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SET8 prevents excessive DNA methylation by methylation-mediated degradation of UHRF1 and DNMT1

机译:Set8通过甲基化介导的UHRF1和DNMT1防止过量的DNA甲基化。

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摘要

Faithful inheritance of DNA methylation across cell division requires DNMT1 and its accessory factor UHRF1. However, how this axis is regulated to ensure DNA methylation homeostasis remains poorly understood. Here we show that SET8, a cell-cycle-regulated protein methyltransferase, controls protein stability of both UHRF1 and DNMT1 through methylation-mediated, ubiquitin-dependent degradation and consequently prevents excessive DNA methylation. SET8 methylates UHRF1 at lysine 385 and this modification leads to ubiquitination and degradation of UHRF1. In contrast, LSD1 stabilizes both UHRF1 and DNMT1 by demethylation. Importantly, SET8 and LSD1 oppositely regulate global DNA methylation and do so most likely through regulating the level of UHRF1 than DNMT1. Finally, we show that UHRF1 downregulation in G2/M by SET8 has a role in suppressing DNMT1-mediated methylation on post-replicated DNA. Altogether, our study reveals a novel role of SET8 in promoting DNA methylation homeostasis and identifies UHRF1 as the hub for tuning DNA methylation through dynamic protein methylation.
机译:忠实遗传细胞分裂的DNA甲基化需要DNMT1及其附属因子UHRF1。然而,这种轴是如何调节的,以确保DNA甲基化稳定仍然明白。在这里,我们显示Set8,一种细胞周期调节的蛋白质甲基转移酶,通过甲基化介导的ubiquitin依赖性降解来控制UHRF1和DNMT1的蛋白质稳定性,并因此防止过量的DNA甲基化。在赖氨酸385时SET8甲基酯UHRF1,该修饰导致UHRF1的泛素化和降解。相反,LSD1通过去甲基化稳定UHRF1和DNMT1。重要的是,SET8和LSD1对立地调节全球DNA甲基化,并且最有可能通过调节UHRF1的水平而不是DNMT1。最后,我们表明UHRF1通过Set8的G2 / M下调在抑制后复制DNA上抑制DNMT1介导的甲基化的作用。完全,我们的研究揭示Set8在促进DNA甲基化稳态方面的新作用,并通过动态蛋白质甲基化识别UHRF1作为调整DNA甲基化的轮毂。

著录项

  • 来源
    《Nucleic Acids Research》 |2019年第17期|共16页
  • 作者单位

    East China Normal Univ Shanghai Key Lab Regulatory Biol Fengxian Dist Cent Hosp ECNU Joint Ctr Translat Med Inst Biomed Sci Shanghai 200241 Peoples R China;

    Soochow Univ Hosp 1 Inst Fetol Suzhou Peoples R China;

    East China Normal Univ Shanghai Key Lab Regulatory Biol Fengxian Dist Cent Hosp ECNU Joint Ctr Translat Med Inst Biomed Sci Shanghai 200241 Peoples R China;

    East China Normal Univ Shanghai Key Lab Regulatory Biol Fengxian Dist Cent Hosp ECNU Joint Ctr Translat Med Inst Biomed Sci Shanghai 200241 Peoples R China;

    Chinese Acad Sci Res Ctr Ecoenvironm Sci State Key Lab Environm Chem &

    Ecotoxicol Beijing 100085 Peoples R China;

    East China Normal Univ Shanghai Key Lab Regulatory Biol Fengxian Dist Cent Hosp ECNU Joint Ctr Translat Med Inst Biomed Sci Shanghai 200241 Peoples R China;

    East China Normal Univ Shanghai Key Lab Regulatory Biol Fengxian Dist Cent Hosp ECNU Joint Ctr Translat Med Inst Biomed Sci Shanghai 200241 Peoples R China;

    East China Normal Univ Shanghai Key Lab Regulatory Biol Fengxian Dist Cent Hosp ECNU Joint Ctr Translat Med Inst Biomed Sci Shanghai 200241 Peoples R China;

    East China Normal Univ Shanghai Key Lab Regulatory Biol Fengxian Dist Cent Hosp ECNU Joint Ctr Translat Med Inst Biomed Sci Shanghai 200241 Peoples R China;

    Chinese Acad Sci Res Ctr Ecoenvironm Sci State Key Lab Environm Chem &

    Ecotoxicol Beijing 100085 Peoples R China;

    East China Normal Univ Shanghai Key Lab Regulatory Biol Fengxian Dist Cent Hosp ECNU Joint Ctr Translat Med Inst Biomed Sci Shanghai 200241 Peoples R China;

    Natl Ctr Prot Sci Beijing Beijing Proteome Res Ctr Inst Lifeom State Key Lab Prote Beijing 102206 Peoples R China;

    East China Normal Univ Shanghai Key Lab Regulatory Biol Fengxian Dist Cent Hosp ECNU Joint Ctr Translat Med Inst Biomed Sci Shanghai 200241 Peoples R China;

    East China Normal Univ Shanghai Key Lab Regulatory Biol Fengxian Dist Cent Hosp ECNU Joint Ctr Translat Med Inst Biomed Sci Shanghai 200241 Peoples R China;

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  • 正文语种 eng
  • 中图分类 生物化学;
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