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The Guardian of the Genome Revisited: p53 Downregulates Genes Required for Telomere Maintenance DNA Repair and Centromere Structure

机译:再谈基因组的守护者:p53下调维持端粒DNA修复和着丝粒结构所需的基因。

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摘要

The p53 protein has been extensively studied for its capacity to prevent proliferation of cells with a damaged genome. Surprisingly, however, our recent analysis of mice expressing a hyperactive mutant p53 that lacks the C-terminal domain revealed that increased p53 activity may alter genome maintenance. We showed that p53 downregulates genes essential for telomere metabolism, DNA repair, and centromere structure and that a sustained p53 activity leads to phenotypic traits associated with dyskeratosis congenita and Fanconi anemia. This downregulation is largely conserved in human cells, which suggests that our findings could be relevant to better understand processes involved in bone marrow failure as well as aging and tumor suppression.
机译:已经对p53蛋白防止具有受损基因组的细胞增殖的能力进行了广泛的研究。然而,令人惊讶的是,我们最近对表达缺乏C末端结构域的高活性突变型p53的小鼠的分析显示,增加的p53活性可能会改变基因组的维持。我们发现p53下调了端粒代谢,DNA修复和着丝粒结构必不可少的基因,持续的p53活性导致与先天性角化不全和范科尼贫血有关的表型特征。这种下调在人类细胞中基本上是保守的,这表明我们的发现可能与更好地了解涉及骨髓衰竭以及衰老和肿瘤抑制的过程有关。

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