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Bisulfighter: accurate detection of methylated cytosines and differentially methylated regions

机译:Bisulfighter:准确检测甲基化胞嘧啶和差异甲基化区域

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摘要

Analysis of bisulfite sequencing data usually requires two tasks: to call methylated cytosines (mCs) in a sample, and to detect differentially methylated regions (DMRs) between paired samples. Although numerous tools have been proposed for mC calling, methods for DMR detection have been largely limited. Here, we present Bisulfighter, a new software package for detecting mCs and DMRs from bisulfite sequencing data. Bisulfighter combines the LAST alignment tool for mC calling, and a novel framework for DMR detection based on hidden Markov models (HMMs). Unlike previous attempts that depend on empirical parameters, Bisulfighter can use the expectation-maximization algorithm for HMMs to adjust parameters for each data set. We conduct extensive experiments in which accuracy of mC calling and DMR detection is evaluated on simulated data with various mC contexts, read qualities, sequencing depths and DMR lengths, as well as on real data from a wide range of biological processes. We demonstrate that Bisulfighter consistently achieves better accuracy than other published tools, providing greater sensitivity for mCs with fewer false positives, more precise estimates of mC levels, more exact locations of DMRs and better agreement of DMRs with gene expression and DNase I hypersensitivity. The source code is available at http://epigenome.cbrc.jp/bisulfighter.
机译:亚硫酸氢盐测序数据的分析通常需要完成两项任务:调用样品中的甲基化胞嘧啶(mC),以及检测配对样品之间的差异甲基化区域(DMR)。尽管已提出了许多用于mC呼叫的工具,但DMR检测的方法受到很大限制。在这里,我们介绍Bisulfighter,这是一个用于从亚硫酸氢盐测序数据中检测mC和DMR的新软件包。 Bisulfighter结合了用于mC调用的LAST对齐工具和基于隐马尔可夫模型(HMM)的DMR检测新框架。与以前的依赖经验参数的尝试不同,Bisulfighter可以对HMM使用期望最大化算法来调整每个数据集的参数。我们进行了广泛的实验,其中对具有各种mC上下文,读取质量,测序深度和DMR长度的模拟数据,以及来自各种生物学过程的真实数据,评估了mC调用和DMR检测的准确性。我们证明Bisulfighter始终比其他已发布的工具具有更高的准确性,它为mC提供了更高的敏感性,而假阳性更少,mC水平的估算更加精确,DMR的位置更加精确,并且DMR与基因表达和DNase I超敏性更好的吻合。源代码可从http://epigenome.cbrc.jp/bisulfighter获得。

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