Impact of whole exome sequencing among Iranian patients with autosomal recessive retinitis pigmentosa.

遗传学 外显子组测序 色素性视网膜炎 移码突变 桑格测序 生物 遗传异质性 突变 错义突变 外显子组 基因 疾病基因鉴定 ABCA4型 生物信息学 表型
作者
Maryam Beheshtian,Samira Saee Rad,Mojgan Babanejad,Marzieh Mohseni,Hassan Hashemi,Arash Eshghabadi,Fedra Hajizadeh,Mohammad R. Akbari,Kimia Kahrizi,Mohammad Riazi Esfahani,Hossein Najmabadi
出处
期刊:PubMed 卷期号:18 (11): 776-85 被引量:21
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摘要

Non-syndromic autosomal recessive Retinitis Pigmentosa (arRP) is a highly heterogeneous genetic visual disorder with a large number of causative genes. We aimed to determine the power of Whole Exome Sequencing (WES) in the identification of the genes responsible for non-syndromic arRP among Iranian patients.We used WES, followed by the Sanger sequencing to identify the underlying gene mutations causing non-syndromic arRP.Our study revealed disease-causing mutations in known arRP genes for 10 of the 13 families studied (76.9%). These mutations included two-frameshift insertion/deletion in CRB1 and ABCA4, one splicing mutation in PDE6B, four missense mutations in RP1, CRB1, PANK2 and IFT140, as well as three stop codon mutations in RDH12, PRCD, and C2orf71. Three remaining families harbored no mutation in previously known RP genes. Of the 10 diseases causing mutations identified among the investigated Iranian patients with non-syndromic arRP, eight variants had not been reported previously. We confirmed segregation of all 10 mutations with disease phenotypes in our studied population.This study supports the genetic heterogeneity of non-syndromic arRP in Iranian patients, and provides an opportunity to show the effectiveness of WES in the identification of pathogenic mutations among patients with non-syndromic arRP born to consanguineous parents.

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