Two novel mutations in the EYS gene are possible major causes of autosomal recessive retinitis pigmentosa in the japanese population

Katsuhiro Hosono; Chie Ishigami; Masayo Takahashi; Dong Ho Park; Yasuhiko Hirami; Hiroshi Nakanishi; Shinji Ueno; Tadashi Yokoi; Akiko Hikoya; Taichi Fujita; Yang Zhao; Sachiko Nishina; Jae Pil Shin; In Taek Kim; Shuichi Yamamoto; Noriyuki Azuma; Hiroko Terasaki; Miho Sato; Mineo Kondo; Shinsei Minoshima; Yoshihiro Hotta

doi:10.1371/journal.pone.0031036

Two novel mutations in the EYS gene are possible major causes of autosomal recessive retinitis pigmentosa in the japanese population

Katsuhiro Hosono, Chie Ishigami, Masayo Takahashi, Dong Ho Park, Yasuhiko Hirami, Hiroshi Nakanishi, Shinji Ueno, Tadashi Yokoi, Akiko Hikoya, Taichi Fujita, Yang Zhao, Sachiko Nishina, Jae Pil Shin, In Taek Kim, Shuichi Yamamoto, Noriyuki Azuma, Hiroko Terasaki, Miho Sato, Mineo Kondo, Shinsei MinoshimaYoshihiro Hotta

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Abstract

Retinitis pigmentosa (RP) is a highly heterogeneous genetic disease including autosomal recessive (ar), autosomal dominant (ad), and X-linked inheritance. Recently, arRP has been associated with mutations in EYS (Eyes shut homolog), which is a major causative gene for this disease. This study was conducted to determine the spectrum and frequency of EYS mutations in 100 Japanese arRP patients. To determine the prevalence of EYS mutations, all EYS exons were screened for mutations by polymerase chain reaction amplification, and sequence analysis was performed. We detected 67 sequence alterations in EYS, of which 21 were novel. Of these, 7 were very likely pathogenic mutations, 6 were possible pathogenic mutations, and 54 were predicted non-pathogenic sequence alterations. The minimum observed prevalence of distinct EYS mutations in our study was 18% (18/100, comprising 9 patients with 2 very likely pathogenic mutations and the remaining 9 with only one such mutation). Among these mutations, 2 novel truncating mutations, c.4957_4958insA (p.S1653KfsX2) and c.8868C&A (p.Y2956X), were identified in 16 patients and accounted for 57.1% (20/35 alleles) of the mutated alleles. Although these 2 truncating mutations were not detected in Japanese patients with adRP or Leber's congenital amaurosis, we detected them in Korean arRP patients. Similar to Japanese arRP results, the c.4957_4958insA mutation was more frequently detected than the c.8868C&A mutation. The 18% estimated prevalence of very likely pathogenic mutations in our study suggests a major involvement of EYS in the pathogenesis of arRP in the Japanese population. Mutation spectrum of EYS in 100 Japanese patients, including 13 distinct very likely and possible pathogenic mutations, was largely different from the previously reported spectrum in patients from non-Asian populations. Screening for c.4957_4958insA and c.8868C&A mutations in the EYS gene may therefore be very effective for the genetic testing and counseling of RP patients in Japan.

Original language	English
Article number	e31036
Journal	PLoS ONE
Volume	7
Issue number	2
DOIs	https://doi.org/10.1371/journal.pone.0031036
State	Published - 17 Feb 2012

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Hosono, K., Ishigami, C., Takahashi, M., Park, D. H., Hirami, Y., Nakanishi, H., Ueno, S., Yokoi, T., Hikoya, A., Fujita, T., Zhao, Y., Nishina, S., Shin, J. P., Kim, I. T., Yamamoto, S., Azuma, N., Terasaki, H., Sato, M., Kondo, M., ... Hotta, Y. (2012). Two novel mutations in the EYS gene are possible major causes of autosomal recessive retinitis pigmentosa in the japanese population. PLoS ONE, 7(2), Article e31036. https://doi.org/10.1371/journal.pone.0031036

