Author/Authors :
keramatipour, m. Department of Medical Genetics - Tehran University of Medical Sciences - Tehran, Iran , ghofrani , m. Department of Medical Genetics - Tehran University of Medical Sciences - Tehran, Iran , yahyaei, m. Department of Medical Genetics - Tehran University of Medical Sciences - Tehran, Iran , brunner, h.g. Department of Human Genetics - Radboud University Medical Center - Nijmegen, the Netherlands , cremers, f.p.m. Department of Human Genetics - Radboud University Medical Center - Nijmegen, the Netherlands , imran khan, m. Department of Human Genetics - Radboud University Medical Center - Nijmegen, the Netherlands , movasat , m. Eye Research Center - Tehran University of Medical Sciences - Farabi Eye Hospital - Tehran, Iran
Abstract :
Inherited retinal diseases (IRDs) are a group of genetic disorders with high degrees of clinical, genetic
and allelic heterogeneity. IRDs generally show progressive retinal cell death resulting in gradual vision loss. IRDs
constitute a broad spectrum of disorders including retinitis pigmentosa and Leber congenital amaurosis. In this
study, we performed genotyping studies to identify the underlying mutations in three Iranian families. Methods:
Having employed homozygosity mapping and Sanger sequencing, we identified the underlying mutations in the
crumbs homologue 1 gene. The CRB1 protein is a part of a macromolecular complex with a vital role in retinal cell
polarity, morphogenesis, and maintenance. Results: We identified a novel homozygous variant (c.1053_1061del;
p.Gly352_Cys354del) in one family, a combination of a novel (c.2086T>C; p.Cys696Arg) and a known variant
(c.2234C>T, p.Thr745Met) in another family and a homozygous novel variant (c.3090T>A; p.Asn1030Lys) in a third
family. Conclusion: This study shows that mutations in CRB1 are relatively common in Iranian non-syndromic IRD
patients.
Keywords :
Iran , Mutation , Leber congenital amaurosis , Retinitis pigmentosa , Retinal degeneration
