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A generalized least-squares framework for rare-variant analysis in family data

机译:用于家庭数据中稀有变异分析的广义最小二乘框架

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摘要

Rare variants may, in part, explain some of the hereditability missing in current genome-wide association studies. Many gene-based rare-variant analysis approaches proposed in recent years are aimed at population-based samples, although analysis strategies for family-based samples are clearly warranted since the family-based design has the potential to enhance our ability to enrich for rare causal variants. We have recently developed the generalized least squares, sequence kernel association test, or GLS-SKAT, approach for the rare-variant analyses in family samples, in which the kinship matrix that was computed from the high dimension genetic data was used to decorrelate the family structure. We then applied the SKAT-O approach for gene-/region-based inference in the decorrelated data. In this study, we applied this GLS-SKAT method to the systolic blood pressure data in the simulated family sample distributed by the Genetic Analysis Workshop 18. We compared the GLS-SKAT approach to the rare-variant analysis approach implemented in family-based association test-v1 and demonstrated that the GLS-SKAT approach provides superior power and good control of type I error rate.
机译:罕见的变异可能部分解释了当前全基因组关联研究中缺少的可遗传性。近年来,许多基于基因的稀有变异分析方法都针对人群样本,尽管基于家庭的样本分析策略显然有必要,因为基于家庭的设计有可能增强我们丰富稀有因果能力的潜力变体。我们最近开发了用于家庭样本中稀有变异分析的广义最小二乘序列核关联检验或GLS-SKAT方法,其中从高维遗传数据中计算出的亲属关系矩阵用于对家庭进行去相关结构体。然后,我们在去相关数据中将SKAT-O方法应用于基于基因/区域的推断。在这项研究中,我们将这种GLS-SKAT方法应用于由遗传分析研讨会18分发的模拟家庭样本中的收缩压数据。我们将GLS-SKAT方法与基于家庭的关联中实施的稀有变异分析方法进行了比较测试v1,并证明了GLS-SKAT方法可提供出众的功能并能很好地控制I型错误率。

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