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Simulating association studies: a data-based resampling method for candidate regions or whole genome scans

机译:模拟关联研究:一种基于数据的重采样方法,用于候选区域或整个基因组扫描

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Motivation: Reductions in genotyping costs have heightened interest in performing whole genome association scans and in the fine mapping of candidate regions. Improvements in study design and analytic techniques will require the simulation of datasets with realistic patterns of linkage disequilibrium and allele frequencies for typed SNPs. Methods: We describe a general approach to simulate genotyped datasets for standard case-control or affected child trio data, by resampling from existing phased datasets. The approach allows for considerable flexibility in disease models, potentially involving a large number of interacting loci. The method is most applicable for diseases caused by common variants that have not been under strong selection, a class specifically targeted by the International HapMap project. Results: Using the three population Phase Ⅰ/Ⅱ HapMap data as a testbed for our approach, we have implemented the approach in HAP-SAMPLE, a web-based simulation tool.
机译:动机:基因分型成本的降低引起了人们对进行全基因组关联扫描和候选区域精细定位的兴趣。研究设计和分析技术的改进将要求对具有类型SNP连锁不平衡和等位基因频率的现实模式的数据集进行仿真。方法:我们描述了一种通过从现有阶段性数据集中重新采样来模拟标准病例对照或受影响的儿童三重奏数据的基因分型数据集的通用方法。该方法在疾病模型中具有相当大的灵活性,可能涉及大量相互作用的基因座。该方法最适用于尚未经过严格选择的常见变体引起的疾病,这是国际HapMap项目专门针对的一类。结果:使用三个总体Ⅰ/Ⅱ期HapMap数据作为我们方法的测试平台,我们已经在基于网络的仿真工具HAP-SAMPLE中实现了该方法。

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