Genome-wide meta-analyses of multi-ethnic cohorts identify multiple new susceptibility loci for refractive error and myopia

Publication Description
Refractive error is the most common eye disorder worldwide, and a prominent cause of blindness. Myopia affects over 30% of Western populations, and up to 80% of Asians. The CREAM consortium conducted genome-wide meta-analyses including 37,382 individuals from 27 studies of European ancestry, and 8,376 from 5 Asian cohorts. We identified 16 new loci for refractive error in subjects of European ancestry, of which 8 were shared with Asians. Combined analysis revealed 8 additional loci. The new loci include genes with functions in neurotransmission (GRIA4), ion channels (KCNQ5), retinoic acid metabolism (RDH5), extracellular matrix remodeling (LAMA2, BMP2), and eye development (SIX6, PRSS56). We also confirmed previously reported associations with GJD2 and RASGRF1. Risk score analysis using associated SNPs showed a tenfold increased risk of myopia for subjects with the highest genetic load. Our results, accumulated across independent multi-ethnic studies, considerably advance understanding of mechanisms involved in refractive error and myopia.

Primary Author
Verhoeven,V. J. M.
Hysi,P.
Wojciechowski,R.
Gorgels, T. G. M. F
Bergen,A. A. B.
Klaver,C. C.
Hammond,C. J.

Volume
45

Issue
3

Start Page
314

Other Pages
318

URL
https://www.narcis.nl/publication/RecordID/oai:pure.knaw.nl:publications%2F6a354a53-5555-4a25-b8e6-314b6a18bae4

PMID
23396134



Reference Type
Journal Article

Periodical Full
Nature genetics

Publication Year
2013

ISSN/ISBN
1061-4036

Document Object Index
10.1038/ng.2554