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Many Phenotypes Without Many False Discoveries: Error Controlling Strategies for Multitrait Association Studies

机译:没有许多错误发现的许多表型:多特征关联研究的错误控制策略

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The genetic basis of multiple phenotypes such as gene expression, metabolite levels, or imaging features is often investigated by testing a large collection of hypotheses, probing the existence of association between each of the traits and hundreds of thousands of genotyped variants. Appropriate multiplicity adjustment is crucial to guarantee replicability of findings, and the false discovery rate (FDR) is frequently adopted as a measure of global error. In the interest of interpretability, results are often summarized so that reporting focuses on variants discovered to be associated to some phenotypes. We show that applying FDR-controlling procedures on the entire collection of hypotheses fails to control the rate of false discovery of associated variants as well as the expected value of the average proportion of false discovery of phenotypes influenced by such variants. We propose a simple hierarchical testing procedure that allows control of both these error rates and provides a more reliable basis for the identification of variants with functional effects. We demonstrate the utility of this approach through simulation studies comparing various error rates and measures of power for genetic association studies of multiple traits. Finally, we apply the proposed method to identify genetic variants that impact flowering phenotypes in Arabidopsis thaliana, expanding the set of discoveries. Published 2015 Wiley Periodicals, Inc.
机译:经常通过测试大量的假设,探究每个特征与成千上万个基因型变异之间的关联性,来研究多种表型的遗传基础,例如基因表达,代谢物水平或成像特征。适当的多重性调整对于保证发现的可复制性至关重要,并且错误发现率(FDR)经常被用作衡量整体误差的一种方法。出于可解释性的考虑,通常会对结果进行汇总,以使报告的重点是发现与某些表型相关的变异。我们表明,在假设的整个集合上应用FDR控制程序无法控制相关变体的错误发现率以及受此类变量影响的表型错误发现的平均比例的预期值。我们提出了一种简单的分层测试程序,该程序可以控制这两个错误率,并为识别具有功能效果的变量提供了更可靠的基础。我们通过比较各种错误率和多种性状遗传关联研究的功效度量的模拟研究证明了这种方法的实用性。最后,我们应用提出的方法来鉴定影响拟南芥开花表型的遗传变异,从而扩大了发现范围。 2015年出版的Wiley Periodicals,Inc.

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