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Rare-variant extensions of the transmission disequilibrium test: Application to autism exome sequence data

机译:传输不平衡测试的稀有扩展:应用于自闭症外显子组序列数据

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Many population-based rare-variant (RV) association tests, which aggregate variants across a region, have been developed to analyze sequence data. A drawback of analyzing population-based data is that it is difficult to adequately control for population substructure and admixture, and spurious associations can occur. For RVs, this problem can be substantial, because the spectrum of rare variation can differ greatly between populations. A solution is to analyze parent-child trio data, by using the transmission disequilibrium test (TDT), which is robust to population substructure and admixture. We extended the TDT to test for RV associations using four commonly used methods. We demonstrate that for all RV-TDT methods, using proper analysis strategies, type I error is well-controlled even when there are high levels of population substructure or admixture. For trio data, unlike for population-based data, RV allele-counting association methods will lead to inflated type I errors. However type I errors can be properly controlled by obtaining p values empirically through haplotype permutation. The power of the RV-TDT methods was evaluated and compared to the analysis of case-control data with a number of genetic and disease models. The RV-TDT was also used to analyze exome data from 199 Simons Simplex Collection autism trios and an association was observed with variants in ABCA7. Given the problem of adequately controlling for population substructure and admixture in RV association studies and the growing number of sequence-based trio studies, the RV-TDT is extremely beneficial to elucidate the involvement of RVs in the etiology of complex traits.
机译:已经开发了许多基于人群的稀有变异(RV)关联测试,这些测试汇总了整个区域的变异,以分析序列数据。分析基于人口的数据的一个缺点是,难以充分控制人口的子结构和混合,并且可能发生虚假关联。对于RVs,这个问题可能很严重,因为不同种群之间稀有变异的频谱差异很大。一种解决方案是通过使用传输不平衡测试(TDT)分析父子三重奏数据,该测试对人口子结构和混合物具有鲁棒性。我们使用四种常用方法将TDT扩展为测试RV关联。我们证明,对于所有RV-TDT方法,使用适当的分析策略,即使存在大量人口子结构或混合物,I型错误也得到了很好的控制。对于三重数据,与基于人群的数据不同,RV等位基因计数关联方法将导致虚假的I型错误。但是,通过单倍型置换凭经验获得p值,可以正确控制I型错误。评估了RV-TDT方法的功能,并将其与具有多种遗传和疾病模型的病例对照数据进行了分析。 RV-TDT还被用于分析来自199个Simons Simplex Collection自闭症三人组的外显子组数据,并且观察到与ABCA7中的变体相关。鉴于在RV关联研究中不能充分控制种群亚结构和混合物的问题,以及基于序列的三重研究的数量不断增加,RV-TDT对于阐明RVs参与复杂性状的病因极为有利。

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