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Locally-efficient robust estimation of haplotype-disease association in family-based studies

机译:基于家庭的研究中单倍型疾病关联的局部有效鲁棒估计

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摘要

Modelling human genetic variation is critical to understanding the genetic basis of complex disease. The Human Genome Project has discovered millions of binary DNA sequence variants, called single nucleotide polymorphisms, and millions more may exist. As coding for proteins takes place along chromosomes, organisation of polymorphisms along each chromosome, the haplotype phase structure, may prove to be most important in discovering genetic variants associated with disease. As haplotype phase is often uncertain, procedures that model the distribution of parental haplotypes can, if this distribution is misspecified, lead to substantial bias in parameter estimates even when complete genotype information is available. Using a geometric approach to estimation in the presence of nuisance parameters, we address this problem and develop locally-efficient estimators of the effect of haplotypes on disease that are robust to incorrect estimates of haplotype frequencies. The methods are demonstrated with a simulation study of a case-parent design.
机译:对人类遗传变异进行建模对于理解复杂疾病的遗传基础至关重要。人类基因组计划已经发现了数百万个称为单核苷酸多态性的二元DNA序列变异,并且可能还会存在数百万个。由于蛋白质的编码沿染色体发生,因此沿每个染色体的多态性组织,单倍型相结构可能被证明对发现与疾病相关的遗传变异最为重要。由于单倍型阶段通常是不确定的,因此,如果未正确指定父母单倍型分布的模型,则该程序可能会导致参数估计出现重大偏差,即使可以获得完整的基因型信息。在存在干扰参数的情况下,使用几何方法进行估计,我们解决了这个问题,并开发了对单倍型对疾病影响的局部有效估计器,该估计器对单倍型频率的不正确估计具有鲁棒性。通过对案例-父母设计的仿真研究证明了这些方法。

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