Lattice corneal dystrophy associated with the Ala546Asp and Pro551Gln missense changes in theTGFBIgene

Purpose To report a phenotypic variant of lattice corneal dystrophy associated with two missense changes, Ala546Asp and Pro551Gln, in the transforming growth factor-β-induced gene (TGFBI). Design Experimental study. Methods Genomic DNA was obtained from the proband as well as affected and unaffected...

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Bibliographic Details
Published inAmerican journal of ophthalmology Vol. 138; no. 5; p. 772
Main Authors Aldave, Anthony J, Gutmark, Julie G, Yellore, Vivek S, Affeldt, John A, Meallet, Mario A, Udar, Nitin, Rao, Narsing A, Small, Kent W, Klintworth, Gordon K
Format Journal Article
LanguageEnglish
Published Chicago Elsevier Limited 01.11.2004
Subjects
Classification
Deoxyribonucleic acid
DNA
Family medical history
Studies
Thermal cycling
Visual impairment
California
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Summary:Purpose To report a phenotypic variant of lattice corneal dystrophy associated with two missense changes, Ala546Asp and Pro551Gln, in the transforming growth factor-β-induced gene (TGFBI). Design Experimental study. Methods Genomic DNA was obtained from the proband as well as affected and unaffected family members. Exons 4, 11, 12, and 14 of theTGFBIgene were amplified and sequenced. Additionally, a corneal button excised from the proband was examined by light and transmission electron microscopy. Haplotype analysis was performed on the proband's family and members of a previously identified pedigree with the sameTGFBIgene missense changes. Results Bilateral, symmetric, radially arranged, branching refractile lines within and surrounding an area of central anterior stromal haze were noted in the proband. Multiple polymorphic, refractile deposits were noted in the mid and posterior stroma in both the proband and her daughter. Light and electron microscopic analyses demonstrated amyloid and excluded the presence of deposits characteristic of granular corneal dystrophy. Screening ofTGFBIexon 12 in the proband and her affected daughter revealed two missense changes, Ala546Asp and Pro551Gln (both absent in 250 control chromosomes). Haplotype analysis suggested that the mutations in this family and in a previously identified pedigree reflect a founder effect, rather than an independent occurrence. Conclusions We present a phenotypic variant of lattice corneal dystrophy associated with the Ala546Asp and Pro551Gln missense changes in exon 12 of theTGFBIgene. A common ancestor appears to account for the missense mutations observed in this pedigree and in a previously reported family.
ISSN:0002-9394
1879-1891
DOI:10.1016/j.ajo.2004.06.021