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Structural insight into maintenance methylation by mouse DNA methyltransferase 1 (Dnmt1)

机译:小鼠DNA甲基转移酶1(Dnmt1)对维持甲基化的结构洞察

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摘要

Methylation of cytosine in DNA plays a crucial role in development through inheritable gene silencing. The DNA methyltransferase Dnmt1 is responsible for the propagation of methylation patterns to the next generation via its preferential methylation of hemimethylated CpG sites in the genome; however, how Dnmt1 maintains methylation patterns is not fully understood. Here we report the crystal structure of the large fragment (291–1620) of mouse Dnmt1 and its complexes with cofactor S-adenosyl-L-methionine and its product S-adenosyl-L-homocystein. Notably, in the absence of DNA, the N-terminal domain responsible for targeting Dnmt1 to replication foci is inserted into the DNA-binding pocket, indicating that this domain must be removed for methylation to occur. Upon binding of S-adenosyl-L-methionine, the catalytic cysteine residue undergoes a conformation transition to a catalytically competent position. For the recognition of hemimethylated DNA, Dnmt1 is expected to utilize a target recognition domain that overhangs the putative DNA-binding pocket. Taking into considerations the recent report of a shorter fragment structure of Dnmt1 that the CXXC motif positions itself in the catalytic pocket and prevents aberrant de novo methylation, we propose that maintenance methylation is a multistep process accompanied by structural changes.
机译:DNA中胞嘧啶的甲基化通过可遗传的基因沉默在发育中起关键作用。 DNA甲基转移酶Dnmt1通过基因组中半甲基化CpG位点的优先甲基化,负责甲基化模式向下一代的传播。但是,Dnmt1如何维持甲基化模式尚不完全清楚。在这里,我们报告小鼠Dnmt1的大片段(291–1620)的晶体结构及其与辅因子S-腺苷-L-蛋氨酸及其产物S-腺苷-L-同型半胱氨酸的复合物。值得注意的是,在没有DNA的情况下,负责将Dnmt1靶向复制灶的N末端结构域插入了DNA结合袋中,表明必须除去该结构域才能发生甲基化。在结合S-腺苷-L-甲硫氨酸后,催化的半胱氨酸残基经历构象转变至催化活性位置。为了识别半甲基化的DNA,Dnmt1有望利用突出于假定的DNA结合口袋的目标识别域。考虑到Dnmt1的较短片段结构的最新报道,即CXXC基序将其自身定位在催化口袋中并防止了异常的从头甲基化,我们建议维持甲基化是一个伴随结构变化的多步过程。

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