首页> 外文期刊>European journal of human genetics: EJHG >Underestimation of heritability using a mixed model with a polygenic covariance structure in a genome-wide association study for complex traits
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Underestimation of heritability using a mixed model with a polygenic covariance structure in a genome-wide association study for complex traits

机译:在复杂性状的全基因组关联研究中,使用具有多基因协方差结构的混合模型低估了遗传力

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Recently, the use of a mixed model methodology in genome-wide association studies (GWAS) has been considered effective for controlling population stratification and explaining the polygenic effects of complex traits. However, estimating polygenic variance components and heritability was biased when the mixed model was used. This bias results from a diluted genetic relationship covariance structure, particularly with a limited number of underlying causal variants. We simulated disease and quantitative phenotypes with a variety of heritabilities (0.1, 0.2, 0.3, 0.4, and 0.5), prevalence rates (0.1, 0.2, 0.3, and 0.5), and causal variant numbers (10, 30, 50, and 100). Heritabilities from the simulated data using restricted maximum likelihood were underestimated in many populations (P<0.05). The underestimation increased with a large heritability, a small prevalence, and a small number of causal variants. The underestimation was larger in analyzing disease traits compared with quantitative traits. This study suggests an underestimated heritability in GWAS upon using the mixed model methodology with an excessively larger number of variants versus causal variants.
机译:最近,在全基因组关联研究(GWAS)中使用混合模型方法已被认为可有效控制种群分层并解释复杂性状的多基因效应。然而,当使用混合模型时,估计多基因变异成分和遗传力是有偏差的。这种偏见是由稀释的遗传关系协方差结构引起的,尤其是在潜在的因果变量数量有限的情况下。我们模拟了具有多种遗传力(0.1、0.2、0.3、0.4和0.5),患病率(0.1、0.2、0.3和0.5)和因果变异数(10、30、50和100)的疾病和定量表型)。在许多人群中,使用受限最大似然法从模拟数据得出的遗传力被低估了(P <0.05)。由于遗传力大,患病率低和因果变体数量少,低估增加了。与定量特征相比,在分析疾病特征时被低估的幅度更大。这项研究表明,在使用混合模型方法的情况下,GWAS的遗传力被低估了,其中变异数比因果变异数大得多。

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