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RNF8-dependent histone ubiquitination during DNA damage response and spermatogenesis

机译:DNA损伤反应和生精过程中依赖RNF8的组蛋白泛素化

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摘要

Histone ubiquitination regulates the chromatin structure that is important for many biological processes. Recently, ubiquitination of histones was observed during the DNA damage response (DDR), and this modification is controlled by really interesting new gene (RING) domain E3 ligase, RNF8. Together with the E2 conjugating enzyme UBC13, RNF8 catalyzes ubiquitination of the histones H2A and H2AX during the DDR, thus facilitating downstream recruitment of DDR factors, such as p53 binding protein 1 (53BP1) and breast cancer type 1 susceptibility protein (BRCA1), to the damage site. Accordingly, the RNF8 knockout mice display phenotypes associated with failed DDR, including hypersensitivity to ionizing radiation, V(D)J recombination deficiency, and a predisposition to cancer. In addition to the DDR phenotypes, RNF8 knockout mice fail to generate mature sperm during spermatogenesis, resulting in male sterility. The RNF8 knockout mice also have a drastic reduction in histone ubiquitination in the testes. These findings indicate that the role of histone ubiquitination during chromatin remodeling in two different biological events could be linked by an RNF8-dependent mechanism. Here, we review the molecular mechanism of RNF8-dependent histone ubiquitination both in DDR and spermatogenesis.
机译:组蛋白泛素化调节染色质结构,这对许多生物学过程都很重要。最近,在DNA损伤反应(DDR)期间观察到了组蛋白的泛素化,而这种修饰是由真正有趣的新基因(RING)域E3连接酶RNF8控制的。 RNF8与E2偶联酶UBC13一起催化DDR期间组蛋白H2A和H2AX的泛素化,从而促进了DDR因子的下游募集,例如p53结合蛋白1(53BP1)和1型乳腺癌易感性蛋白(BRCA1)。损坏部位。因此,RNF8基因敲除小鼠表现出与DDR失败相关的表型,包括对电离辐射的超敏性,V(D)J重组缺乏和对癌症的易感性。除DDR表型外,RNF8基因敲除小鼠在生精过程中无法生成成熟的精子,导致雄性不育。 RNF8基因敲除小鼠的睾丸中组蛋白泛素化程度也大大降低。这些发现表明,组蛋白泛素化在两个不同生物学事件中的染色质重塑过程中的作用可能与RNF8依赖性机制有关。在这里,我们回顾了DDR和精子发生中RNF8依赖的组蛋白泛素化的分子机制。

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  • 来源
    《Acta Biochimica et Biophysica Sinica》 |2011年第5期|p.339-345|共7页
  • 作者

    Xiaochun Yu;

  • 作者单位

    , University of Michigan Medical School, @%@;

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