A hypomorphic variant in EYS detected by genome-wide association study contributes toward retinitis pigmentosa

Author:

Nishiguchi Koji M.,Miya FuyukiORCID,Mori Yuka,Fujita Kosuke,Akiyama Masato,Kamatani Takashi,Koyanagi Yoshito,Sato KotaORCID,Takigawa Toru,Ueno Shinji,Tsugita Misato,Kunikata Hiroshi,Cisarova Katarina,Nishino Jo,Murakami AkiraORCID,Abe Toshiaki,Momozawa Yukihide,Terasaki Hiroko,Wada Yuko,Sonoda Koh-Hei,Rivolta CarloORCID,Tsunoda TatsuhikoORCID,Tsujikawa Motokazu,Ikeda Yasuhiro,Nakazawa Toru

Abstract

AbstractThe genetic basis of Japanese autosomal recessive retinitis pigmentosa (ARRP) remains largely unknown. Herein, we applied a 2-step genome-wide association study (GWAS) in 640 Japanese patients. Meta-GWAS identified three independent peaks at P < 5.0 × 10−8, all within the major ARRP gene EYS. Two of the three were each in linkage disequilibrium with a different low frequency variant (allele frequency < 0.05); a known founder Mendelian mutation (c.4957dupA, p.S1653Kfs*2) and a non-synonymous variant (c.2528 G > A, p.G843E) of unknown significance. mRNA harboring c.2528 G > A failed to restore rhodopsin mislocalization induced by morpholino-mediated knockdown of eys in zebrafish, consistent with the variant being pathogenic. c.2528 G > A solved an additional 7.0% of Japanese ARRP cases. The third peak was in linkage disequilibrium with a common non-synonymous variant (c.7666 A > T, p.S2556C), possibly representing an unreported disease-susceptibility signal. GWAS successfully unraveled genetic causes of a rare monogenic disorder and identified a high frequency variant potentially linked to development of local genome therapeutics.

Publisher

Springer Science and Business Media LLC

Subject

General Agricultural and Biological Sciences,General Biochemistry, Genetics and Molecular Biology,Medicine (miscellaneous)

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