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Statistical methods for detecting differentially methylated loci and regions

机译:检测差异甲基化基因座和区域的统计方法

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摘要

DNA methylation, the reversible addition of methyl groups at CpG dinucleotides, represents an important regulatory layer associated with gene expression. Changed methylation status has been noted across diverse pathological states, including cancer. The rapid development and uptake of microarrays and large scale DNA sequencing has prompted an explosion of data analytic methods for processing and discovering changes in DNA methylation across varied data types. In this mini-review, we present a compact and accessible discussion of many of the salient challenges, such as experimental design, statistical methods for differential methylation detection, critical considerations such as cell type composition and the potential confounding that can arise from batch effects. From a statistical perspective, our main interests include the use of empirical Bayes or hierarchical models, which have proved immensely powerful in genomics, and the procedures by which false discovery control is achieved.
机译:DNA甲基化是CpG二核苷酸上甲基的可逆添加,代表了与基因表达相关的重要调控层。在包括癌症在内的各种病理状态中都注意到甲基化状态的改变。微阵列的快速发展和吸收以及大规模DNA测序已促使用于处理和发现各种数据类型的DNA甲基化变化的数据分析方法激增。在此迷你审查中,我们提出了许多重要挑战的紧凑且易于访问的讨论,例如实验设计,差异甲基化检测的统计方法,诸如细胞类型组成等关键考虑因素以及批次效应可能引起的混淆。从统计的角度来看,我们的主要兴趣包括使用经验贝叶斯或层次模型(已证明在基因组学方面极为强大)以及实现错误发现控制的程序。

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