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Translation initiation site prediction on a genomic scale: beauty in simplicity

机译:基因组范围内的翻译起始位点预测:简单而美丽

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Motivation: The correct identification of translation initiation sites (TIS) remains a challenging problem for computational methods that automatically try to solve this problem. Furthermore, the lion's share of these computational techniques focuses on the identification of TIS in transcript data. However, in the gene prediction context the identification of TIS occurs on the genomic level, which makes things even harder because at the genome level many more pseudo-TIS occur, resulting in models that achieve a higher number of false positive predictions. Results: In this article, we evaluate the performance of several 'simple' TIS recognition methods at the genomic level, and compare them to state-of-the-art models for TIS prediction in transcript data. We conclude that the simple methods largely outperform the complex ones at the genomic scale, and we propose a new model for TIS recognition at the genome level that combines the strengths of these simple models. The new model obtains a false positive rate of 0.125 at a sensitivity of 0.80 on a well annotated human chromosome ( chromosome 21). Detailed analyses show that the model is useful, both on its own and in a simple gene prediction setting.
机译:动机:对于自动尝试解决此问题的计算方法,正确识别翻译起始位点(TIS)仍然是一个具有挑战性的问题。此外,这些计算技术中的大部分都集中在笔录数据中TIS的识别上。但是,在基因预测的背景下,TIS的鉴定发生在基因组水平,这使事情变得更加困难,因为在基因组水平上,出现了更多的伪TIS,从而导致模型获得了更多的假阳性预测。结果:在本文中,我们评估了几种“简单” TIS识别方法在基因组水平上的性能,并将其与用于笔录数据中TIS预测的最新模型进行了比较。我们得出结论,在基因组规模上,简单方法在很大程度上优于复杂方法,并且我们提出了一种在基因组水平上用于TIS识别的新模型,该模型结合了这些简单模型的优势。新模型在注释良好的人类染色体(21号染色体)上以0.80的灵敏度获得0.125的假阳性率。详细的分析表明,该模型无论在其自身上还是在简单的基因预测环境中都是有用的。

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