Paper detail

A model selection approach to genome wide association studies

For the vast majority of genome wide association studies (GWAS) published so far, statistical analysis was performed by testing markers individually. In this article we present some elementary statistical considerations which clearly show that in case of complex traits the approach based on multiple regression or generalized linear models is preferable to multiple testing. We introduce a model selection approach to GWAS based on modifications of Bayesian Information Criterion (BIC) and develop some simple search strategies to deal with the huge number of potential models. Comprehensive simulations based on real SNP data confirm that model selection has larger power than multiple testing to detect causal SNPs in complex models. On the other hand multiple testing has substantial problems with proper ranking of causal SNPs and tends to detect a certain number of false positive SNPs, which are not linked to any of the causal mutations. We show that this behavior is typical in GWAS for complex traits and can be explained by an aggregated influence of many small random sample correlations between genotypes of a SNP under investigation and other causal SNPs. We believe that our findings at least partially explain problems with low power and nonreplicability of results in many real data GWAS. Finally, we discuss the advantages of our model selection approach in the context of real data analysis, where we consider publicly available gene expression data as traits for individuals from the HapMap project.