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Classical non-homologous end-joining pathway utilizes nascent RNA for error-free double-strand break repair of transcribed genes

机译:经典的非同源末端连接途径利用新生的RNA对转录的基因进行无错误的双链断裂修复

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摘要

DNA double-strand breaks (DSBs) leading to loss of nucleotides in the transcribed region can be lethal. Classical non-homologous end-joining (C-NHEJ) is the dominant pathway for DSB repair (DSBR) in adult mammalian cells. Here we report that during such DSBR, mammalian C-NHEJ proteins form a multiprotein complex with RNA polymerase II and preferentially associate with the transcribed genes after DSB induction. Depletion of C-NHEJ factors significantly abrogates DSBR in transcribed but not in non-transcribed genes. We hypothesized that nascent RNA can serve as a template for restoring the missing sequences, thus allowing error-free DSBR. We indeed found pre-mRNA in the C-NHEJ complex. Finally, when a DSB-containing plasmid with several nucleotides deleted within the E. coli lacZ gene was allowed time to repair in lacZ-expressing mammalian cells, a functional lacZ plasmid could be recovered from control but not C-NHEJ factor-depleted cells, providing important mechanistic insights into C-NHEJ-mediated error-free DSBR of the transcribed genome.
机译:导致转录区核苷酸丢失的DNA双链断裂(DSB)可能是致命的。经典的非同源末端连接(C-NHEJ)是成年哺乳动物细胞中DSB修复(DSBR)的主要途径。在这里,我们报道在这种DSBR期间,哺乳动物C-NHEJ蛋白与RNA聚合酶II形成多蛋白复合物,并在DSB诱导后优先与转录的基因缔合。 C-NHEJ因子的耗竭可显着消除已转录但未转录的基因中的DSBR。我们假设新生的RNA可以用作恢复缺失序列的模板,从而实现无错误的DSBR。我们确实在C-NHEJ复合物中发现了前mRNA。最后,当在大肠杆菌lacZ基因中缺失了几个核苷酸的含DSB的质粒在表达lacZ的哺乳动物细胞中有时间修复时,可以从对照中回收功能性lacZ质粒,但不能从C-NHEJ因子缺失的细胞中回收,提供了有关C-NHEJ介导的转录基因组无错误DSBR的重要机制的见解。

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