| Literature DB >> 10704279 |
R S Smith1, N L Hawes, B Chang, T H Roderick, E C Akeson, J R Heckenlively, X Gong, X Wang, M T Davisson.
Abstract
A new cataract mutation was discovered in an ongoing program to identify new mouse models of hereditary eye disease. Lens opacity 12 (Lop12) is a semidominant mutation that results in an irregular nuclear lens opacity similar to the human Coppock cataract. Lop12 is associated with a small nonrecombining segment that maps to mouse Chromosome 1 close to the eye lens obsolescence mutation (Cryge(Cat2-Elo)), a member of the gamma-crystallin gene cluster (Cryg). Using a systemic candidate gene approach to analyze the entire Cryg cluster, a G to A transition was found in exon 3 of Crygd associated with the Lop12 mutation and has been designated Crygd(Lop12). The mutation Crygd(Lop12) leads to the formation of an in-frame stop codon that produces a truncated protein of 156 amino acids. It is predicted that the defective gene product alters protein folding of the gamma-crystallin(s) and results in lens opacity. Copyright 2000 Academic Press.Entities:
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Year: 2000 PMID: 10704279 DOI: 10.1006/geno.1999.6054
Source DB: PubMed Journal: Genomics ISSN: 0888-7543 Impact factor: 5.736