Molecular genetic and histopathological examinations for genotype-phenotype analysis in patients with TGFBI-linked corneal dystrophy

Molecular genetic and histopathological examinations for genotype-phenotype analysis in patients with TGFBI-linked corneal dystrophy

Different missense mutations in the TGFBI gene cause granular (Groenouw CDGG1, Avellino CDA, Reis-Bücklers CDB1) and lattice (Type I; Biber-Haab-Dimmer; CDL1) corneal dystrophies and, in some reports, corneal dystrophy Thiel-Behnke (CDB2). We report on the mutation spectrum and the genotype-phenotyp...

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Veröffentlicht in:Klinische Monatsblätter für Augenheilkunde 2006-10, Vol.223 (10), p.829
Hauptverfasser: Grünauer-Kloevekorn, C, Braeutigam, S, Weidle, E, Wolter-Roessler, M, Tost, F, Auw-Haedrich, C, Völcker, H E, Heinritz, W, Froster, U, Duncker, G
Format: Artikel
Sprache:ger
Schlagworte:
Adult
Corneal Dystrophies, Hereditary - classification
Corneal Dystrophies, Hereditary - genetics
Corneal Dystrophies, Hereditary - pathology
DNA Mutational Analysis
Extracellular Matrix Proteins - genetics
Female
Genetic Carrier Screening - methods
Genetic Markers - genetics
Genetic Predisposition to Disease - genetics
Genetic Testing - methods
Genotype
Humans
Male
Middle Aged
Mutation
Phenotype
Transforming Growth Factor beta - genetics
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Zusammenfassung:Different missense mutations in the TGFBI gene cause granular (Groenouw CDGG1, Avellino CDA, Reis-Bücklers CDB1) and lattice (Type I; Biber-Haab-Dimmer; CDL1) corneal dystrophies and, in some reports, corneal dystrophy Thiel-Behnke (CDB2). We report on the mutation spectrum and the genotype-phenotype correlations on the basis of clinical and histopathological examinations of 13 German families with TGFBI-linked corneal dystrophies. In 31 patients with different corneal dystrophies, DNA was extracted from leukocytes of the peripheral blood and mutation analysis was performed by direct sequencing of the TGFBI gene. Clinical and histopathological findings were compared with the molecular genetic findings for genotype-phenotype correlations. In 6 patients (2 families/one single person) with clinical and histopathological CDL1 we found a Missense mutation Arg124Cys and in 7 patients (3 families/one single person) with clinical and histopathological CDA we found a Missense mutation Arg124His in the exon 4 of the TGFBI gene. In 12 patients (4 families/2 single persons) with clinical and histopathological CDGG1 we found a Missense mutation Arg555Trypt in the codon 12 of the TGFBI gene. In all five patients (1 family/4 single persons) with clinical and histopathological CDB2 we could not find any mutation in the TGFBI gene. In one patient with exceptional clinical and histopathological findings we found a Missense mutation Ala546Asp, which was reported before only twice in connection with polymorphous corneal amyloidosis. In comparison of our clinical and histopathological findings and the molecular genetic results we found a strong genotype-phenotype correlation in patients with TGFBI-linked corneal dystrophies. Rare mutations can lead to exceptional clinical and histopathological findings which cannot be classified into the different groups of corneal dystrophies. In our patients with CDB2 we could not find any molecular genetic correlation to the TGFBI gene.
ISSN:0023-2165
DOI:10.1055/s-2006-926694