Distribution of COL8A2 and COL8A1 gene variants in Caucasian primary open angle glaucoma patients with thin central corneal thickness

T Desronvil; D Logan-Wyatt; W Abdrabou; M Triana; R Jones; S Taheri; E Del Bono; L R Pasquale; M Olivier; J L Haines; B J Fan; J L Wiggs

Distribution of COL8A2 and COL8A1 gene variants in Caucasian primary open angle glaucoma patients with thin central corneal thickness

Mol Vis. 2010 Oct 29:16:2185-91.

Authors

T Desronvil¹, D Logan-Wyatt, W Abdrabou, M Triana, R Jones, S Taheri, E Del Bono, L R Pasquale, M Olivier, J L Haines, B J Fan, J L Wiggs

Affiliation

¹ Department of Ophthalmology, Harvard Medical School and Massachusetts Eye and Ear Infirmary, Boston, MA 02114, USA.

PMID: 21139683
PMCID: PMC2994337

Abstract

Purpose: One approach to identify genes that contribute to common complex ocular disorders such as primary open angle glaucoma (POAG) is to study the genetic determinates of endophenotypes that are defined by underlying pre-disposing heritable quantitative traits such as central corneal thickness (CCT). Collagen VIII is a major component of Descemet's membrane and studies in mice have indicated that targeted inactivation of the genes encoding the collagen type 8 alpha1 (Col8a1) and collagen type 8 alpha2 (Col8a2) subunits (COL8A1 and COL8A2) results in thinning of the corneal stroma and of Descemet's membrane. The purpose of this study is to evaluate COL8A1 and COL8A2 as candidate genes for thin CCT in human POAG patients.

Methods: 100 Caucasian POAG patients were enrolled in this study. The entire COL8A1 and COL8A2 coding sequence was determined in 8 patients with CCT<513 µm (one standard deviation (36 microns) below the mean (550 microns) and 8 patients with CCT>586 µm (one standard deviation above the mean). Selected COL8A2 exons containing variants of interest were sequenced in the full POAG cohort. Association and quantitative trait analyses were performed.

Results: Three patients with CCT less than 513 µm and advanced POAG were found to have missense changes in COL8A2; two patients had a previously identified mutation, R155Q and one had a novel change, P678L (p=0.0035, Fisher's exact test). Missense changes were not found in any of the patients with CCT>513 µm and missense changes in the COL8A1 gene were not found in any patient. One common COL8A2 SNP, rs274754 was also statistically associated with CCT (p=0.018).

Conclusions: In this study we have identified COL8A2 missense changes in a group of Caucasian patients with very thin CCT and advanced POAG. These results suggest that DNA sequence variants in the COL8A2 gene may be associated with thin corneas in some glaucoma patients. Further study of COL8A2 variants in other patient populations, especially those with thinner CCT such as African-Americans would provide further support for a role of COL8A2 in corneal thickness and in glaucoma.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Aged
Amino Acid Sequence
Amino Acid Substitution / genetics
Animals
Base Sequence
Collagen Type VIII / chemistry
Collagen Type VIII / genetics*
Conserved Sequence / genetics
Cornea / pathology*
Evolution, Molecular
Female
Glaucoma, Open-Angle / genetics*
Glaucoma, Open-Angle / pathology*
Heterozygote
Humans
Male
Mice
Molecular Sequence Data
Mutation, Missense / genetics
Phenotype
Polymorphism, Single Nucleotide / genetics*
Protein Structure, Tertiary
Quantitative Trait Loci / genetics
White People / genetics*

Substances

COL8A2 protein, human
Collagen Type VIII

Abstract

Publication types

MeSH terms

Substances

Grants and funding