Abstract
Inherited retinal dystrophies are characterized by progressive retina degeneration and mutations in at least 250 genes have been associated as disease-causing. CRB1 is one of many genes analyzed in molecular diagnosis for inherited retinal dystrophy. Crumbs homolog-1 protein encoded by CRB1 is important for cell-to-cell contact, polarization of epithelial cells and the morphogenesis of photoreceptors. Pathogenic variants in CRB1 lead to a huge variety of phenotypes ranging from milder forms of inherited retinal dystrophy, such as retinitis pigmentosa to more severe phenotypes such as Leber congenital amaurosis. In this study, seven novel likely-pathogenic variants were identified: four missense variants (p.Leu479Pro, p.Ala921Pro, p.Cys948Arg and p.Asp1031Asn), two frameshift deletions (c.2536_2542del7 and c.3460_3461delTG) and one frameshift indel variant (c.276_294delinsTGAACACTGTAC). Furthermore, two patients with cone-rod dystrophy due to mutations in CRB1 were reported, supporting previous data, in which mutations in CRB1 can also cause cone-rod dystrophy. Finally, our data suggested there was a direct relation between phenotype severity and the mutation effect on protein functionality in 15 Brazilian CRB1 patients.
Highlights
The CRB1 gene is associated with some inherited retinal dystrophies (IRD)
Crumbs homolog-1 is in a subapical region of photoreceptors, it has a large extracellular part composed of 19 epidermal growth factor (EGF)-like domains and 3 laminin A globular (AG)-like domains, one transmembrane segment and a small cytoplasmic domain
The main diseases caused by mutations in CRB1 are: retinitis pigmentosa (RP) either with or without paraarteriolar preservation of retinal pigment epithelium (PPRPE), Leber congenital amaurosis (LCA) and pigmented paravenous chorioretinal atrophy[6, 7]
Summary
The CRB1 gene is associated with some inherited retinal dystrophies (IRD). In humans, it is located on chromosome 1q31.3, composed of 12 exons and encodes a protein with 1406 amino acids, called Crumbs homolog-1. It is located on chromosome 1q31.3, composed of 12 exons and encodes a protein with 1406 amino acids, called Crumbs homolog-1 This protein participates in a conserved protein network involved in the morphogenesis of photoreceptors and the establishment and maintenance of apico-basal polarization and adherent junctions of epithelial cells[1,2,3]. Mutations in CRB1 lead to retinal abnormalities such as thickening, coarse lamination patterns and loss of photoreceptor signalling[1]. Nystagmus; Severe visual loss; Minimum residual temporal visual field in the right eye; Divergent strabismus in the left eye
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