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Retroviral promoters in the human genome.

机译:人类基因组中的逆转录病毒启动子。

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Endogenous retrovirus (ERV) elements have been shown to contribute promoter sequences that can initiate transcription of adjacent human genes. However, the extent to which retroviral sequences initiate transcription within the human genome is currently unknown. We analyzed genome sequence and high-throughput expression data to systematically evaluate the presence of retroviral promoters in the human genome. RESULTS: We report the existence of 51,197 ERV-derived promoter sequences that initiate transcription within the human genome, including 1743 cases where transcription is initiated from ERV sequences that are located in gene proximal promoter or 5' untranslated regions (UTRs). A total of 114 of the ERV-derived transcription start sites can be demonstrated to drive transcription of 97 human genes, producing chimeric transcripts that are initiated within ERV long terminal repeat (LTR) sequences and read-through into known gene sequences. ERV promoters drive tissue-specific and lineage-specific patterns of gene expression and contribute to expression divergence between paralogs. These data illustrate the potential of retroviral sequences to regulate human transcription on a large scale consistent with a substantial effect of ERVs on the function and evolution of the human genome.
机译:内源性逆转录病毒(ERV)元素已被证明有助于启动子序列,可以启动相邻人类基因的转录。然而,逆转录病毒序列在人类基因组内起始转录的程度目前尚不清楚。我们分析了基因组序列和高通量表达数据,以系统地评估人类基因组中逆转录病毒启动子的存在。结果:我们报告了存在人类基因组中起始转录的51,197个ERV衍生启动子序列,包括1743例从位于基因近端启动子或5'非翻译区(UTR)的ERV序列起始转录的案例。可以证明总共有114个ERV衍生的转录起始位点可以驱动97个人类基因的转录,产生嵌合的转录本,这些嵌合的转录本可以在ERV长末端重复序列(LTR)序列内启动,并通读到已知的基因序列中。 ERV启动子驱动基因表达的组织特异性和谱系特异性模式,并促进旁系同源物之间的表达差异。这些数据说明了逆转录病毒序列在大规模调控人类转录方面的潜力,这与ERV对人类基因组功能和进化的实质影响相一致。

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