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Incorporating Single-Locus Tests into Haplotype Cladistic Analysis in Case-Control Studies

机译:在案例对照研究中将单基因座检验纳入单倍型分类分析

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摘要

In case-control studies, genetic associations for complex diseases may be probed either with single-locus tests or with haplotype-based tests. Although there are different views on the relative merits and preferences of the two test strategies, haplotype-based analyses are generally believed to be more powerful to detect genes with modest effects. However, a main drawback of haplotype-based association tests is the large number of distinct haplotypes, which increases the degrees of freedom for corresponding test statistics and thus reduces the statistical power. To decrease the degrees of freedom and enhance the efficiency and power of haplotype analysis, we propose an improved haplotype clustering method that is based on the haplotype cladistic analysis developed by Durrant et al. In our method, we attempt to combine the strengths of single-locus analysis and haplotype-based analysis into one single test framework. Novel in our method is that we develop a more informative haplotype similarity measurement by using p-values obtained from single-locus association tests to construct a measure of weight, which to some extent incorporates the information of disease outcomes. The weights are then used in computation of similarity measures to construct distance metrics between haplotype pairs in haplotype cladistic analysis. To assess our proposed new method, we performed simulation analyses to compare the relative performances of (1) conventional haplotype-based analysis using original haplotype, (2) single-locus allele-based analysis, (3) original haplotype cladistic analysis (CLADHC) by Durrant et al., and (4) our weighted haplotype cladistic analysis method, under different scenarios. Our weighted cladistic analysis method shows an increased statistical power and robustness, compared with the methods of haplotype cladistic analysis>, single-locus test, and the traditional haplotype-based analyses. The real data analyses also show that our proposed method has practical significance in the human genetics field.
机译:在病例对照研究中,可以通过单基因座检测或基于单倍型的检测来探究复杂疾病的遗传关联。尽管对两种测试策略的相对优缺点有不同的看法,但通常认为基于单倍型的分析更有效地检测具有中等作用的基因。但是,基于单元型的关联测试的主要缺点是大量不同的单元型,这增加了相应测试统计的自由度,从而降低了统计功效。为了降低自由度并提高单倍型分析的效率和功效,我们提出了一种改进的单倍型聚类方法,该方法基于Durrant等人开发的单倍型分类分析。在我们的方法中,我们尝试将单基因座分析和基于单倍型分析的优势结合到一个单一的测试框架中。我们的方法中的新颖之处在于,我们通过使用从单位点关联测试获得的p值来构建权重度量,从而在某种程度上结合了疾病结果的信息,从而开发出更具信息量的单倍型相似性度量。然后将权重用于相似性度量的计算中,以在单体型分类分析中构建单体型对之间的距离度量。为了评估我们提出的新方法,我们进行了仿真分析,以比较(1)使用原始单倍型的常规基于单倍型的分析,(2)基于单基因座等位基因的分析,(3)原始单倍型分类分析(CLADHC)的相对性能(4)在不同情况下的加权单倍型分类分析方法。与单倍型分类分析>,单点测试和传统的基于单倍型的分析方法相比,我们的加权进化分析方法显示出更高的统计能力和稳健性。实际数据分析还表明,本文提出的方法在人类遗传学领域具有实际意义。

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