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title = "Two novel mutations in the EYS gene are possible major causes of autosomal recessive retinitis pigmentosa in the japanese population",

abstract = "Retinitis pigmentosa (RP) is a highly heterogeneous genetic disease including autosomal recessive (ar), autosomal dominant (ad), and X-linked inheritance. Recently, arRP has been associated with mutations in EYS (Eyes shut homolog), which is a major causative gene for this disease. This study was conducted to determine the spectrum and frequency of EYS mutations in 100 Japanese arRP patients. To determine the prevalence of EYS mutations, all EYS exons were screened for mutations by polymerase chain reaction amplification, and sequence analysis was performed. We detected 67 sequence alterations in EYS, of which 21 were novel. Of these, 7 were very likely pathogenic mutations, 6 were possible pathogenic mutations, and 54 were predicted non-pathogenic sequence alterations. The minimum observed prevalence of distinct EYS mutations in our study was 18% (18/100, comprising 9 patients with 2 very likely pathogenic mutations and the remaining 9 with only one such mutation). Among these mutations, 2 novel truncating mutations, c.4957_4958insA (p.S1653KfsX2) and c.8868C&A (p.Y2956X), were identified in 16 patients and accounted for 57.1% (20/35 alleles) of the mutated alleles. Although these 2 truncating mutations were not detected in Japanese patients with adRP or Leber's congenital amaurosis, we detected them in Korean arRP patients. Similar to Japanese arRP results, the c.4957_4958insA mutation was more frequently detected than the c.8868C&A mutation. The 18% estimated prevalence of very likely pathogenic mutations in our study suggests a major involvement of EYS in the pathogenesis of arRP in the Japanese population. Mutation spectrum of EYS in 100 Japanese patients, including 13 distinct very likely and possible pathogenic mutations, was largely different from the previously reported spectrum in patients from non-Asian populations. Screening for c.4957_4958insA and c.8868C&A mutations in the EYS gene may therefore be very effective for the genetic testing and counseling of RP patients in Japan.",

author = "Katsuhiro Hosono and Chie Ishigami and Masayo Takahashi and Park, {Dong Ho} and Yasuhiko Hirami and Hiroshi Nakanishi and Shinji Ueno and Tadashi Yokoi and Akiko Hikoya and Taichi Fujita and Yang Zhao and Sachiko Nishina and Shin, {Jae Pil} and Kim, {In Taek} and Shuichi Yamamoto and Noriyuki Azuma and Hiroko Terasaki and Miho Sato and Mineo Kondo and Shinsei Minoshima and Yoshihiro Hotta",

year = "2012",

month = feb,

day = "17",

doi = "10.1371/journal.pone.0031036",

language = "English",

volume = "7",

journal = "PLoS ONE",

issn = "1932-6203",

publisher = "Public Library of Science",

number = "2",

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Hosono, K, Ishigami, C, Takahashi, M, Park, DH, Hirami, Y, Nakanishi, H, Ueno, S, Yokoi, T, Hikoya, A, Fujita, T, Zhao, Y, Nishina, S, Shin, JP, Kim, IT, Yamamoto, S, Azuma, N, Terasaki, H, Sato, M, Kondo, M, Minoshima, S & Hotta, Y 2012, 'Two novel mutations in the EYS gene are possible major causes of autosomal recessive retinitis pigmentosa in the japanese population', PLoS ONE, vol. 7, no. 2, e31036. https://doi.org/10.1371/journal.pone.0031036

TY - JOUR

T1 - Two novel mutations in the EYS gene are possible major causes of autosomal recessive retinitis pigmentosa in the japanese population

