Genotypic Profile and Clinical Characteristics of CRX-Associated Retinopathy in Koreans

Dong Geun Kim; Kwangsic Joo; Jinu Han; Mihyun Choi; Seong-Woo Kim; Kyu Hyung Park; Sang Jun Park; Christopher Seungkyu Lee; Suk Ho Byeon; Se Joon Woo

doi:10.3390/genes14051057

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Genotypic Profile and Clinical Characteristics of CRX-Associated Retinopathy in Koreans

Authors: Dong Geun Kim ; Kwangsic Joo ; Jinu Han ; Mihyun Choi ; Seong-Woo Kim ; Kyu Hyung Park ; Sang Jun Park ; Christopher Seungkyu Lee ; Suk Ho Byeon ; Se Joon Woo

Citation: GENES, Vol.14(5) : 1057, 2023-05

Journal Title: GENES

Issue Date: 2023-05

MeSH: Adolescent ; Adult ; Child ; Cone-Rod Dystrophies* / genetics ; East Asian People ; Female ; Humans ; Leber Congenital Amaurosis* / genetics ; Macular Degeneration* / genetics ; Male ; Middle Aged ; Pedigree ; Retinal Dystrophies* ; Retinitis Pigmentosa* / genetics ; Retrospective Studies ; Young Adult

Keywords: CRX ; Korean population ; Leber congenital amaurosis ; cone-rod dystrophy ; macular dystrophy ; retinitis pigmentos

Abstract: This study aimed to investigate the clinical characteristics of Korean patients with retinal dystrophy associated with pathogenic variants of cone rod homeobox-containing gene (CRX). We retrospectively enrolled Korean patients with CRX-associated retinal dystrophy (CRX-RD) who visited two tertiary referral hospitals. Pathogenic variants were identified using targeted panel sequencing or whole-exome sequencing. We analyzed clinical features and phenotypic spectra according to genotype. Eleven patients with CRX-RD were included in this study. Six patients with cone-rod dystrophy (CORD), two with macular dystrophy (MD), two with Leber congenital amaurosis (LCA), and one with retinitis pigmentosa (RP) were included. One patient (9.1%) had autosomal recessive inheritance, and the other ten patients (90.9%) had autosomal dominant inheritance. Six patients (54.5%) were male, and the mean age of symptom onset was 27.0 ± 17.9 years. At the first presentation, the mean age was 39.4 ± 20.6 years, and best-corrected visual acuity (BCVA) (logMAR) was 0.76 ± 0.90 in the better eye. Negative electroretinography (ERG) was observed in seven (63.6%) patients. Nine pathogenic variants were identified, including two novel variants, c.101-1G>A and c.898T>C:p.(*300Glnext*118). Taken together with the variants reported in prior studies, all variants within the homeodomain are missense variants, whereas most variants downstream of the homeodomain are truncating variants (88%). The clinical features of pathogenic variants within the homeodomain are either CORD or MD with bull's eye maculopathy, whereas variants downstream of the homeodomain cause more diverse phenotypes, with CORD and MD in 36%, LCA in 40%, and RP in 24%. This is the first case series in Korea to investigate the CRX-RD genotype-phenotype correlation. Pathogenic variants downstream of the homeodomain of the CRX gene are present as RP, LCA, and CORD, whereas pathogenic variants within the homeodomain are mainly present as CORD or MD with bull's eye maculopathy. This trend was similar to previous genotype-phenotype analyses of CRX-RD. Further molecular biologic research on this correlation is required.