Association of CAV1/CAV2 Genomic Variants with Primary Open-angle Glaucoma Overall and by Gender and Pattern of Visual Field Loss

Overview

Journal Ophthalmology

Publisher Elsevier

Specialty Ophthalmology

Date 2014 Feb 28

PMID 24572674

Citations 60

Authors

Stephanie J Loomis

Jae H Kang

Robert N Weinreb

Brian L Yaspan

Jessica N Cooke Bailey

Douglas Gaasterland

Terry Gaasterland

Richard K Lee

Paul R Lichter

Donald L Budenz

Yutao Liu

Tony Realini

David S Friedman

Catherine A McCarty

Sayoko E Moroi

Lana Olson

Joel S Schuman

Kuldev Singh

Douglas Vollrath

Gadi Wollstein

Donald J Zack

Murray Brilliant

Arthur J Sit

William G Christen

John Fingert

Peter Kraft

Kang Zhang

R Rand Allingham

Margaret A Pericak-Vance

Julia E Richards

Michael A Hauser

Jonathan L Haines

Louis R Pasquale

Janey L Wiggs

Affiliations

Soon will be listed here.

Abstract

Purpose: The CAV1/CAV2 (caveolin 1 and caveolin 2) genomic region previously was associated with primary open-angle glaucoma (POAG), although replication among independent studies has been variable. The aim of this study was to assess the association between CAV1/CAV2 single nucleotide polymorphisms (SNPs) and POAG in a large case-control dataset and to explore associations by gender and pattern of visual field (VF) loss further.

Design: Case-control study.

Participants: We analyzed 2 large POAG data sets: the Glaucoma Genes and Environment (GLAUGEN) study (976 cases, 1140 controls) and the National Eye Institute Glaucoma Human Genetics Collaboration (NEIGHBOR) consortium (2132 cases, 2290 controls).

Methods: We studied the association between 70 SNPs located within the CAV1/CAV2 genomic region in the GLAUGEN and NEIGHBOR studies, both genotyped on the Illumina Human 660WQuadv1C BeadChip array and imputed with the Markov Chain Haplotyping algorithm using the HapMap 3 reference panel. We used logistic regression models of POAG in the overall population and separated by gender, as well as by POAG subtypes defined by type of VF defect (peripheral or paracentral). Results from GLAUGEN and NEIGHBOR were meta-analyzed, and a Bonferroni-corrected significance level of 7.7 × 10(-4) was used to account for multiple comparisons.

Main Outcome Measures: Overall POAG, overall POAG by gender, and POAG subtypes defined by pattern of early VF loss.

Results: We found significant associations between 10 CAV1/CAV2 SNPs and POAG (top SNP, rs4236601; pooled P = 2.61 × 10(-7)). Of these, 9 were significant only in women (top SNP, rs4236601; pooled P = 1.59 × 10(-5)). Five of the 10 CAV1/CAV2 SNPs were associated with POAG with early paracentral VF (top SNP, rs17588172; pooled P = 1.07 × 10(-4)), and none of the 10 were associated with POAG with peripheral VF loss only or POAG among men.

Conclusions: CAV1/CAV2 SNPs were associated significantly with POAG overall, particularly among women. Furthermore, we found an association between CAV1/CAV2 SNPs and POAG with paracentral VF defects. These data support a role for caveolin 1, caveolin 2, or both in POAG and suggest that the caveolins particularly may affect POAG pathogenesis in women and in patients with early paracentral VF defects.

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