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Clustering of haplotypes based on phylogeny: how good a strategy for association testing?

机译:基于系统发育的单倍型聚类:关联测试的策略有多好?

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Haplotypes are now widely used in association studies between markers and disease susceptibility locus. However, when a large number of markers are considered, the number of possible haplotypes increases leading to two problems: an increased number of degrees of freedom that may result in a lack of power and the existence of rare haplotypes that may be difficult to take into account in the statistical analysis. In a recent paper, Durrant et al proposed a method, CLADHC, to group haplotypes based on distance matrices and showed that this could considerably increase the power of the association test as compared to either single-locus analysis or haplotype analysis without prior grouping. Although the authors considered different one-disease-locus susceptibility models in their simulations, they did not study the impact of the linkage disequilibrium (LD) pattern and of the susceptibility allele frequency on their conclusions. Here, we show, using haplotype data from five regions of the genome of differentlengths and with different LD patterns, that, when a single disease susceptibility locus is simulated, the prior grouping of haplotypes based on the algorithm of Durrant et al does not increase the power of association testing except in very particular situations of LD patterns and allele frequencies.
机译:单倍型现已广泛用于标记物与疾病易感性基因座之间的关联研究。但是,当考虑大量标记时,可能的单倍型数量增加,导致两个问题:增加的自由度数量可能会导致缺乏动力,并且存在罕见的单倍型,可能难以考虑统计分析中的帐户。在最近的一篇论文中,Durrant等人提出了一种基于距离矩阵对单倍型进行分组的方法CLADHC,结果表明,与不进行事先分组的单基因座分析或单倍型分析相比,这可以大大提高关联测试的能力。尽管作者在模拟中考虑了不同的一病-位点易感性模型,但他们并未研究连锁不平衡(LD)模式和易感性等位基因频率对其结论的影响。在这里,我们显示,使用来自不同长度和不同LD模式的五个基因组区域的单倍型数据,当模拟单个疾病易感性基因座时,基于Durrant等人算法的先前单倍型分组不会增加关联测试的强大功能,但在LD模式和等位基因频率的特殊情况下除外。

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