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Enzymatic Removal of Ribonucleotides from DNA Is Essential for Mammalian Genome Integrity and Development

机译:从DNA酶去除核糖核苷酸对于哺乳动物基因组完整性和发育至关重要

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摘要

The presence of ribonucleotides in genomic DNA is undesirable given their increased susceptibility to hydrolysis. Ribonuclease (RNase) H enzymes that recognize and process such embedded ribonucleotides are present in all domains of life. However, in unicellular organisms such as budding yeast, they are not required for viability or even efficient cellular proliferation, while in humans, RNase H2 hypomorphic mutations cause the neuroinflammatory disorder Aicardi-Goutières syndrome. Here, we report that RNase H2 is an essential enzyme in mice, required for embryonic growth from gastrulation onward. RNase H2 null embryos accumulate large numbers of single (or di-) ribonucleotides embedded in their genomic DNA (>1,000,000 per cell), resulting in genome instability and a p53-dependent DNA-damage response. Our findings establish RNase H2 as a key mammalian genome surveillance enzyme required for ribonucleotide removal and demonstrate that ribonucleotides are the most commonly occurring endogenous nucleotide base lesion in replicating cells.
机译:考虑到它们对水解的敏感性增加,在基因组DNA中不存在核糖核苷酸。识别和处理这种嵌入的核糖核苷酸的核糖核酸酶(RNase)H酶存在于生活的所有域中。然而,在诸如芽孢酵母之类的单细胞生物中,它们并不是生存力甚至不需要有效的细胞增殖所必需的,而在人类中,RNase H2亚型突变会引起神经炎性疾病艾卡迪-古特雷斯综合症。在这里,我们报道RNase H2是小鼠中必不可少的酶,从胚芽发育到胚胎生长都是必需的。 RNase H2空胚会在其基因组DNA中积聚大量的单(或二)核糖核苷酸(每个细胞> 1,000,000),导致基因组不稳定和p53依赖的DNA损伤反应。我们的发现将RNase H2建立为核糖核苷酸去除所需的关键哺乳动物基因组监测酶,并证明了核糖核苷酸是复制细胞中最常见的内源核苷酸碱基病变。

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