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通过联合使用病例-父母三联体和病例-父母对来推断单倍型/疾病关联。

Inferring haplotype/disease association by joint use of case-parents trios and case-parent pairs.

作者信息

Hu Yue-Qing, Zhou Ji-Yuan

机构信息

Institute of Biostatistics, School of Life Sciences, Fudan University, Shanghai 200433, China.

出版信息

Ann Hum Genet. 2010 May;74(3):263-74. doi: 10.1111/j.1469-1809.2010.00563.x.

DOI:10.1111/j.1469-1809.2010.00563.x
PMID:20529016
Abstract

Recently interest has been increasing in genetic association studies using several closely linked loci. The HAP-TDT method, which uses case-parents trios is powerful for such a task. However, it is not uncommon in practice that one parent is missing for some reason, such as late onset. The case-parents trios are thus reduced to case-parent pairs. Discarding such data could lead to a severe loss of power. In this paper, we propose the HAP-1-TDT method based on case-parent pairs to detect haplotype/disease association. A permutation-based randomisation technique is devised to assess the significance of the test statistic. Furthermore, the combined statistic HAP-C-TDT is developed to use jointly case-parents trios and case-parent pairs. These test statistics can be applied to either phase-known or phase-unknown data. A number of simulation studies are conducted to investigate the validity of the proposed tests; these studies show that the statistics are robust to population structure. Using several disease genes from the literature, we illustrate that incorporating case-parent pairs into an association study leads to noticeable power gain. Moreover, our simulation results suggest that our method has better size and power than UNPHASED. Finally, in simulated scenarios where there are only a few SNPs and risk is determined by two haplotypes that are complementary or near-complementary, our method has better power than TRIMM.

摘要

最近,使用几个紧密连锁位点的基因关联研究越来越受到关注。使用病例-父母三联体的HAP-TDT方法在这项任务中很有效。然而,在实际中由于某些原因(如迟发性)导致一方父母缺失的情况并不少见。这样病例-父母三联体就减少为病例-父母对。丢弃这些数据可能会导致检验效能严重损失。在本文中,我们提出了基于病例-父母对的HAP-1-TDT方法来检测单倍型与疾病的关联。设计了一种基于排列的随机化技术来评估检验统计量的显著性。此外,还开发了联合统计量HAP-C-TDT,以联合使用病例-父母三联体和病例-父母对。这些检验统计量可应用于已知相位或未知相位的数据。进行了大量模拟研究以调查所提出检验的有效性;这些研究表明这些统计量对群体结构具有稳健性。利用文献中的几个疾病基因,我们说明了将病例-父母对纳入关联研究可显著提高检验效能。此外,我们的模拟结果表明我们的方法比UNPHASED具有更好的检验规模和检验效能。最后,在只有少数单核苷酸多态性(SNP)且风险由两个互补或近乎互补的单倍型决定的模拟场景中,我们的方法比TRIMM具有更好的检验效能。

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