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Pathway-based approach using hierarchical components of rare variants to analyze multiple phenotypes

机译:基于途径的方法,使用罕见变体的分层组分分析多种表型

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Background: As one possible solution to the "missing heritability" problem, many methods have been proposed that apply pathway-based analyses, using rare variants that are detected by next generation sequencing technology. However, while a number of methods for pathway-based rare-variant analysis of multiple phenotypes have been proposed, no method considers a unified model that incorporate multiple pathways.Results: Simulation studies successfully demonstrated advantages of multivariate analysis, compared to univariate analysis, and comparison studies showed the proposed approach to outperform existing methods. Moreover, real data analysis of six type 2 diabetes-related traits, using large-scale whole exome sequencing data, identified significant pathways that were not found by univariate analysis. Furthermore, strong relationships between the identified pathways, and their associated metabolic disorder risk factors, were found via literature search, and one of the identified pathway, was successfully replicated by an analysis with an independent dataset.Conclusions: Herein, we present a powerful, pathway-based approach to investigate associations between multiple pathways and multiple phenotypes. By reflecting the natural hierarchy of biological behavior, and considering correlation between pathways andphenotypes, the proposed method is capable of analyzing multiple phenotypes and multiple pathways simultaneously.
机译:背景:作为“遗失遗传性”问题的一个可能的解决方案,已经提出了许多方法,以利用由下一代测序技术检测的罕见变体应用途径的分析。然而,在已经提出了许多基于途径的易于变异分析的途径稀有变体分析的虽然已经提出了多种表型的统一模型,但统一模型包含多种途径。结果:模拟研究成功地证明了多元分析的优势,与单变量分析相比,和比较研究表明,卓越的现有方法的方法。此外,使用大规模全外壳测序数据的六种糖尿病相关性状的实际数据分析鉴定了单变量分析未发现的显着途径。此外,通过文献搜索,通过文献搜索找到识别的途径和其相关的代谢紊乱风险因素之间的强烈关系,并通过与独立数据集的分析成功复制了一个识别的途径。结论:在此,我们呈现强大的,基于途径的途径研究多种途径与多种表型之间的关联。通过反映生物学行为的自然等级,并考虑途径和脑脊液之间的相关性,所提出的方法能够同时分析多种表型和多种途径。

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