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Homology-mediated end-capping as a primary step of sister chromatid fusion in the breakage-fusion-bridge cycles

机译:同源性介导的封端作为断裂-融合桥循环中姐妹染色单体融合的第一步

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摘要

Breakage-fusion-bridge (BFB) cycle is a series of chromosome breaks and duplications that could lead to the increased copy number of a genomic segment (gene amplification). A critical step of BFB cycles leading to gene amplification is a palindromic fusion of sister chromatids following the rupture of a dicentric chromosome during mitosis. It is currently unknown how sister chromatid fusion is produced from a mitotic break. To delineate the process, we took an integrated genomic, cytogenetic and molecular approach for the recurrent MCL1 amplicon at chromosome 1 in human tumor cells. A newly developed next-generation sequencing-based approach identified a cluster of palindromic fusions within the amplicon at similar to 50-kb intervals, indicating a series of breaks and fusions by BFB cycles. The physical location of the amplicon (at the end of a broken chromosome) further indicated BFB cycles as underlying processes. Three palindromic fusions were mediated by the homologies between two nearby inverted Alu repeats, whereas the other two fusions exhibited microhomology-mediated events. Such breakpoint sequences indicate that homology-mediated fold-back capping of broken ends followed by DNA replication is an underlying mechanism of sister chromatid fusion. Our results elucidate nucleotide-level events during BFB cycles and end processing for naturally occurring mitotic breaks.
机译:断裂融合桥(BFB)循环是一系列染色体断裂和重复,可能导致基因组片段的拷贝数增加(基因扩增)。 BFB循环导致基因扩增的关键步骤是有丝分裂期间双着丝粒染色体破裂后姐妹染色单体的回文融合。目前尚不清楚如何从有丝分裂中产生姐妹染色单体融合。为了描述该过程,我们对人类肿瘤细胞中1号染色体上的MCL1复发分子采取了基因组学,细胞遗传学和分子生物学的综合方法。一种新开发的基于下一代测序的方法在扩增子中以大约50 kb的间隔识别出回文融合簇,表明通过BFB循环发生了一系列断裂和融合。扩增子的物理位置(在断裂的染色体末端)进一步表明BFB循环是潜在的过程。三个回文融合由两个附近的反向Alu重复之间的同源性介导,而其他两个融合表现出微同源性介导的事件。此类断点序列表明,同源介导的折断末端折叠后加DNA复制是姐妹染色单体融合的潜在机制。我们的结果阐明了BFB循环和自然发生的有丝分裂断裂的最终加工过程中的核苷酸水平事件。

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