Trans-Ethnic Fine-Mapping of Lipid Loci Identifies Population-Specific Signals and Allelic Heterogeneity That Increases the Trait Variance Explained
Permanent link
https://hdl.handle.net/10037/6053Date
2013Type
Journal articleTidsskriftartikkel
Peer reviewed
Author
Wu, Y; Waite, LL; Jackson, Anne U.; Sheu, WHH; Buyske, Steven; Absher, D; Arnett, DK; Boerwinkle, E; Bonnycastle, LL; Carty, CL; Cheng, I; Cochran, B; Croteau-Chonka, DC; Dumitrescu, L; Eaton, CB; Franceschini, N; Guo, XQ; Henderson, BE; Hindorff, LA; Kim, E; Kinnunen, L; Komulainen, P; Lee, WJ; Le Marchand, L; Lin, Y; Lindstrom, J; Holmen, Oddgeir; Mitchell, SL; Narisu, N; Robinson, JG; Schumacher, F; Stancaakovaa, A; Sundvall, J; Sung, YJ; Swift, AJ; Wang, WC; Wilkens, L; Wilsgaard, Tom; Young, AM; Adair, LS; Ballantyne, CM; Buzkova, P; Chakravarti, A; Collins, FS; Duggan, D; Feranil, AB; Ho, LT; Hung, YJ; Hunt, SC; Hveem, Kristian; Juang, JMJ; Kesaniemi, AY; Kuusisto, J; Laakso, M; Lakka, TA; Lee, IT; Leppert, MF; Matise, TC; Moilanen, L; Njølstad, Inger; Peters, U; Quertermous, T; Rauramaa, R; Rotter, JI; Saramies, J; Tuomilehto, J; Uusitupa, M; Wang, TD; Boehnke, M; Haiman, CA; Chen, YDI; Kooperberg, C; Assimes, TL; Crawford, DC; Hsiung, CA; North, KE; Mohlke, Karen L.Abstract
Genome-wide association studies (GWAS) have identified ~ 100 loci associated with blood lipid levels, but much of the trait
heritability remains unexplained, and at most loci the identities of the trait-influencing variants remain unknown. We
conducted a trans-ethnic fine-mapping study at 18, 22, and 18 GWAS loci on the Metabochip for their association with
triglycerides (TG), high-density lipoprotein cholesterol (HDL-C), and low-density lipoprotein cholesterol (LDL-C), respectively,
in individuals of African American (n = 6,832), East Asian (n = 9,449), and European (n = 10,829) ancestry. We aimed to
identify the variants with strongest association at each locus, identify additional and population-specific signals, refine
association signals, and assess the relative significance of previously described functional variants. Among the 58 loci, 33
exhibited evidence of association at P,161024 in at least one ancestry group. Sequential conditional analyses revealed that
ten, nine, and four loci in African Americans, Europeans, and East Asians, respectively, exhibited two or more signals. At
these loci, accounting for all signals led to a 1.3- to 1.8-fold increase in the explained phenotypic variance compared to the
strongest signals. Distinct signals across ancestry groups were identified at PCSK9 and APOA5. Trans-ethnic analyses
narrowed the signals to smaller sets of variants at GCKR, PPP1R3B, ABO, LCAT, and ABCA1. Of 27 variants reported previously
to have functional effects, 74% exhibited the strongest association at the respective signal. In conclusion, trans-ethnic highdensity
genotyping and analysis confirm the presence of allelic heterogeneity, allow the identification of population-specific
variants, and limit the number of candidate SNPs for functional studies.
Publisher
PLoSCitation
PLoS Genetics (2013), vol. 9(3): e1003379.Metadata
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