首页> 外文期刊>PLoS Biology >The RSF1 Histone-Remodelling Factor Facilitates DNA Double-Strand Break Repair by Recruiting Centromeric and Fanconi Anaemia Proteins
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The RSF1 Histone-Remodelling Factor Facilitates DNA Double-Strand Break Repair by Recruiting Centromeric and Fanconi Anaemia Proteins

机译:RSF1组蛋白重塑因子通过募集着丝粒和Fanconi贫血蛋白促进DNA双链断裂修复

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摘要

ATM is a central regulator of the cellular responses to DNA double-strand breaks (DSBs). Here we identify a biochemical interaction between ATM and RSF1 and we characterise the role of RSF1 in this response. The ATM–RSF1 interaction is dependent upon both DSBs and ATM kinase activity. Together with SNF2H/SMARCA5, RSF1 forms the RSF chromatin-remodelling complex. Although RSF1 is specific to the RSF complex, SNF2H/SMARCA5 is a catalytic subunit of several other chromatin-remodelling complexes. Although not required for checkpoint signalling, RSF1 is required for efficient repair of DSBs via both end-joining and homology-directed repair. Specifically, the ATM-dependent recruitment to sites of DSBs of the histone fold proteins CENPS/MHF1 and CENPX/MHF2, previously identified at centromeres, is RSF1-dependent. In turn these proteins recruit and regulate the mono-ubiquitination of the Fanconi Anaemia proteins FANCD2 and FANCI. We propose that by depositing CENPS/MHF1 and CENPX/MHF2, the RSF complex either directly or indirectly contributes to the reorganisation of chromatin around DSBs that is required for efficient DNA repair.
机译:ATM是细胞对DNA双链断裂(DSB)响应的中央调节器。在这里,我们确定了ATM和RSF1之间的生化相互作用,并描述了RSF1在此响应中的作用。 ATM-RSF1相互作用取决于DSB和ATM激酶活性。 RSF1与SNF2H / SMARCA5一起形成RSF染色质重塑复合体。尽管RSF1特定于RSF复合物,但SNF2H / SMARCA5是其他几种染色质重塑复合物的催化亚基。尽管对于检查点信令不是必需的,但RSF1对于通过末端连接和同源性定向修复进行DSB的有效修复是必需的。具体而言,先前在着丝粒处鉴定的组蛋白折叠蛋白CENPS / MHF1和CENPX / MHF2的DSB位置的ATM依赖性募集是RSF1依赖性的。反过来,这些蛋白质募集并调节Fanconi贫血蛋白质FANCD2和FANCI的单泛素化。我们建议通过沉积CENPS / MHF1和CENPX / MHF2,RSF复合物直接或间接有助于有效DNA修复所需的DSB周围的染色质重组。

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