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Shrinkage Estimators for Robust and Efficient Inference in Haplotype-Based Case-Control Studies

机译:基于单倍型病例对照研究的鲁棒有效估计的收缩估计

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摘要

Case-control association studies often aim to investigate the role of genes and gene-environment interactions in terms of the underlying haplotypes (i.e., the combinations of alleles at multiple genetic loci along chromosomal regions). The goal of this article is to develop robust but efficient approaches to the estimation of disease odds-ratio parameters associated with haplotypes and haplotype-environment interactions. We consider "shrinkage" estimation techniques that can adaptively relax the model assumptions of Hardy-Weinberg-Equilibrium and gene-environment independence required by recently proposed efficient "retrospective" methods. Our proposal involves first development of a novel retrospective approach to the analysis of case-control data, one that is robust to the nature of the gene-environment distribution in the underlying population. Next, it involves shrinkage of the robust retrospective estimator toward a more precise, but model-dependent, retrospective estimator using novel empirical Bayes and penalized regression techniques. Methods for variance estimation are proposed based on asymptotic theories. Simulations and two data examples illustrate both the robustness and efficiency of the proposed methods.
机译:病例对照关联研究通常旨在根据潜在的单倍型(即沿着染色体区域的多个遗传位点的等位基因的组合)研究基因和基因-环境相互作用的作用。本文的目的是开发强大而有效的方法来估计与单倍型和单倍型-环境相互作用相关的疾病比值比参数。我们考虑了“收缩”估计技术,该技术可以适应性地放宽最近提出的有效“回顾”方法所需的Hardy-Weinberg-Equilibrium模型假设和基因环境独立性。我们的建议涉及首先开发一种新颖的回顾性方法来分析病例对照数据,该方法对基础人群中基因-环境分布的性质具有鲁棒性。接下来,它涉及使用新的经验贝叶斯和惩罚回归技术,将健壮的回顾性估算器缩小为更精确的,但与模型相关的回顾性估算器。提出了基于渐近理论的方差估计方法。仿真和两个数据示例说明了所提出方法的鲁棒性和效率。

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