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Differential DNA mismatch repair underlies mutation rate variation across the human genome

机译:差异DNA错配修复是整个人类基因组突变率变异的基础

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摘要

Cancer genome sequencing has revealed considerable variation in somatic mutation rates across the human genome, with mutation rates elevated inheterochromatic late replicating regionsand reduced in early replicating euchromatin(1-5). Multiple mechanisms have been suggested to underlie this(2,6-10), but the actual cause is unknown. Here we identify variable DNA mismatch repair (MMR) as the basis of this variation. Analysing similar to 17 million single-nucleotide variants from the genomes of 652 tumours, we show that regional autosomal mutation rates at megabase resolution are largely stable across cancer types, with differences related to changes in replication timing and gene expression. However, mutations arising after the inactivation of MMR are no longer enriched in late replicating heterochromatin relative to early replicating euchromatin. Thus, differential DNA repair and not differential mutation supply is the primary cause of the large-scale regional mutation rate variation across the human genome.
机译:癌症基因组测序已揭示出整个人类基因组中体细胞突变率的显着变化,其中异源色后期复制区域的突变率升高,而早期复制的常染色质则降低了突变率(1-5)。有人提出了多种机制来作为这个问题的基础(2,6-10),但实际原因尚不清楚。在这里,我们确定可变DNA错配修复(MMR)作为这种变异的基础。分析来自652个肿瘤的基因组的约1,700万个单核苷酸变体,我们显示,在百万碱基分辨率下的区域常染色体突变率在各种癌症类型中基本稳定,差异与复制时机和基因表达的变化有关。但是,相对于早期复制的常染色质,MMR失活后产生的突变不再富集在晚期复制的异染色质中。因此,差异DNA修复而不是差异突变供应是整个人类基因组中大规模区域突变率变化的主要原因。

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  • 来源
    《Nature》 |2015年第7550期|81-84|共4页
  • 作者

    Supek Fran; Lehner Ben;

  • 作者单位

    CRG, EMBL CRG Syst Biol Unit, Barcelona 08003, Spain|UPF, Barcelona 08003, Spain|Rudjer Boskovic Inst, Div Elect, Zagreb 10000, Croatia;

    CRG, EMBL CRG Syst Biol Unit, Barcelona 08003, Spain|UPF, Barcelona 08003, Spain|ICREA, Barcelona 08010, Spain;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
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  • 正文语种 eng
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