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人类逆转录转座子中的p53反应元件

p53 responsive elements in human retrotransposons.

作者信息

Harris C R, Dewan A, Zupnick A, Normart R, Gabriel A, Prives C, Levine A J, Hoh J

机构信息

Raymond and Beverly Sackler Foundation, New Brunswick, NJ 08540, USA.

出版信息

Oncogene. 2009 Nov 5;28(44):3857-65. doi: 10.1038/onc.2009.246. Epub 2009 Aug 31.

Abstract

Long interspersed nuclear elements-1 (L1s) are highly repetitive DNA elements that are capable of altering the human genome through retrotransposition. To protect against L1 retroposition, the cell downregulates the expression of L1 proteins by various mechanisms, including high-density cytosine methylation of L1 promoters and DICER-dependent destruction of L1 mRNAs. In this report, a large number of p53 responsive elements, or p53 DNA binding sites, were detected in L1 elements within the human genome. At least some of these p53 responsive elements are functional and can act to increase the levels of L1 mRNA expression. The p53 protein can directly bind to a short 15-nucleotide sequence within the L1 promoter. This p53 responsive element within L1 is a recent addition to evolution, appearing approximately 20 million years ago. This suggests an interplay between L1 elements, which have a rich history of causing changes in the genome, and the p53 protein, the function of which is to protect against genomic changes. To understand these observations, a model is proposed in which the increased expression of L1 mRNAs by p53 actually increases, rather than decreases, the genomic stability through amplification of p53-dependent processes for genomic protection.

摘要

长散在核元件1(L1s)是高度重复的DNA元件,能够通过逆转座改变人类基因组。为了防止L1逆转座,细胞通过多种机制下调L1蛋白的表达,包括L1启动子的高密度胞嘧啶甲基化和DICER依赖性的L1 mRNA降解。在本报告中,在人类基因组的L1元件中检测到大量p53反应元件或p53 DNA结合位点。这些p53反应元件中至少有一些是有功能的,并且可以起到增加L1 mRNA表达水平的作用。p53蛋白可以直接结合到L1启动子内一段短的15个核苷酸的序列上。L1内的这个p53反应元件是进化过程中最近才出现的,大约在2000万年前出现。这表明在具有丰富基因组改变历史的L1元件和具有防止基因组改变功能的p53蛋白之间存在相互作用。为了解释这些观察结果,提出了一个模型,其中p53导致的L1 mRNA表达增加实际上通过增强p53依赖性的基因组保护过程而增加而非降低基因组稳定性。

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