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Loss of heterozygosity preferentially occurs in early replicating regions in cancer genomes

机译:杂合性的丧失优先发生在癌症基因组的早期复制区域中

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Erroneous repair of DNA double-strand breaks by homologous recombination (HR) leads to loss of heterozygosity (LOH). Analysing 22 392 and 74 415 LOH events in 363 glioblastoma and 513 ovarian cancer samples, respectively, and using three different metrics, we report that LOH selectively occurs in early replicating regions; this pattern differs from the trends for point mutations and somatic deletions, which are biased toward late replicating regions. Our results are independent of BRCA1 and BRCA2 mutation status. The LOH events are significantly clustered near RNA polII-bound transcription start sites, consistent with the reports that slow replication near paused RNA polII might initiate HR-mediated repair. The frequency of LOH events is higher in the chromosomes with shorter inter-homolog distance inside the nucleus. We propose that during early replication, HR-mediated rescue of replication near paused RNA polII using homologous chromosomes as template leads to LOH. The difference in the preference for replication timing between different classes of genomic alterations in cancer genomes also provokes a testable hypothesis that replicating cells show changing preference between various DNA repair pathways, which have different levels of efficiency and fidelity, as the replication progresses.
机译:同源重组(HR)对DNA双链断裂的错误修复导致杂合性(LOH)的丧失。分别分析了363个胶质母细胞瘤和513个卵巢癌样本中的22392和74415个LOH事件,并使用三个不同的指标,我们报道了LOH选择性地发生在早期复制区域。这种模式不同于点突变和体细胞缺失的趋势,后者倾向于后期复制区域。我们的结果与BRCA1和BRCA2突变状态无关。 LOH事件明显聚集在RNA polII结合的转录起始位点附近,这与有关在暂停的RNA polII附近缓慢复制可能启动HR介导的修复的报道相一致。 LOH事件的频率在核内同源距离较短的染色体中较高。我们建议,在早期复制期间,使用同源染色体作为模板,HR介导的复制RNA polII附近的复制的挽救将导致LOH。癌症基因组中不同类别的基因组改变之间在复制时间上的偏好差异也引起了一个可检验的假设,即复制细胞在各种DNA修复途径之间表现出变化的偏好,这些途径随着复制的进行具有不同的效率和保真度。

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