@ARTICLE{10.3389/fgene.2011.00041, AUTHOR={Wang, Kai and Edmondson, Andrew and Li, Mingyao and Gao, Fan and Qasim, Atif and Devaney, Joseph and Burnett, Mary Susan and Waterworth, Dawn and Mooser, Vincent and Grant, Struan and Epstein, Stephen and Reilly, Muredach and Hakonarson, Hakon and Rader, Daniel}, TITLE={Pathway-Wide Association Study Implicates Multiple Sterol Transport and Metabolism Genes in HDL Cholesterol Regulation}, JOURNAL={Frontiers in Genetics}, VOLUME={2}, YEAR={2011}, URL={https://www.frontiersin.org/articles/10.3389/fgene.2011.00041}, DOI={10.3389/fgene.2011.00041}, ISSN={1664-8021}, ABSTRACT={Pathway-based association methods have been proposed to be an effective approach in identifying disease genes, when single-marker association tests do not have sufficient power. The analysis of quantitative traits may be benefited from these approaches, by sampling from two extreme tails of the distribution. Here we tested a pathway association approach on a small genome-wide association study (GWAS) on 653 subjects with extremely high high-density lipoprotein cholesterol (HDL-C) levels and 784 subjects with low HDL-C levels. We identified 102 genes in the sterol transport and metabolism pathways that collectively associate with HDL-C levels, and replicated these association signals in an independent GWAS. Interestingly, the pathways include 18 genes implicated in previous GWAS on lipid traits, suggesting that genuine HDL-C genes are highly enriched in these pathways. Additionally, multiple biologically relevant loci in the pathways were not detected by previous GWAS, including genes implicated in previous candidate gene association studies (such as LEPR, APOA2, HDLBP, SOAT2), genes that cause Mendelian forms of lipid disorders (such as DHCR24), and genes expressing dyslipidemia phenotypes in knockout mice (such as SOAT1, PON1). Our study suggests that sampling from two extreme tails of a quantitative trait and examining genetic pathways may yield biological insights from smaller samples than are generally required using single-marker analysis in large-scale GWAS. Our results also implicate that functionally related genes work together to regulate complex quantitative traits, and that future large-scale studies may benefit from pathway-association approaches to identify novel pathways regulating HDL-C levels.} }