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Gene-set Analysis with CGI Information for Differential DNA Methylation Profiling

机译:使用CGI信息进行基因组分析以进行DNA甲基化差异分析

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摘要

DNA methylation is a well-established epigenetic biomarker for many diseases. Studying the relationships among a group of genes and their methylations may help to unravel the etiology of diseases. Since CpG-islands (CGIs) play a crucial role in the regulation of transcription during methylation, including them in the analysis may provide further information in understanding the pathogenesis of cancers. Such CGI information, however, has usually been overlooked in existing gene-set analyses. Here we aimed to include both pathway information and CGI status to rank competing gene-sets and identify among them the genes most likely contributing to DNA methylation changes. To accomplish this, we devised a Bayesian model for matched case-control studies with parameters for CGI status and pathway associations, while incorporating intra-gene-set information. Three cancer studies with candidate pathways were analyzed to illustrate this approach. The strength of association for each candidate pathway and the influence of each gene were evaluated. Results show that, based on probabilities, the importance of pathways and genes can be determined. The findings confirm that some of these genes are cancer-related and may hold the potential to be targeted in drug development.
机译:DNA甲基化是许多疾病中公认的表观遗传标记。研究一组基因及其甲基化之间的关系可能有助于弄清疾病的病因。由于CpG岛(CGI)在甲基化过程中的转录调控中起着至关重要的作用,因此在分析中将它们包括在内可能会为了解癌症的发病机理提供进一步的信息。但是,此类CGI信息通常在现有的基因组分析中被忽略。在这里,我们旨在包括途径信息和CGI状态,以对竞争的基因集进行排名,并在其中确定最有可能导致DNA甲基化变化的基因。为了实现这一目标,我们设计了一个贝叶斯模型,用于匹配的病例对照研究,其中包含CGI状态和途径关联的参数,同时整合了基因组内信息。分析了三个具有候选途径的癌症研究,以说明这种方法。评估每种候选途径的缔合强度和每种基因的影响。结果表明,基于概率,可以确定途径和基因的重要性。这些发现证实这些基因中的一些与癌症有关,并且可能具有靶向药物开发的潜力。

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