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DNMT3B shapes the mCA landscape and regulates mCG for promoter bivalency in human embryonic stem cells

机译:DNMT3B将MCA横向形状,并调节MCG以进行人胚胎干细胞的启动子偏差

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摘要

DNMT3B is known as a de novo DNA methyltransferase. However, its preferential target sites for DNA methylation are largely unknown. Our analysis on ChIP-seq experiment in human embryonic stem cells (hESC) revealed that DNMT3B, mCA and H3K36me3 share the same genomic distribution profile. Deletion of DNMT3B or its histone-interacting domain (PWWP) demolished mCA in hESCs, suggesting that PWWP domain of DNMT3B directs the formation of mCA landscape. In contrast to the common presumption that PWWP guides DNMT3B-mediated mCG deposition, we found that deleting PWWP does not affect the mCG landscape. Nonetheless, DNMT3B knockout led to the formation of 2985 de novo hypomethylated regions at annotated promoter sites. Upon knockout, most of these promoters gain the bivalent marks, H3K4me3 and H3K27me3. We call them spurious bivalent promoters. Gene ontology analysis associated spurious bivalent promoters with development and cell differentiation. Overall, we found the importance of DNMT3B for shaping the mCA landscape and for maintaining the fidelity of the bivalent promoters in hESCs.
机译:DNMT3B称为DE Novo DNA甲基转移酶。然而,其用于DNA甲基化的优先靶位位点在很大程度上是未知的。我们对人胚胎干细胞(HESC)的芯片-SEQ实验分析显示DNMT3B,MCA和H3K36ME3共享相同的基因组分布曲线。删除DNMT3B或其组蛋白交互域(PWWP)在HESC中拆除MCA,表明DNMT3B的PWWP域指示MCA景观的形成。与PWWP指导DNMT3B介导的MCG沉积的共同推测相比,我们发现删除PWWP不会影响MCG景观。尽管如此,DNMT3B敲除导致在注释的启动子位点处形成2985德诺甲基甲基化区。敲除,大多数这些启动子获得二价标记,H3K4ME3和H3K27ME3。我们称他们为虚假的二价促销员。基因本体学分析相关的杂散二价促进剂,具有发育和细胞分化。总的来说,我们发现DNMT3B为塑造MCA景观的重要性以及维持HESC中二价促进剂的保真度。

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  • 来源
    《Nucleic Acids Research》 |2019年第14期|共16页
  • 作者单位

    Natl Univ Singapore Canc Sci Inst Singapore 14 Med Dr 12-01 Singapore 117599 Singapore;

    Natl Univ Singapore Canc Sci Inst Singapore 14 Med Dr 12-01 Singapore 117599 Singapore;

    Natl Univ Singapore Canc Sci Inst Singapore 14 Med Dr 12-01 Singapore 117599 Singapore;

    Natl Univ Singapore Canc Sci Inst Singapore 14 Med Dr 12-01 Singapore 117599 Singapore;

    Cell Signaling Technol 3 Trask Lane Danvers MA 01923 USA;

    Cell Signaling Technol 3 Trask Lane Danvers MA 01923 USA;

    Natl Univ Singapore Canc Sci Inst Singapore 14 Med Dr 12-01 Singapore 117599 Singapore;

    Univ Piemonte Orientale Dept Translat Med I-28100 Novara NO Italy;

    Natl Univ Singapore Canc Sci Inst Singapore 14 Med Dr 12-01 Singapore 117599 Singapore;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
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