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亚端粒处的重组受物理距离、双链断裂切除和染色质状态的调控。

Recombination at subtelomeres is regulated by physical distance, double-strand break resection and chromatin status.

作者信息

Batté Amandine, Brocas Clémentine, Bordelet Hélène, Hocher Antoine, Ruault Myriam, Adjiri Adouda, Taddei Angela, Dubrana Karine

机构信息

Institute of Molecular and Cellular Radiobiology, CEA/DRF, Fontenay-aux-Roses cedex, France.

Inserm U967, Fontenay-aux-Roses cedex, France.

出版信息

EMBO J. 2017 Sep 1;36(17):2609-2625. doi: 10.15252/embj.201796631. Epub 2017 Jul 28.

Abstract

Homologous recombination (HR) is a conserved mechanism that repairs broken chromosomes via intact homologous sequences. How different genomic, chromatin and subnuclear contexts influence HR efficiency and outcome is poorly understood. We developed an assay to assess HR outcome by gene conversion (GC) and break-induced replication (BIR), and discovered that subtelomeric double-stranded breaks (DSBs) are preferentially repaired by BIR despite the presence of flanking homologous sequences. Overexpression of a silencing-deficient mutant led to active grouping of telomeres and specifically increased the GC efficiency between subtelomeres. Thus, physical distance limits GC at subtelomeres. However, the repair efficiency between reciprocal intrachromosomal and subtelomeric sequences varies up to 15-fold, depending on the location of the DSB, indicating that spatial proximity is not the only limiting factor for HR deletion limited the resection at subtelomeric DSBs and improved GC efficiency. The presence of repressive chromatin at subtelomeric DSBs also favoured recombination, by counteracting -mediated resection. Thus, repressive chromatin promotes HR at subtelomeric DSBs by limiting DSB resection and protecting against genetic information loss.

摘要

同源重组(HR)是一种保守的机制,通过完整的同源序列修复断裂的染色体。目前对于不同的基因组、染色质和亚核环境如何影响HR效率和结果了解甚少。我们开发了一种通过基因转换(GC)和断裂诱导复制(BIR)来评估HR结果的检测方法,并发现尽管存在侧翼同源序列,但端粒附近的双链断裂(DSB)优先通过BIR进行修复。沉默缺陷型突变体的过表达导致端粒的活跃聚集,并特别提高了亚端粒之间的GC效率。因此,物理距离限制了亚端粒处的GC。然而,相互的染色体内和亚端粒序列之间的修复效率变化高达15倍,这取决于DSB的位置,表明空间接近度不是HR的唯一限制因素。缺失限制了亚端粒DSB处的切除并提高了GC效率。亚端粒DSB处抑制性染色质的存在也通过抵消介导的切除而有利于重组。因此,抑制性染色质通过限制DSB切除和防止遗传信息丢失来促进亚端粒DSB处的HR。

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