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Prediction of mRNA polyadenylation sites by support vector machine

机译:支持向量机预测mRNA聚腺苷酸化位点

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mRNA polyadenylation is responsible for the 3' end formation of most mRNAs in eukaryotic cells and is linked to termination of transcription. Prediction of mRNA polyadenylation sites [poly(A) sites] can help identify genes, define gene boundaries, and elucidate regulatory mechanisms. Current methods for poly(A) site prediction achieve moderate sensitivity and specificity. Here, we present a method using support vector machine for poly(A) site prediction. Using 15 cis-regulatory elements that are over-represented in various regions surrounding poly(A) sites, this method achieves higher sensitivity and similar specificity when compared with polyadq, a common tool for poly(A) site prediction. In addition, we found that while the polyadenylation signal AAUAAA and U-rich elements are primary determinants for poly(A) site prediction, other elements contribute to both sensitivity and specificity of the prediction, indicating a combinatorial mechanism involving multiple elements when choosing poly(A) sites in human cells.
机译:mRNA聚腺苷酸负责真核细胞中大多数mRNA的3'末端形成,并与转录终止有关。 mRNA多聚腺苷酸化位点[poly(A)位点]的预测可以帮助鉴定基因,定义基因边界并阐明调节机制。当前的poly(A)站点预测方法可实现中等灵敏度和特异性。在这里,我们提出一种使用支持​​向量机的poly(A)网站预测方法。与在poly(A)位点预测的常用工具polyadq相比,使用15个在多聚(A)位点周围各个区域中过量表达的顺式调控元件,该方法可获得更高的灵敏度和相似的特异性。此外,我们发现虽然聚腺苷酸化信号AAUAAA和富含U的元素是poly(A)位点预测的主要决定因素,但其他元素对预测的敏感性和特异性都有贡献,这表明在选择poly(A)时涉及多个元素的组合机制A)人细胞中的位点。

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