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Association Mapping of Complex Trait Loci With Context-Dependent Effects and Unknown Context Variable

机译:具有上下文相关效应和未知上下文变量的复杂性状基因座的关联映射

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摘要

A novel method for Bayesian analysis of genetic heterogeneity and multilocus association in random population samples is presented. The method is valid for quantitative and binary traits as well as for multiallelic markers. In the method, individuals are stochastically assigned into two etiological groups that can have both their own, and possibly different, subsets of trait-associated (disease-predisposing) loci or alleles. The method is favorable especially in situations when etiological models are stratified by the factors that are unknown or went unmeasured, that is, if genetic heterogeneity is due to, for example, unknown genes × environment or genes × gene interactions. Additionally, a heterogeneity structure for the phenotype does not need to follow the structure of the general population; it can have a distinct selection history. The performance of the method is illustrated with simulated example of genes × environment interaction (quantitative trait with loosely linked markers) and compared to the results of single-group analysis in the presence of missing data. Additionally, example analyses with previously analyzed cystic fibrosis and type 2 diabetes data sets (binary traits with closely linked markers) are presented. The implementation (written in WinBUGS) is freely available for research purposes from .
机译:提出了一种新的随机样本中遗传异质性和多基因座关联的贝叶斯分析方法。该方法适用于定量和二元性状以及多等位标记。在该方法中,将个体随机分配到两个病因学组,这两个病学学组可以具有自己的特征,也可能是不同的与性状相关(疾病易感)基因座或等位基因的子集。该方法特别适用于病因模型被未知或无法测量的因素分层的情况,即遗传异质性是由于例如未知基因×环境或基因×基因相互作用引起的。此外,表型的异质性结构不必遵循一般人群的结构;它可以具有独特的选择历史。该方法的性能通过基因×环境相互作用的模拟示例(带有宽松链接的标记的定量性状)进行了说明,并与缺少数据的情况下的单组分析结果进行了比较。此外,还提供了使用先前分析的囊性纤维化和2型糖尿病数据集(具有紧密链接的标记的二进制特征)进行的示例分析。该实现(用WinBUGS编写)可从中免费用于研究目的。

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