Elastic-net regularization approaches for genome-wide association studies of rheumatoid arthritis

被引:0
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作者
Seoae Cho
Haseong Kim
Sohee Oh
Kyunga Kim
Taesung Park
机构
[1] Seoul National University,Interdisciplinary Program in Bioinformatics
[2] Imperial College London,Department of Electrical and Electronic Engineering
[3] Seoul National University,Department of Statistics
关键词
Genetic Analysis Workshop; Screen Step; Ridge Penalty; Autocrine Motility Factor Receptor; Automatic Variable Selection;
D O I
10.1186/1753-6561-3-S7-S25
中图分类号
学科分类号
摘要
The current trend in genome-wide association studies is to identify regions where the true disease-causing genes may lie by evaluating thousands of single-nucleotide polymorphisms (SNPs) across the whole genome. However, many challenges exist in detecting disease-causing genes among the thousands of SNPs. Examples include multicollinearity and multiple testing issues, especially when a large number of correlated SNPs are simultaneously tested. Multicollinearity can often occur when predictor variables in a multiple regression model are highly correlated, and can cause imprecise estimation of association. In this study, we propose a simple stepwise procedure that identifies disease-causing SNPs simultaneously by employing elastic-net regularization, a variable selection method that allows one to address multicollinearity. At Step 1, the single-marker association analysis was conducted to screen SNPs. At Step 2, the multiple-marker association was scanned based on the elastic-net regularization. The proposed approach was applied to the rheumatoid arthritis (RA) case-control data set of Genetic Analysis Workshop 16. While the selected SNPs at the screening step are located mostly on chromosome 6, the elastic-net approach identified putative RA-related SNPs on other chromosomes in an increased proportion. For some of those putative RA-related SNPs, we identified the interactions with sex, a well known factor affecting RA susceptibility.
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