AU - Hosono, Katsuhiro

AU - Ishigami, Chie

AU - Takahashi, Masayo

AU - Park, Dong Ho

AU - Hirami, Yasuhiko

AU - Nakanishi, Hiroshi

AU - Ueno, Shinji

AU - Yokoi, Tadashi

AU - Hikoya, Akiko

AU - Fujita, Taichi

AU - Zhao, Yang

AU - Nishina, Sachiko

AU - Shin, Jae Pil

AU - Kim, In Taek

AU - Yamamoto, Shuichi

AU - Azuma, Noriyuki

AU - Terasaki, Hiroko

AU - Sato, Miho

AU - Kondo, Mineo

AU - Minoshima, Shinsei

AU - Hotta, Yoshihiro

PY - 2012/2/17

Y1 - 2012/2/17

N2 - Retinitis pigmentosa (RP) is a highly heterogeneous genetic disease including autosomal recessive (ar), autosomal dominant (ad), and X-linked inheritance. Recently, arRP has been associated with mutations in EYS (Eyes shut homolog), which is a major causative gene for this disease. This study was conducted to determine the spectrum and frequency of EYS mutations in 100 Japanese arRP patients. To determine the prevalence of EYS mutations, all EYS exons were screened for mutations by polymerase chain reaction amplification, and sequence analysis was performed. We detected 67 sequence alterations in EYS, of which 21 were novel. Of these, 7 were very likely pathogenic mutations, 6 were possible pathogenic mutations, and 54 were predicted non-pathogenic sequence alterations. The minimum observed prevalence of distinct EYS mutations in our study was 18% (18/100, comprising 9 patients with 2 very likely pathogenic mutations and the remaining 9 with only one such mutation). Among these mutations, 2 novel truncating mutations, c.4957_4958insA (p.S1653KfsX2) and c.8868C&A (p.Y2956X), were identified in 16 patients and accounted for 57.1% (20/35 alleles) of the mutated alleles. Although these 2 truncating mutations were not detected in Japanese patients with adRP or Leber's congenital amaurosis, we detected them in Korean arRP patients. Similar to Japanese arRP results, the c.4957_4958insA mutation was more frequently detected than the c.8868C&A mutation. The 18% estimated prevalence of very likely pathogenic mutations in our study suggests a major involvement of EYS in the pathogenesis of arRP in the Japanese population. Mutation spectrum of EYS in 100 Japanese patients, including 13 distinct very likely and possible pathogenic mutations, was largely different from the previously reported spectrum in patients from non-Asian populations. Screening for c.4957_4958insA and c.8868C&A mutations in the EYS gene may therefore be very effective for the genetic testing and counseling of RP patients in Japan.

AB - Retinitis pigmentosa (RP) is a highly heterogeneous genetic disease including autosomal recessive (ar), autosomal dominant (ad), and X-linked inheritance. Recently, arRP has been associated with mutations in EYS (Eyes shut homolog), which is a major causative gene for this disease. This study was conducted to determine the spectrum and frequency of EYS mutations in 100 Japanese arRP patients. To determine the prevalence of EYS mutations, all EYS exons were screened for mutations by polymerase chain reaction amplification, and sequence analysis was performed. We detected 67 sequence alterations in EYS, of which 21 were novel. Of these, 7 were very likely pathogenic mutations, 6 were possible pathogenic mutations, and 54 were predicted non-pathogenic sequence alterations. The minimum observed prevalence of distinct EYS mutations in our study was 18% (18/100, comprising 9 patients with 2 very likely pathogenic mutations and the remaining 9 with only one such mutation). Among these mutations, 2 novel truncating mutations, c.4957_4958insA (p.S1653KfsX2) and c.8868C&A (p.Y2956X), were identified in 16 patients and accounted for 57.1% (20/35 alleles) of the mutated alleles. Although these 2 truncating mutations were not detected in Japanese patients with adRP or Leber's congenital amaurosis, we detected them in Korean arRP patients. Similar to Japanese arRP results, the c.4957_4958insA mutation was more frequently detected than the c.8868C&A mutation. The 18% estimated prevalence of very likely pathogenic mutations in our study suggests a major involvement of EYS in the pathogenesis of arRP in the Japanese population. Mutation spectrum of EYS in 100 Japanese patients, including 13 distinct very likely and possible pathogenic mutations, was largely different from the previously reported spectrum in patients from non-Asian populations. Screening for c.4957_4958insA and c.8868C&A mutations in the EYS gene may therefore be very effective for the genetic testing and counseling of RP patients in Japan.

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U2 - 10.1371/journal.pone.0031036

DO - 10.1371/journal.pone.0031036

M3 - Article

C2 - 22363543

AN - SCOPUS:84857172787

SN - 1932-6203

VL - 7

JO - PLoS ONE

JF - PLoS ONE

IS - 2

M1 - e31036

ER -

Two novel mutations in the EYS gene are possible major causes of autosomal recessive retinitis pigmentosa in the japanese population

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