TY - JOUR
T1 - Clinical and Genetic Characteristics of 18 Patients from 13 Japanese Families with CRX-associated retinal disorder
T2 - Identification of Genotype-phenotype Association
AU - Japan Eye Genetics Consortium
AU - Fujinami-Yokokawa, Yu
AU - Fujinami, Kaoru
AU - Kuniyoshi, Kazuki
AU - Hayashi, Takaaki
AU - Ueno, Shinji
AU - Mizota, Atsushi
AU - Shinoda, Kei
AU - Arno, Gavin
AU - Pontikos, Nikolas
AU - Yang, Lizhu
AU - Liu, Xiao
AU - Sakuramoto, Hiroyuki
AU - Katagiri, Satoshi
AU - Mizobuchi, Kei
AU - Kominami, Taro
AU - Terasaki, Hiroko
AU - Nakamura, Natsuko
AU - Kameya, Shuhei
AU - Yoshitake, Kazutoshi
AU - Miyake, Yozo
AU - Kurihara, Toshihide
AU - Tsubota, Kazuo
AU - Miyata, Hiroaki
AU - Iwata, Takeshi
AU - Tsunoda, Kazushige
AU - Nishimura, Toshihide
AU - Hayashizaki, Yoshihide
AU - Kondo, Mineo
AU - Shimozawa, Nobuhiro
AU - Horiguchi, Masayuki
AU - Yamamoto, Shuichi
AU - Kuze, Manami
AU - Naoi, Nobuhisa
AU - Machida, Shigeki
AU - Shimada, Yoshiaki
AU - Nakamura, Makoto
AU - Fujikado, Takashi
AU - Hotta, Yoshihiro
AU - Takahashi, Masayo
AU - Mochizuki, Kiyofumi
AU - Murakami, Akira
AU - Kondo, Hiroyuki
AU - Ishida, Susumu
AU - Nakazawa, Mitsuru
AU - Hatase, Tetsuhisa
AU - Matsunaga, Tatsuo
AU - Maeda, Akiko
AU - Noda, Kosuke
AU - Tanikawa, Atsuhiro
AU - Yamamoto, Syuji
N1 - Publisher Copyright:
© 2020, The Author(s).
PY - 2020/12/1
Y1 - 2020/12/1
N2 - Inherited retinal disorder (IRD) is a leading cause of blindness, and CRX is one of a number of genes reported to harbour autosomal dominant (AD) and recessive (AR) causative variants. Eighteen patients from 13 families with CRX-associated retinal disorder (CRX-RD) were identified from 730 Japanese families with IRD. Ophthalmological examinations and phenotype subgroup classification were performed. The median age of onset/latest examination was 45.0/62.5 years (range, 15–77/25–94). The median visual acuity in the right/left eye was 0.52/0.40 (range, −0.08–2.00/−0.18–1.70) logarithm of the minimum angle of resolution (LogMAR) units. There was one family with macular dystrophy, nine with cone-rod dystrophy (CORD), and three with retinitis pigmentosa. In silico analysis of CRX variants was conducted for genotype subgroup classification based on inheritance and the presence of truncating variants. Eight pathogenic CRX variants were identified, including three novel heterozygous variants (p.R43H, p.P145Lfs*42, and p.P197Afs*22). A trend of a genotype-phenotype association was revealed between the phenotype and genotype subgroups. A considerably high proportion of CRX-RD in ADCORD was determined in the Japanese cohort (39.1%), often showing the mild phenotype (CORD) with late-onset disease (sixth decade). Frequently found heterozygous missense variants located within the homeodomain underlie this mild phenotype. This large cohort study delineates the disease spectrum of CRX-RD in the Japanese population.
AB - Inherited retinal disorder (IRD) is a leading cause of blindness, and CRX is one of a number of genes reported to harbour autosomal dominant (AD) and recessive (AR) causative variants. Eighteen patients from 13 families with CRX-associated retinal disorder (CRX-RD) were identified from 730 Japanese families with IRD. Ophthalmological examinations and phenotype subgroup classification were performed. The median age of onset/latest examination was 45.0/62.5 years (range, 15–77/25–94). The median visual acuity in the right/left eye was 0.52/0.40 (range, −0.08–2.00/−0.18–1.70) logarithm of the minimum angle of resolution (LogMAR) units. There was one family with macular dystrophy, nine with cone-rod dystrophy (CORD), and three with retinitis pigmentosa. In silico analysis of CRX variants was conducted for genotype subgroup classification based on inheritance and the presence of truncating variants. Eight pathogenic CRX variants were identified, including three novel heterozygous variants (p.R43H, p.P145Lfs*42, and p.P197Afs*22). A trend of a genotype-phenotype association was revealed between the phenotype and genotype subgroups. A considerably high proportion of CRX-RD in ADCORD was determined in the Japanese cohort (39.1%), often showing the mild phenotype (CORD) with late-onset disease (sixth decade). Frequently found heterozygous missense variants located within the homeodomain underlie this mild phenotype. This large cohort study delineates the disease spectrum of CRX-RD in the Japanese population.
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U2 - 10.1038/s41598-020-65737-z
DO - 10.1038/s41598-020-65737-z
M3 - Article
C2 - 32533067
AN - SCOPUS:85086361389
SN - 2045-2322
VL - 10
JO - Scientific reports
JF - Scientific reports
IS - 1
M1 - 9531
ER -