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Transposable element derived DNaseI-hypersensitive sites in the human genome

机译:人类基因组中转座因子衍生的DNaseI超敏感位点

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摘要

BackgroundTransposable elements (TEs) are abundant genomic sequences that have been found to contribute to genome evolution in unexpected ways. Here, we characterize the evolutionary and functional characteristics of TE-derived human genome regulatory sequences uncovered by the high throughput mapping of DNaseI-hypersensitive (HS) sites.ResultsHuman genome TEs were found to contribute substantially to HS regulatory sequences characterized in CD4+ T cells: 23% of HS sites contain TE-derived sequences. While HS sites are far more evolutionarily conserved than non HS sites in the human genome, consistent with their functional importance, TE-derived HS sites are highly divergent. Nevertheless, TE-derived HS sites were shown to be functionally relevant in terms of driving gene expression in CD4+ T cells. Genes involved in immune response are statistically over-represented among genes with TE-derived HS sites. A number of genes with both TE-derived HS sites and immune tissue related expression patterns were found to encode proteins involved in immune response such as T cell specific receptor antigens and secreted cytokines as well as proteins with clinical relevance to HIV and cancer. Genes with TE-derived HS sites have higher average levels of sequence and expression divergence between human and mouse orthologs compared to genes with non TE-derived HS sites.
机译:背景转座因子(TE)是丰富的基因组序列,已发现它们以意想不到的方式有助于基因组进化。在这里,我们表征了DNaseI超敏(HS)位点的高通量图谱所揭示的TE衍生的人类基因组调控序列的进化和功能特征。结果发现人类基因组TEs基本上对CD4 + T细胞中表征的HS调控序列有贡献: HS位点的23%包含TE衍生的序列。尽管人类基因组中的HS位点比非HS位点在进化上保守得多,但与其功能重要性相符,但TE衍生的HS位点却高度不同。然而,从驱动CD4 + T细胞中的基因表达来看,TE衍生的HS位点在功能上是相关的。在具有TE衍生的HS位点的基因中,参与免疫应答的基因在统计学上被过度代表。发现许多具有TE衍生的HS位点和免疫组织相关表达模式的基因编码参与免疫应答的蛋白质,例如T细胞特异性受体抗原和分泌的细胞因子,以及与HIV和癌症具有临床相关性的蛋白质。与具有非TE衍生HS位点的基因相比,具有TE衍生HS位点的基因在人和小鼠直系同源物之间具有更高的平均序列水平和表达差异。

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