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Tudor-domain protein PHF20L1 reads lysine methylated retinoblastoma tumour suppressor protein

机译:铎域蛋白质pHF20L1读取赖氨酸甲基化视网膜母细胞瘤肿瘤抑制蛋白

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摘要

The retinoblastoma tumour suppressor protein (pRb) classically functions to regulate early cell cycle progression where it acts to enforce a number of checkpoints in response to cellular stress and DNA damage. Methylation at lysine (K) 810, which occurs within a critical CDK phosphorylation site and antagonises a CDK-dependent phosphorylation event at the neighbouring S807 residue, acts to hold pRb in the hypo-phosphorylated growth-suppressing state. This is mediated in part by the recruitment of the reader protein 53BP1 to di-methylated K810, which allows pRb activity to be effectively integrated with the DNA damage response. Here, we report the surprising observation that an additional methylation-dependent interaction occurs at K810, but rather than the di-methyl mark, it is selective for the mono-methyl K810 mark. Binding of the mono-methyl PHF20L1 reader to methylated pRb occurs on E2F target genes, where it acts to mediate an additional level of control by recruiting the MOF acetyltransferase complex to E2F target genes. Significantly, we find that the interplay between PHF20L1 and mono-methyl pRb is important for maintaining the integrity of a pRb-dependent G1-S-phase checkpoint. Our results highlight the distinct roles that methyl-lysine readers have in regulating the biological activity of pRb.
机译:视网膜母细胞瘤肿瘤抑制蛋白(pRb)通常起到调节早期细胞周期进程的作用,在细胞应激和DNA损伤的情况下,pRb会执行许多检查点。赖氨酸(K)810的甲基化发生在关键CDK磷酸化位点内,并拮抗相邻S807残基处的CDK依赖性磷酸化事件,其作用是将pRb保持在低磷酸化生长抑制状态。这在一定程度上是通过将阅读蛋白53BP1招募到二甲基化K810来介导的,这使得pRb活性能够有效地与DNA损伤反应整合。在这里,我们报告了一个令人惊讶的观察结果,即在K810处发生了额外的甲基化依赖性相互作用,但不是双甲基标记,而是对单甲基K810标记具有选择性。单甲基PHF20L1读取器与甲基化pRb的结合发生在E2F靶基因上,它通过将MOF乙酰转移酶复合物招募到E2F靶基因上来调节额外水平的控制。值得注意的是,我们发现PHF20L1和单甲基pRb之间的相互作用对于维持依赖pRb的G1-S期检查点的完整性非常重要。我们的结果强调了甲基赖氨酸读者在调节pRb生物活性中的独特作用。

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  • 来源
    《Cell death and differentiation》 |2017年第12期|共11页
  • 作者单位

    Univ Oxford Dept Oncol Old Rd Campus Res Bldg Old Rd Campus Roosevelt Dr Oxford OX3 7DQ England;

    Univ Oxford Dept Oncol Old Rd Campus Res Bldg Old Rd Campus Roosevelt Dr Oxford OX3 7DQ England;

    Univ Texas MD Anderson Canc Ctr Dept Mol Carcinogenesis Smithville TX 77030 USA;

    Univ Oxford Nuffield Dept Clin Med Struct Genom Consortium Old Rd Campus Res Bldg Old Rd Campus;

    Univ Texas MD Anderson Canc Ctr Dept Mol Carcinogenesis Smithville TX 77030 USA;

    Univ Oxford Dept Oncol Old Rd Campus Res Bldg Old Rd Campus Roosevelt Dr Oxford OX3 7DQ England;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 细胞生物学;
  • 关键词

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