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The deterministic role of 5-mers in microRNA-gene targeting

机译:microRNA-基因靶向5mer的确定性作用

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MiRNAs play a central role in physiological and pathological processes. Both for the biological understanding and for their clinical application, it is essential to understand the interaction of miRNAs and their targets. Target identification largely hinges on in-silico prediction, which requires a complete consideration of miRNA binding sites within the UTRs of target genes. Here, we show that 5-mer sites might also play an essential role for human miRNA-target binding. We implemented and employed an algorithm to all pairs of 2,588 human miRNAs annotated in miRBase and the 3 UTRs of 16725 genes (43 million combinations). Our in-silico analysis showed a highly significant enrichment (p = 1.4 x 10(-69)) of 5-mer binding sites in 3 UTRs across all experimentally validated miRNA-target gene pairs. We next confirmed the central role of 5-mer binding sites by reporter assays and demonstrated that two non-canonical 5-mer sites of miR-34a in the 3 UTR of T-cell receptor alpha (TCRA) have a significantly stronger influence on its posttranscriptional regulation than the canonical binding sites. These observations indicate an essential role of 5-mer binding sites for the miRNA targeting in human cells.
机译:MiRNA在生理和病理过程中发挥着核心作用。对于生物学理解和临床应用,必须了解miRNA及其目标的相互作用。目标识别在很大程度上涉及硅预测,这需要完全考虑靶基因的UTR内的miRNA结合位点。在这里,我们表明5-MEL网站也可能为人体miRNA-target结合发挥重要作用。我们实施并使用了在MIRBASE注释的所有2,588个人miRNA的算法和16725个基因的3个UTR(& 4300万组合)。我们的硅基分析显示出在所有实验验证的miRNA-靶基因对的3个UTR中的5-MER结合位点的高度显着的富集(P = 1.4×10(-69))。接下来,我们通过记者测定证实了5-MER结合位点的中心作用,并证明了T细胞受体α(TCRA)3 UTR中的miR-34a的两个非规范化5-mer位点对其产生显着强烈的影响后术式调节比规范结合位点。这些观察结果表明5-MER结合位点的MiRNA靶向人细胞的必要作用。

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