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A method for analyzing multiple continuous phenotypes in rare variant association studies allowing for flexible correlations in variant effects

机译:一种在稀有变异关联研究中分析多个连续表型的方法,可以在变异效应中实现灵活的关联

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摘要

For region-based sequencing data, power to detect genetic associations can be improved through analysis of multiple related phenotypes. With this motivation, we propose a novel test to detect association simultaneously between a set of rare variants, such as those obtained by sequencing in a small genomic region, and multiple continuous phenotypes. We allow arbitrary correlations among the phenotypes and build on a linear mixed model by assuming the effects of the variants follow a multivariate normal distribution with a zero mean and a specific covariance matrix structure. In order to account for the unknown correlation parameter in the covariance matrix of the variant effects, a data-adaptive variance component test based on scoretype statistics is derived. As our approach can calculate the P-value analytically, the proposed test procedure is computationally efficient. Broad simulations and an application to the UK10K project show that our proposed multivariate test is generally more powerful than univariate tests, especially when there are pleiotropic effects or highly correlated phenotypes.
机译:对于基于区域的测序数据,可以通过分析多个相关表型来提高检测遗传关联的能力。以此动机为基础,我们提出了一种新颖的测试方法,可以同时检测一组稀有变体(例如通过在小基因组区域中测序获得的稀有变体)与多个连续表型之间的关联。我们允许表型之间的任意相关性,并通过假设变量的影响遵循具有零均值和特定协方差矩阵结构的多元正态分布来建立线性混合模型。为了考虑变量效应的协方差矩阵中的未知相关参数,导出了基于得分类型统计数据的数据自适应方差分量检验。由于我们的方法可以解析地计算P值,因此所提出的测试程序在计算上是有效的。广泛的仿真和对UK10K项目的应用表明,我们提出的多变量检验通常比单变量检验更强大,尤其是在存在多效效应或高度相关的表型时。

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