Abstract
We conducted targeted next-generation sequencing (TGS) and/or whole exome sequencing (WES) to assess the genetic profiles of clinically suspected retinitis pigmentosa (RP) in the Korean population. A cohort of 279 unrelated Korean patients with clinically diagnosed RP and available family members underwent molecular analyses using TGS consisting of 88 RP-causing genes and/or WES with clinical variant interpretation. The combined genetic tests (TGS and/or WES) found a mutation in the 44 RP-causing genes and seven inherited retinal disease (IRD)-causing genes, and the total mutation detection rate was 57%. The mutation detection rate was higher in patients who experienced visual deterioration at a younger age (75.4%, age of symptom onset under 10 years) and who had a family history of RP (70.7%). The most common causative genes were EYS (8.2%), USH2A (6.8%), and PDE6B (4.7%), but mutations were dispersed among the 51 RP/IRD genes generally. Meanwhile, the PDE6B mutation was the most common in patients experiencing initial symptoms in their first decade, EYS in their second to third decades, and USH2A in their fifth decades and older. Of note, WES revealed some unexpected genotypes: ABCC6, CHM, CYP4V2, RS1, TGFBI, VPS13B, and WDR19, which were verified by ophthalmological re-phenotyping.
Highlights
Inherited retinal diseases (IRDs) are a group of heterogenous conditions in which progressive visual impairment is caused by retinal degeneration and are mainly caused by Mendelian mutations in 1 out of at least 300 genes, and the prevalence of inherited retinal disease (IRD) is expected as about 1:1000 in the East Asian populations [1,2]
The study was conducted according to the tenets of of the Declaration of Helsinki, and all study-related data acquisitions were approved by the Declaration of Helsinki, and all study-related data acquisitions were approved by the the Institutional Review Board of Asan Medical Center (AMC IRB No 2019-0106)
We recruited a total of 279 unrelated probands with Retinitis pigmentosa (RP); 170 probands underwent targeted next-generation sequencing (TGS)
Summary
Inherited retinal diseases (IRDs) are a group of heterogenous conditions in which progressive visual impairment is caused by retinal degeneration and are mainly caused by Mendelian mutations in 1 out of at least 300 genes, and the prevalence of IRDs is expected as about 1:1000 in the East Asian populations [1,2]. More than 80 genes have been identified as being responsible for RP [1,4]. Diverse functions of RP causative genes involve various pathways, i.e., phototransduction, vitamin A metabolism, signaling, cell–cell interaction, and protein synthesis, i.e., structural or cytoskeletal proteins, synaptic interaction proteins, mRNA intron-splicing factors, trafficking of intracellular proteins, maintenance of cilia/ciliated cells, phagocytosis, pH regulator and a few encode proteins with yet-unknown function [5].
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