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Network-Based Model Weighting to Detect Multiple Loci Influencing Complex Diseases

机译:基于网络的模型加权可检测多种影响复杂疾病的基因座

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摘要

For genome-wide association studies it has been increasingly recognized that the popular locus-by-locus search for DNA variants associated with disease susceptibility may not be effective especially when there are interactions between or among multiple loci, for which a multi-loci search strategy may be more productive. However, even if computationally feasible, a genome-wide search over all possible multiple loci requires exploring a huge model space and making costly adjustment for multiple testing, leading to reduced statistical power. On the other hand, there are accumulating data suggesting that protein products of many disease-causing genes tend to interact with each other, or cluster in the same biological pathway. To incorporate this prior knowledge and existing data on gene networks we propose a gene network-based method to improve statistical power over that of the exhaustive search by giving higher weights to models involving genes nearby in a network. We use simulated data under realistic scenarios, including a large-scale human protein-protein interaction network and 23 known ataxia-causing genes to demonstrate potential gain by our proposed method when disease-genes are clustered in a network.
机译:对于全基因组关联研究,人们越来越认识到,流行的逐基因位点搜索与疾病易感性相关的DNA变异可能不是有效的,尤其是当多个基因座之间或多个基因座之间存在相互作用时,为此需要多基因座搜索策略可能会更有效率。但是,即使在计算上可行,对所有可能的多个基因座进行全基因组搜索也需要探索巨大的模型空间,并对多个测试进行昂贵的调整,从而导致统计能力降低。另一方面,越来越多的数据表明,许多致病基因的蛋白质产物倾向于相互影响,或者聚集在同一生物学途径中。为了将这种先验知识和现有数据整合到基因网络中,我们提出了一种基于基因网络的方法,通过对网络中涉及基因的模型赋予更高的权重,从而提高了穷举搜索的统计能力。我们在现实情况下使用模拟数据,包括大规模的人类蛋白质-蛋白质相互作用网络和23个已知的共济失调基因,以当疾病基因聚集在网络中时,通过我们提出的方法证明潜在的收益。

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