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Rare variant collapsing in conjunction with mean log p-value and gradient boosting approaches applied to Genetic Analysis Workshop 17 data

机译:罕见变体折叠与均值p p值和梯度增强方法结合使用,应用于遗传分析研讨会17数据

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In addition to methods that can identify common variants associated with susceptibility to common diseases, there has been increasing interest in approaches that can identify rare genetic variants. We use the simulated data provided to the participants of Genetic Analysis Workshop 17 (GAW17) to identify both rare and common single-nucleotide polymorphisms and pathways associated with disease status. We apply a rare variant collapsing approach and the usual association tests for common variants to identify candidates for further analysis using pathway-based and tree-based ensemble approaches. We use the mean log p-value approach to identify a top set of pathways and compare it to those used in simulation of GAW17 dataset. We conclude that the mean log p-value approach is able to identify those pathways in the top list and also related pathways. We also use the stochastic gradient boosting approach for the selected subset of single-nucleotide polymorphisms. When compared the result of this tree-based method with the list of single-nucleotide polymorphisms used in dataset simulation, in addition to correct SNPs we observe number of false positives.
机译:除了可以识别与常见疾病易感性相关的常见变异的方法外,人们对可以识别稀有遗传变异的方法也越来越感兴趣。我们使用提供给遗传分析研讨会17(GAW17)参与者的模拟数据来识别罕见和常见的单核苷酸多态性以及与疾病状态相关的途径。我们应用了罕见的变体折叠方法和常见变体的常用关联测试,以识别候选对象,以使用基于路径和基于树的集成方法进行进一步分析。我们使用均值对数p值方法来识别一组顶级途径,并将其与GAW17数据集模拟中使用的途径进行比较。我们得出结论,对数p值均值方法能够识别出最顶层列表中的那些路径以及相关路径。我们还对单核苷酸多态性的选定子集使用随机梯度增强方法。当将这种基于树的方法的结果与数据集模拟中使用的单核苷酸多态性列表进行比较时,除了正确的SNP外,我们还观察到假阳性的数量。

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