| Literature DB >> 33419980 |
Go Mawatari1, Kaoru Fujinami2,3,4,5, Xiao Liu2,3,6, Lizhu Yang2,3, Yu-Fujinami Yokokawa2,7,8, Shiori Komori9, Shinji Ueno9, Hiroko Terasaki9, Satoshi Katagiri10, Takaaki Hayashi10, Kazuki Kuniyoshi11, Yozo Miyake2,12, Kazushige Tsunoda2, Kazutoshi Yoshitake13, Takeshi Iwata13, Nobuhisa Nao-I14.
Abstract
Variants in the retinitis pigmentosa GTPase regulator (RPGR) gene are a major cause of X-linked inherited retinal disorder (IRD). We herein describe the clinical and genetic features of 14 patients from 13 Japanese families harboring RPGR variants in a nationwide cohort. Comprehensive ophthalmological examinations were performed to classify the patients into one of the phenotype subgroups: retinitis pigmentosa (RP) and cone rod dystrophy (CORD). The mean age of onset/at examination was 13.8/38.1 years (range, 0-50/11-72), respectively. The mean visual acuity in the right/left eye was 0.43/0.43 (range, 0.1-1.7/-0.08-1.52) LogMAR unit. Eight patients had RP, and six had CORD. Whole-exome sequencing with target analyses identified 13 RPGR variants in 730 families with IRD, including 8 novel variants. An association between the phenotype subgroup and the position of variants (cutoff of amino acid 950) was revealed. To conclude, the clinical and genetic spectrum of RPGR-associated retinal disorder was first illustrated in a Japanese population, with a high proportion of novel variants. These results suggest the distinct genetic background of RPGR in the Japanese population, in which the genotype-phenotype association was affirmed. This evidence should be helpful monitoring and counseling patients and in selecting patients for future therapeutic trials.Year: 2019 PMID: 33419980 DOI: 10.1038/s41439-019-0065-7
Source DB: PubMed Journal: Hum Genome Var ISSN: 2054-345X