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The nucleosome acidic patch plays a critical role in RNF168-dependent ubiquitination of histone H2A

机译:核小体酸性补丁在RNF168依赖的组蛋白H2A泛素化中起关键作用

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During DNA damage response, the RING E3 ligase RNF168 ubiquitinates nucleosomal H2A at K13–15. Here we show that the ubiquitination reaction is regulated by its substrate. We define a region on the RING domain important for target recognition and identify the H2A / H2B dimer as the minimal substrate to confer lysine specificity to the RNF168 reaction. Importantly, we find an active role for the substrate in the reaction. H2A / H2B dimers and nucleosomes enhance the E3-mediated discharge of ubiquitin from the E2 and redirect the reaction towards the relevant target, in a process that depends on an intact acidic patch. This active contribution of a region distal from the target lysine provides regulation of the specific K13–15 ubiquitination reaction during the complex signalling process at DNA damage sites.
机译:在DNA损伤反应期间,RING E3连接酶RNF168在K13-15处泛素化核小体H2A。在这里,我们显示泛素化反应受其底物调节。我们在RING域上定义了一个对靶标识别很重要的区域,并将H2A / H2B二聚体确定为向RNF168反应赋予赖氨酸特异性的最小底物。重要的是,我们发现底物在反应中起积极作用。 H2A / H2B二聚体和核小体增强了E3介导的泛素从E2的释放,并将反应重定向至相关靶标,该过程取决于完整的酸性补丁。靶赖氨酸远端区域的这种主动作用可在DNA损伤部位复杂的信号传导过程中调节特定的K13-15泛素化反应。

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