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首页> 外文期刊>Epigenetics: official journal of the DNA Methylation Society >UHRF1, a modular multi-domain protein, regulates replication-coupled crosstalk between DNA methylation and histone modifications.
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UHRF1, a modular multi-domain protein, regulates replication-coupled crosstalk between DNA methylation and histone modifications.

机译:UHRF1是一种模块化的多域蛋白,可调节DNA甲基化与组蛋白修饰之间的复制偶联串扰。

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摘要

Cytosine methylation in DNA is a major epigenetic signal, and plays a central role in propagating chromatin status during cell division. However the mechanistic links between DNA methylation and histone methylation are poorly understood. A multi-domain protein UHRF1 (ubiquitin-like, containing PHD and RING finger domains 1) is required for DNA CpG maintenance methylation at replication forks, and mouse UHRF1-null cells show enhanced susceptibility to DNA replication arrest and DNA damaging agents. Recent data demonstrated that the SET and RING associated (SRA) domain of UHRF1 binds hemimethylated CpG and flips 5-methylcytosine out of the DNA helix, whereas its tandom tudor domain and PHD domain bind the tail of histone H3 in a highly methylation sensitive manner. We hypothesize that UHRF1 brings the two components (histones and DNA) carrying appropriate markers (on the tails of H3 and hemimethylated CpG sites) ready to be assembled into a nucleosome after replication.
机译:DNA中的胞嘧啶甲基化是主要的表观遗传信号,并且在细胞分裂过程中在传播染色质状态中起着核心作用。然而,人们对DNA甲基化和组蛋白甲基化之间的机制联系了解甚少。复制叉处的DNA CpG维持甲基化需要多域蛋白UHRF1(类泛素,包含PHD和RING指域1),小鼠UHRF1空细胞显示出对DNA复制停止和DNA破坏剂的敏感性增加。最近的数据表明,UHRF1的SET和RING相关(SRA)域与半甲基化的CpG结合,并将5-甲基胞嘧啶从DNA螺旋中翻转出来,而其固有的tudor域和PHD域则以高度甲基化敏感的方式与组蛋白H3的尾部结合。我们假设UHRF1使携带适当标记的两个组分(组蛋白和DNA)(在H3的尾部和半甲基化的CpG位点)准备好在复制后组装成核小体。

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