnmt3a is likely the H3-K9 specific SUV39H1 enzyme since we find that it interacts both in vitro and in vivo with Dnmt3a, using its PHD-like motif. We find that SUV39H1 also binds to Dnmt1 and, consistent with these interactions, SUV39H1 can purify DNA methyltransferase activity from nuclear extracts. In addition, we show that HP1β, a SUV39H1-interacting partner, binds directly to Dnmt1 and Dnmt3a and that native HP1β associates with DNA methyltransferase activity. Our data show a direct connection between the enzymes responsible for DNA methylation and histone methylation. These results further substantiate the notion of a self-reinforcing repressive chromatin state through the interplay between these two global epigenetic modifications.
机译:DNA甲基转移酶Dnmts是负责哺乳动物中DNA甲基化的酶,可导致基因沉默。 DNA甲基化的抑制作用部分地由募集甲基CpG结合蛋白MeCP2介导。最近,MeCP2被证明与H3的Lys9结合并促进组蛋白甲基化,这是参与基因沉默的关键表观遗传修饰。在这里,我们显示内源性Dnmt3a主要与组蛋白H3-K9甲基转移酶活性相关,以及在较小程度上与H3-K4酶活性相关。与酶活性的关联是由Dnmt3a的保守PHD样基序介导的。结合Dnmt3a的H3-K9组蛋白甲基转移酶很可能是H3-K9特异的SUV39H1酶,因为我们发现它利用PHD样基序与Dnmt3a在体内和体外相互作用。我们发现SUV39H1也与Dnmt1结合,并且与这些相互作用一致,SUV39H1可以从核提取物中纯化DNA甲基转移酶活性。此外,我们表明,与SUV39H1相互作用的伴侣HP1β直接与Dnmt1和Dnmt3a结合,并且天然HP1β与DNA甲基转移酶活性相关。我们的数据显示了负责DNA甲基化和组蛋白甲基化的酶之间的直接联系。这些结果通过这两个全局表观遗传修饰之间的相互作用进一步证实了自我增强的抑制染色质状态。

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