Bayesian inference analyses of the polygenic architecture of rheumatoid arthritis.

Stahl, Ea; Wegmann, D; Trynka, G; Gutierrez Achury, J; Do, R; Voight, Bf; Kraft, P; Chen, R; Kallberg, Hj; Kurreeman, Fa; Diabetes Genetics Replication,; Meta Analysis Consortium,; Myocardial Infarction Genetics Consortium,; Kathiresan, S; Wijmenga, C; Gregersen, Pk; Alfredsson, L; Siminovitch, Ka; Worthington, J; De Bakker, Pi; Raychaudhuri, S; Plenge, Rm; Voight, Bf; Scott, Lj; Steinthorsdottir, V; Morris, Ap; Dina, C; Welch, Rp; Zeggini, E; Huth, C; Aulchenko, Ys; Thorleifsson, G; Mcculloch, Lj; Ferreira, T; Grallert, H; Amin, N; Wu, G; Willer, Cj; Raychaudhuri, S; Mccarroll, Sa; Langenberg, C; Hofmann, Om; Dupuis, J; Qi, L; Segrè, Av; Van Hoek, M; Navarro, P; Ardlie, K; Balkau, B; Benediktsson, R; Bennett, Aj; Blagieva, R; Boerwinkle, E; Bonnycastle, Ll; Boström, Kb; Bravenboer, B; Bumpstead, S; Burtt, Np; Charpentier, G; Chines, Ps; Cornelis, M; Couper, Dj; Crawford, G; Doney, As; Elliott, Ks; Elliott, Al; Erdos, Mr; Fox, Cs; Franklin, Cs; Ganser, M; Gieger, C; Grarup, N; Green, T; Griffin, S; Groves, Cj; Guiducci, C; Hadjadj, S; Hassanali, N; Herder, C; Isomaa, B; Jackson, Au; Johnson, Pr; Jørgensen, T; Kao, Wh; Klopp, N; Kong, A; Kraft, P; Kuusisto, J; Lauritzen, T; Li, M; Lieverse, A; Lindgren, Cm; Lyssenko, V; Marre, M; Meitinger, T; Midthjell, K; Morken, Ma; Narisu, N; Nilsson, P; Owen, Kr; Payne, F; Perry, Jr; Petersen, Ak; Platou, C; Proença, C; Prokopenko, I; Rathmann, W; Rayner, Nw; Robertson, Nr; Rocheleau, G; Roden, M; Sampson, Mj; Saxena, R; Shields, Bm; Shrader, P; Sigurdsson, G; Sparsø, T; Strassburger, K; Stringham, Hm; Sun, Q; Swift, Aj; Thorand, B; Tichet, J; Tuomi, T; Van Dam, Rm; Van Haeften, Tw; Van Herpt, T; Van Vliet Ostaptchouk, Jv; Walters, Gb; Weedon, Mn; Wijmenga, C; Witteman, J; Bergman, Rn; Cauchi, S; Collins, Fs; Gloyn, Al; Gyllensten, U; Hansen, T; Hide, Wa; Hitman, Ga; Hofman, A; Hunter, Dj; Hveem, K; Laakso, M; Mohlke, Kl; Morris, Ad; Palmer, Cn; Pramstaller, Pp; Rudan, I; Sijbrands, E; Stein, Ld; Tuomilehto, J; Uitterlinden, A; Walker, M; Wareham, Nj; Watanabe, Rm; Abecasis, Gr; Boehm, Bo; Campbell, H; Daly, Mj; Hattersley, At; Fb, Hu; Meigs, Jb; Pankow, Js; Pedersen, O; Wichmann, He; Barroso, I; Florez, Jc; Frayling, Tm; Groop, L; Sladek, R; Thorsteinsdottir, U; Wilson, Jf; Illig, T; Froguel, P; Van Duijn, Cm; Stefansson, K; Altshuler, D; Boehnke, M; Mccarthy, Mi; Kathiresan, S; Meigs, Jb; Williams, G; Nathan, Dm; Macrae, Ca; O'Donnell, Cj; Ardissino, D; Merlini, Pa; Berzuini, C; Bernardinelli, Luisa; Peyvandi, F; Tubaro, M; Celli, P; Ferrario, M; Fetiveau, R; Marziliano, N; Casari, G; Galli, M; Ribichini, F; Rossi, M; Bernardi, F; Zonzin, P; Piazza, A; Mannucci, Pm; Schwartz, Sm; Siscovick, Ds; Yee, J; Friedlander, Y; Elosua, R; Marrugat, J; Lucas, G; Subirana, I; Sala, J; Ramos, R; Salomaa, V; Havulinna, As; Peltonen, L; Melander, O; Berglund, G; Voight, Bf; Kathiresan, S; Hirschhorn, Jn; Asselta, R; Duga, S; Spreafico, M; Musunuru, K; Daly, Mj; Purcell, S; Schwartz, Sm; Yee, J; Kathiresan, S; Lucas, G; Subirana, I; Elosua, R; Surti, A; Guiducci, C; Gianniny, L; Mirel, D; Parkin, M; Burtt, N; Gabriel, S. B.

doi:10.1038/ng.2232

The genetic architectures of common, complex diseases are largely uncharacterized. We modeled the genetic architecture underlying genome-wide association study (GWAS) data for rheumatoid arthritis and developed a new method using polygenic risk-score analyses to infer the total liability-scale variance explained by associated GWAS SNPs. Using this method, we estimated that, together, thousands of SNPs from rheumatoid arthritis GWAS explain an additional 20% of disease risk (excluding known associated loci). We further tested this method on datasets for three additional diseases and obtained comparable estimates for celiac disease (43% excluding the major histocompatibility complex), myocardial infarction and coronary artery disease (48%) and type 2 diabetes (49%). Our results are consistent with simulated genetic models in which hundreds of associated loci harbor common causal variants and a smaller number of loci harbor multiple rare causal variants. These analyses suggest that GWAS will continue to be highly productive for the discovery of additional susceptibility loci for common diseases.