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Abstract #12692 Published in IGR 7-3

VAMP5 and VAMP8 are most likely not involved in primary open-angle glaucoma

Brinkmann JFF; Ottenheim CPE; de Jong LAMS; Zegers RHC; de Smet MD; de Jong PTVM; Bergen AAB
Molecular Vision 2005; 11: 582-586


PURPOSE: To select and characterize novel POAG disease genes. On the basis of genetic position (GLC1B), expression in the optic nerve, and biochemical function (targeted membrane transport processes), we selected the human VAMP5 and VAMP8 (encoding vesicle-associated membrane proteins 5 and 8) as potential candidate disease genes for POAG. We subsequently analyzed whether or not sequence changes in VAMP5 or VAMP8 were implicated in POAG. METHODS: Genomic DNA samples from 90 POAG cases and 60 controls were screened by denaturing high performance liquid chromatography of fragments amplified by the polymerase chain reaction. Direct sequencing identified nucleotide changes. RESULTS: No nonsynonymous rare sequence variants were found in VAMP5 or VAMP8. In VAMP5, three previously identified and five new single nucleotide polymorphisms (SNPs) were found. In VAMP8, four known and two new SNPs were detected. All new SNPs did not appear to change gene function or alter gene splicing. No significant differences were found between the allele frequencies in POAG cases and controls. CONCLUSIONS: Our findings indicate that VAMP5 and VAMP8 are not involved in POAG in the Dutch population.

Dr. A.A.B. Bergen, Department of Clinical and Molecular Ophthalmogenetics, Division of Development, Aging and Genetics Diseases of the Eye, The Netherlands Ophthalmic Research Institute, Amsterdam, The Netherlands


Classification:

3.4.1 Linkage studies (Part of: 3 Laboratory methods > 3.4 Molecular genetics)



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