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哺乳动物 Rap1 通过与端粒和端粒外位点结合来控制端粒功能和基因表达。

Mammalian Rap1 controls telomere function and gene expression through binding to telomeric and extratelomeric sites.

机构信息

Telomeres and Telomerase Group, Molecular Oncology Program, Spanish National Cancer Research Centre (CNIO), Melchor Fernández Almagro 3, Madrid, E-28029, Spain.

出版信息

Nat Cell Biol. 2010 Aug;12(8):768-80. doi: 10.1038/ncb2081. Epub 2010 Jul 11.

Abstract

Rap1 is a component of the shelterin complex at mammalian telomeres, but its in vivo role in telomere biology has remained largely unknown to date. Here we show that Rap1 deficiency is dispensable for telomere capping but leads to increased telomere recombination and fragility. We generated cells and mice deleted for Rap1; mice with Rap1 deletion in stratified epithelia were viable but had shorter telomeres and developed skin hyperpigmentation in adulthood. By performing chromatin immunoprecipitation coupled with ultrahigh-throughput sequencing, we found that Rap1 binds to both telomeres and to extratelomeric sites through the (TTAGGG)(2) consensus motif. Extratelomeric Rap1-binding sites were enriched at subtelomeric regions, in agreement with preferential deregulation of subtelomeric genes in Rap1-deficient cells. More than 70% of extratelomeric Rap1-binding sites were in the vicinity of genes, and 31% of the genes deregulated in Rap1-null cells contained Rap1-binding sites, suggesting a role for Rap1 in transcriptional control. These findings place a telomere protein at the interface between telomere function and transcriptional regulation.

摘要

Rap1 是哺乳动物端粒庇护体复合物的一个组成部分,但它在端粒生物学中的体内作用迄今为止在很大程度上仍是未知的。在这里,我们表明 Rap1 缺失对于端粒加帽并非必需,但会导致端粒重组和脆弱性增加。我们生成了 Rap1 缺失的细胞和小鼠;在分层上皮细胞中删除 Rap1 的小鼠是存活的,但它们的端粒较短,成年后会出现皮肤色素沉着过度。通过进行染色质免疫沉淀结合超高通量测序,我们发现 Rap1 既结合于端粒,也通过(TTAGGG)(2)共有序列结合于端粒外位点。端粒外 Rap1 结合位点在端粒附近的亚端粒区域富集,这与 Rap1 缺陷细胞中端粒外基因的优先失调一致。超过 70%的端粒外 Rap1 结合位点位于基因附近,在 Rap1 缺失细胞中失调的基因中有 31%含有 Rap1 结合位点,这表明 Rap1 在转录控制中发挥作用。这些发现将一个端粒蛋白置于端粒功能和转录调控的界面上。

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