Identification of a rare coding variant in complement 3 associated with age-related macular degeneration

Xiaowei Zhan,Kang Zhang,Stuart Cantsilieris,Dajiang Liu,Albert Hofman,Mohammad Othman,Goo Jun,Hyun Min Kang,Hongrong Luo,John Blangero,Christoph Licht,Youna Hu,Alexis Boleda,Chaolong Wang,Matthew Brooks,Humma Shahid,Anand Swaroop,Rinki Ratnapriya,Valentina Cipriani,Dwight Stambolian,Hong Ouyang,Yingda Jiang,Richard K Wilson ,Caroline C.w Klaver ,Lindsay A Farrer ,Elaine R Mardis ,Cornelia M Van Duijn ,Daniel C Koboldt ,Yuri V Sergeev ,Michael L Klein ,Emily Y Chew ,David E Larson ,Claudia N Von Strachwitz ,Daniel E Weeks ,Felix Graßmann ,Margaret A Pericak‐Vance ,Matthew P Johnson ,Lana M Olson ,Kari Branham ,John R Yates ,Robyn H Guymer ,Fred G Pluthero ,Gabriëlle H.s Buitendijk ,Mindy M Zhang ,Paul N Baird ,Robert S Fulton ,Ivana K Kim ,Jennifer L Bragg‐Gresham ,Jonathan L Haines ,John R Heckenlively ,Margaret M Deangelis ,Catrina C Fronick ,Yvette P Conley ,Michael B Gorin ,Lucinda L Fulton ,Andrea J Richardson ,Bernhard H F Weber ,Denise J Morgan ,Anthony T Moore ,Goncalo R Abeçasis

doi:10.1038/ng.2758

Abstract

Macular degeneration is a common cause of blindness in the elderly. To identify rare coding variants associated with a large increase in risk of age-related macular degeneration (AMD), we sequenced 2,335 cases and 789 controls in 10 candidate loci (57 genes). To increase power, we augmented our control set with ancestry-matched exome sequenced controls. An analysis of coding variation in 2,268 AMD cases and 2,268 ancestry matched controls revealed two large-effect rare variants; previously described R1210C in the CFH gene (fcase = 0.51%, fcontrol = 0.02%, OR = 23.11), and newly identified K155Q in the C3 gene (fcase = 1.06%, fcontrol = 0.39%, OR = 2.68). The variants suggest decreased inhibition of C3 by Factor H, resulting in increased activation of the alternative complement pathway, as a key component of disease biology.

Full Text