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DNA replication timing and higher-order nuclear organization determine single-nucleotide substitution patterns in cancer genomes

机译:DNA复制时间和高级核组织决定了癌症基因组中的单核苷酸取代模式

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Single-nucleotide substitutions are a defining characteristic of cancer genomes. Many single-nucleotide substitutions in cancer genomes arise because of errors in DNA replication, which is spatio-temporally stratified. Here we propose that DNA replication patterns help shape the mutational landscapes of normal and cancer genomes. Using data on five fully sequenced cancer types and two personal genomes, we determined that the frequency of intergenic single-nucleotide substitution is significantly higher in late DNA replication timing regions, even after controlling for a number of genomic features. Furthermore, some substitution signatures are more frequent in certain DNA replication timing zones. Finally, integrating data on higher-order nuclear organization, we found that genomic regions in close spatial proximity to late-replicating domains display similar mutation spectra as the late-replicating regions themselves. These data suggest that DNA replication timing together with higher-order genomic organization contribute to the patterns of single-nucleotide substitution in normal and cancer genomes.
机译:单核苷酸取代是癌症基因组的定义特征。癌症基因组中的许多单核苷酸取代是由于DNA复制错误(时空分层)而出现的。在这里,我们建议DNA复制模式有助于塑造正常和癌症基因组的突变景观。使用关于五种完全测序的癌症类型和两个个人基因组的数据,我们确定了即使在控制了许多基因组特征之后,后期DNA复制时序区域中基因间单核苷酸取代的频率也明显更高。此外,某些替代签名在某些DNA复制时间段中更为常见。最后,通过对高阶核组织的数据进行整合,我们发现在空间上与后期复制域紧密接近的基因组区域显示出与后期复制区域本身相似的突变谱。这些数据表明,DNA复制时机以及更高阶的基因组组织有助于正常和癌症基因组中单核苷酸的替换。

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