Chinese family with atypical granular corneal dystrophy type I caused by the typical R555W mutation in TGFBI.

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To investigate the clinical features and genetic defects in four generations of a Chinese family affected with atypical granular corneal dystrophy type I (GCD type I ).Family history and clinical data were recorded . Genomic DNA samples were obtained from peripheral blood leukocytes of all participated . Exons of the transforming growth factor -β-induced (TGFBI ) gene were directly sequenced after being amplified by polymerase chain reaction (PCR ), and multi-point linkage analysis using microsatellite makers flanking the gene was applied to identify the disease-causing mutation .Clinical features were quite variable in patients , some patients only had opacities in the epithelium , and others revealed multiple bilateral circular , discrete , crumb-like opacities mainly in the epithelium , with several in different depths of corneal stroma , and the performance was different bilaterally , even in the same patient . Directly nucleotide sequencing revealed a heterozygous p .R 555 W mutation in the coding sequence of the TGFBI gene in all affected individuals of the family , but was not found in all unaffected . The maximum logarithm of odds (LOD ) score obtained by multi-point analysis was detected at marker locus D 5 S 393 (LOD =2 .740 ; α =1 .000 ).Our case presented with clinical futures and the pathogenic mutations in TGFBI gene , the phenotype of the pedigree was quite different from typical GCD type I , so we suggested that this phenotype was a variant of GCD type I . These findings expand the knowledge about GCD type I , and demonstrate that molecular genetic analysis is important to make an accurate diagnosis of patients with variable corneal dystrophies in clinic .