首页> 外文期刊>The American Journal of Human Genetics >ROADTRIPS: case-control association testing with partially or completely unknown population and pedigree structure.
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ROADTRIPS: case-control association testing with partially or completely unknown population and pedigree structure.

机译:ROADTRIPS:病例对照对照测试,其中包括部分或完全未知的种群和血统结构。

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摘要

Genome-wide association studies are routinely conducted to identify genetic variants that influence complex disorders. It is well known that failure to properly account for population or pedigree structure can lead to spurious association as well as reduced power. We propose a method, ROADTRIPS, for case-control association testing in samples with partially or completely unknown population and pedigree structure. ROADTRIPS uses a covariance matrix estimated from genome-screen data to correct for unknown population and pedigree structure while maintaining high power by taking advantage of known pedigree information when it is available. ROADTRIPS can incorporate data on arbitrary combinations of related and unrelated individuals and is computationally feasible for the analysis of genetic studies with millions of markers. In simulations with related individuals and population structure, including admixture, we demonstrate that ROADTRIPS provides a substantial improvement over existing methods in terms of power and type 1 error. The ROADTRIPS method can be used across a variety of study designs, ranging from studies that have a combination of unrelated individuals and small pedigrees to studies of isolated founder populations with partially known or completely unknown pedigrees. We apply the method to analyze two data sets: a study of rheumatoid arthritis in small UK pedigrees, from Genetic Analysis Workshop 15, and data from the Collaborative Study of the Genetics of Alcoholism on alcohol dependence in a sample of moderate-size pedigrees of European descent, from Genetic Analysis Workshop 14. We detect genome-wide significant association, after Bonferroni correction, in both studies.
机译:通常进行全基因组关联研究,以鉴定影响复杂疾病的遗传变异。众所周知,不正确考虑人口或血统结构会导致虚假联想并降低权力。我们提出了一种ROADTRIPS方法,用于对具有部分或完全未知的总体和血统结构的样本进行病例对照关联测试。 ROADTRIPS使用从基因组筛选数据估计的协方差矩阵来校正未知种群和血统结构,同时利用已知的血统信息(如果可用)来保持较高的功效。 ROADTRIPS可以合并有关和无关的个体的任意组合的数据,对于具有数百万个标记的遗传研究分析在计算上是可行的。在与相关个体和总体结构(包括混合)的模拟中,我们证明ROADTRIPS在功效和1类错误方面比现有方法有了实质性的改进。 ROADTRIPS方法可用于多种研究设计,从具有无关个人和小血统的组合的研究到具有部分已知或完全未知的谱系的孤立创始人群体的研究。我们应用该方法分析了两个数据集:遗传分析研讨会15上的英国小家谱中的类风湿性关节炎研究,以及欧洲中型谱系样本中酒精依赖遗传学对酒精依赖的协同研究数据遗传分析工作室14的血统。在两项研究中,在Bonferroni校正后,我们检测到全基因组显着关联。

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