Genetic Spectrum of EYS-associated Retinal Disease in a Large Japanese Cohort: Identification of Disease-associated Variants with Relatively High Allele Frequency

Lizhu Yang,Lihua Xiao ,Shuhei Kameya,Go Mawatari,Satoshi Katagiri,Natsuko Nakamura,Takeshi Iwata,Kazuki Kuniyoshi,Mineo Kondo,Taro Kominami,Gavin Arno,Kazutoshi Yoshitake,Kei Mizobuchi,Kei Shinoda,Kaoru Fujinami,Shinji Ueno,Hiroyuki Sakuramoto,Hiroko Terasaki,Yoichi Miyake ,Michio Ohta ,Yu Fujinami‐Yokokawa ,Atsushi Mizota,Nikolas Pontikos,Takaaki Hayashi,Nobuhisa Nao‐I ,Kazushige Tsunoda

doi:10.1038/s41598-020-62119-3

Abstract

Biallelic variants in the EYS gene are a major cause of autosomal recessive inherited retinal disease (IRD), with a high prevalence in the Asian population. The purpose of this study was to identify pathogenic EYS variants, to determine the clinical/genetic spectrum of EYS-associated retinal disease (EYS-RD), and to discover disease-associated variants with relatively high allele frequency (1%-10%) in a nationwide Japanese cohort. Sixty-six affected subjects from 61 families with biallelic or multiple pathogenic/disease-associated EYS variants were ascertained by whole-exome sequencing. Three phenotype groups were identified in EYS-RD: retinitis pigmentosa (RP; 85.94%), cone-rod dystrophy (CORD; 10.94%), and Leber congenital amaurosis (LCA; 3.12%). Twenty-six pathogenic/disease-associated EYS variants were identified, including seven novel variants. The two most prevalent variants, p.(Gly843Glu) and p.(Thr2465Ser) were found in 26 and twelve families (42.6%, 19.7%), respectively, for which the allele frequency (AF) in the Japanese population was 2.2% and 3.0%, respectively. These results expand the phenotypic and genotypic spectrum of EYS-RD, accounting for a high proportion of EYS-RD both in autosomal recessive RP (23.4%) and autosomal recessive CORD (9.9%) in the Japanese population. The presence of EYS variants with relatively high AF highlights the importance of considering the pathogenicity of non-rare variants in relatively prevalent Mendelian disorders.

Highlights

Several phenotypes have been associated with pathogenic eyes shut homologue (EYS) variants, such as retinitis pigmentosa (RP) and cone-rod dystrophy (CORD); “EYS-associated retinal disease (EYS-RD)” can be used as an accurate description for this disease, in consideration of the phenotypic spectrum[5,11,12,13]
The purpose of this study was to determine pathogenic/disease-associated EYS variants utilizing an analysis of variants with relatively high allele frequency (AF) and to clarify the clinical and genetic spectrum of EYS-RD in a large nationwide Japanese cohort
The genetic spectrum of EYS-RD is illustrated in a well-characterized large Japanese cohort of 61 families

Summary

Introduction

These results expand the phenotypic and genotypic spectrum of EYS-RD, accounting for a high proportion of EYS-RD both in autosomal recessive RP (23.4%) and autosomal recessive CORD (9.9%) in the Japanese population. Inherited retinal disease (IRD) is one of the major causes of blindness in children and the working population in developed countries[1]. In 2008, variants in the eyes shut homologue (EYS) gene (OMIM: 612424) were first identified as disease-causing for autosomal recessive retinitis pigmentosa (ARRP) by Abd El–Aziz et al and Collins et al, independently[4,5]. Over 270 disease-associated variants have been reported according to the Human Gene Mutation Database (HGMD; 2018.4 version, https://portal.biobase-international.com)[6]. Several phenotypes have been associated with pathogenic EYS variants, such as RP and CORD; “EYS-associated retinal disease (EYS-RD)” can be used as an accurate description for this disease, in consideration of the phenotypic spectrum[5,11,12,13]

Objectives

Results

Conclusion