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The SRA domain of UHRF1 flips 5-methylcytosine out of the DNA helix

机译:UHRF1的SRA域将5-甲基胞嘧啶从DNA螺旋中翻转出来

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Maintenance methylation of hemimethylated CpG dinucleotides at DNA replication forks is the key to faithful mitotic inheritance of genomic methylation patterns. UHRF1 (ubiquitin-like, containing PHD and RING finger domains 1) is required for maintenance methylation by interacting with DNA nudeotide methyltransferase 1 (DNMT1), the maintenance methyltransferase, and with hemimethylated CpG, the substrate for DNMT1 (refs 1 and 2). Here we present the crystal structure of the SET and RING-associated (SRA) domain of mouse UHRF1 in complex with DNA containing a hemimethylated CpG site. The DNA is contacted in both the major and minor grooves by two loops that penetrate into the middle of the DNA helix. The 5-methylcytosine has flipped completely out of the DNA helix and is positioned in a binding pocket with planar stacking contacts, Watson-Crick polar hydrogen bonds and van der Waals interactions specific for 5-methylcytosine. Hence, UHRF1 contains a previously unknown DNA-binding module and is the first example of a non-enzymatic, sequence-specific DNA-binding protein domain to use the base flipping mechanism to interact with DNA.
机译:在DNA复制叉处维持半甲基化CpG二核苷酸的甲基化是基因组甲基化模式忠实有丝分裂遗传的关键。 UHRF1(类泛素,含有PHD和RING指结构域1)通过与DNA核苷酸甲基转移酶1(DNMT1),维持甲基转移酶和半甲基化的CpG(DNMT1的底物)相互作用来维持甲基化(参考文献1和2)。在这里,我们介绍与包含半甲基化CpG位点的DNA配合的小鼠UHRF1的SET和RING相关(SRA)域的晶体结构。 DNA在两个主要环和次要凹槽中都通过两个环相互接触,这些环渗透到DNA螺旋的中间。 5-甲基胞嘧啶已经完全脱离了DNA螺旋结构,并被定位在具有平面堆叠接触,Watson-Crick极性氢键和5-甲基胞嘧啶特有的范德华相互作用的结合口袋中。因此,UHRF1包含一个以前未知的DNA结合模块,并且是使用碱基翻转机制与DNA相互作用的非酶序列特异性DNA结合蛋白结构域的第一个示例。

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