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The RNF168 paralog RNF169 defines a new class of ubiquitylated histone reader involved in the response to DNA damage

机译:RNF168旁系同源物RNF169定义了一类新的泛素化组蛋白阅读器参与了对DNA损伤的反应

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摘要

Site-specific histone ubiquitylation plays a central role in orchestrating the response to DNA double-strand breaks (DSBs). DSBs elicit a cascade of events controlled by the ubiquitin ligase RNF168, which promotes the accumulation of repair factors such as 53BP1 and BRCA1 on the chromatin flanking the break site. RNF168 also promotes its own accumulation, and that of its paralog RNF169, but how they recognize ubiquitylated chromatin is unknown. Using methyl-TROSY solution NMR spectroscopy and molecular dynamics simulations, we present an atomic resolution model of human RNF169 binding to a ubiquitylated nucleosome, and validate it by electron cryomicroscopy. We establish that RNF169 binds to ubiquitylated H2A-Lys13/Lys15 in a manner that involves its canonical ubiquitin-binding helix and a pair of arginine-rich motifs that interact with the nucleosome acidic patch. This three-pronged interaction mechanism is distinct from that by which 53BP1 binds to ubiquitylated H2A-Lys15 highlighting the diversity in site-specific recognition of ubiquitylated nucleosomes.>DOI:
机译:特定于位点的组蛋白泛素化在协调对DNA双链断裂(DSB)的反应中起着核心作用。 DSB引发由泛素连接酶RNF168控制的一系列事件,泛素连接酶RNF168促进了修复因子(如53BP1和BRCA1)在断裂位点两侧的染色质上的积累。 RNF168还促进其自身和其类似物RNF169的积累,但是如何识别泛素化染色质尚不清楚。使用甲基TROSY溶液核磁共振波谱学和分子动力学模拟,我们提出了人类RNF169与泛素化核小体结合的原子分辨率模型,并通过电子低温显微镜对其进行了验证。我们建立RNF169绑定到泛素化的H2A-Lys13 / Lys15涉及其规范的泛素结合螺旋和一对与核小体酸性补丁相互作用的富含精氨酸的基序的方式。这种三管齐下的相互作用机制不同于53BP1与泛素化H2A-Lys15结合的机制,突出了泛素化核小体在位点特异性识别上的多样性。> DOI:

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