Genome-wide scan reveals association of psoriasis with IL-23 and NF-B pathways

Rajan P. Nair, Univ Mich
Kristina C. Duffin, Univ Utah
Cynthia Helms, Wash U
Jun Ding, Univ Mich
Philip E. Stuart, Univ Mich
David Goldgar, Univ Utah
Johann E. Gudjonsson, Univ Mich
Yun Li, Univ Mich
Trilokraj Tejasvi, Univ Mich
Bing-Jiag Feng, Univ Utah
Andreas Ruether, University of Kiel
Stefan Schreiber, University of Kiel
Michael Weichenthal, University of Kiel
Dafna Gladman, University of Toronto
Proton Rahman, Memorial University
Steven J. Schrodi, Celera, Inc
Sampath Prahalad, Univ Utah
Stephen L. Guthery, Univ Utah
Judith Fischer, Commissariat à l'Énergie Atomique
Wilson Liao, UCSF
Pui-Yan Kwok, UCSF
Alan Menter, Baylor University Medical Center
G Mark Lathrop, Commissariat à l'Énergie Atomique
Carol A. Wise, Texas Scottish Rite Hospital for Children
Ann B. Begovich, Celera/Roche
John J. Voorhees, Univ Utah
James T. Elder, Univ Mich
Gerald G. Krueger, Univ Utah
Anne M. Bowcock, Wash Univ
Goncalo R. Abecasis, Univ Mich

Abstract

Psoriasis is a common immune-mediated disorder that affects the skin, nails and joints. To identify psoriasis susceptibility loci, we genotyped 438,670 SNPs in 1,409 psoriasis cases and 1,436 controls of European ancestry. We followed up 21 promising SNPs in 5,048 psoriasis cases and 5,041 controls. Our results provide strong support for the association of at least seven genetic loci and psoriasis (each with combined P < 5 10-8). Loci with confirmed association include HLA-C, three genes involved in IL-23 signaling (IL23A, IL23R, IL12B), two genes that act downstream of TNF- and regulate NF-B signaling (TNIP1, TNFAIP3) and two genes involved in the modulation of Th2 immune responses (IL4, IL13). Although the proteins encoded in these loci are known to interact biologically, we found no evidence for epistasis between associated SNPs. Our results expand the catalog of genetic loci implicated in psoriasis susceptibility and suggest priority targets for study in other auto-immune disorders.