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MRG15 binds directly to PALB2 and stimulates homology-directed repair of chromosomal breaks

机译:MRG15直接与PALB2结合并刺激同源性指导的染色体断裂修复

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摘要

PALB2 physically and functionally connects the proteins encoded by the BRCA1 and BRCA2 breast and ovarian cancer genes into a DNA-damage-response network. However, it remains unclear how these proteins associate with chromatin that contains damaged DNA. We show here that PALB2 binds directly to a conserved chromodomain protein, MRG15, which is a component of histone acetyltransferase-deacetylase complexes. This interaction was identified by analysis of purified MRG15- and PALB2-containing protein complexes. Furthermore, MRG15 interacts with the entire BRCA complex, which contains BRCA1, PALB2, BRCA2 and RAD51. Interestingly, MRG15-deficient cells, similarly to cells deficient in PALB2 or BRCA2, showed reduced efficiency for homology-directed DNA repair and hypersensitivity to DNA interstrand crosslinking agents. Additionally, knockdown of MRG15 diminished the recruitment of PALB2, BRCA2 and RAD51 to sites of DNA damage and reduced chromatin loading of PALB2 and BRCA2. These results suggest that MRG15 mediates DNA-damage-response functions of the BRCA complex in chromatin.
机译:PALB2在物理上和功能上将由BRCA1和BRCA2乳腺癌和卵巢癌基因编码的蛋白质连接到DNA损伤反应网络中。但是,尚不清楚这些蛋白质如何与含有受损DNA的染色质结合。我们在这里显示,PALB2直接与保守的染色体结构域蛋白MRG15结合,MRG15是组蛋白乙酰转移酶-去乙酰化酶复合物的组成部分。通过分析纯化的含MRG15和PALB2的蛋白质复合物可以确定这种相互作用。此外,MRG15与包含BRCA1,PALB2,BRCA2和RAD51的整个BRCA复合体进行交互。有趣的是,与缺乏PALB2或BRCA2的细胞相似,缺乏MRG15的细胞显示出降低的同源性指导DNA修复效率和对DNA链间交联剂的超敏性。另外,敲低MRG15可以减少PALB2,BRCA2和RAD51对DNA损伤部位的募集,并减少PALB2和BRCA2的染色质负载。这些结果表明,MRG15介导染色质中BRCA复合物的DNA损伤反应功能。

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