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Common genetic variants near the Brittle Cornea Syndrome locus ZNF469 influence the blinding disease risk factor central corneal thickness Publication
Authors
Yi Lu
David P. Dimasi
+49 more
Pirro G. Hysi
Alex W. Hewitt
Kathryn P. Burdon
Tze'Yo Toh
Jonathan B. Ruddle
Yi Ju Li
Paul Mitchell
Paul R. Healey
Grant W. Montgomery
Narelle Hansell
Timothy D. Spector
Nicholas G. Martin
Terri L. Young
Christopher J. Hammond
Stuart Macgregor
Jamie E. Craig
David A. Mackey
Greg Gibson
HA Quigley
S Miglior
MO Gordon
MC Leske
DP Dimasi
U Pedersen
C Evereklioglu
DP Dimasi
F Segev
G Sultan
JD Brandt
OJ Lehmann
A Abu
JH Fingert
FB Berry
DY Nishimura
NK Hansell
MR Simpson
DA Mackey
P Healey
AL Price
BP McEvoy
BN Howie
GR Abecasis
A Jawaid
JE Craig
KM Brown
S Macgregor
S Macgregor
BE Huang
RC Wolfs
Publication date
1 January 2010
Publisher
'Public Library of Science (PLoS)'
Doi
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on
PubMed
Abstract
Copyright: © 2010 Lu et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.Central corneal thickness (CCT), one of the most highly heritable human traits (h2 typically>0.9), is important for the diagnosis of glaucoma and a potential risk factor for glaucoma susceptibility. We conducted genome-wide association studies in five cohorts from Australia and the United Kingdom (total N = 5058). Three cohorts were based on individually genotyped twin collections, with the remaining two cohorts genotyped on pooled samples from singletons with extreme trait values. The pooled sample findings were validated by individual genotyping the pooled samples together with additional samples also within extreme quantiles. We describe methods for efficient combined analysis of the results from these different study designs. We have identified and replicated quantitative trait loci on chromosomes 13 and 16 for association with CCT. The locus on chromosome 13 (nearest gene FOXO1) had an overall meta-analysis p-value for all the individually genotyped samples of 4.6×10−10. The locus on chromosome 16 was associated with CCT with p = 8.95×10−11. The nearest gene to the associated chromosome 16 SNPs was ZNF469, a locus recently implicated in Brittle Cornea Syndrome (BCS), a very rare disorder characterized by abnormal thin corneas. Our findings suggest that in addition to rare variants in ZNF469 underlying CCT variation in BCS patients, more common variants near this gene may contribute to CCT variation in the general population
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