Abstract

Background: The USH2A gene encodes usherin, a basement membrane protein that is involved in the development and homeostasis of the inner ear and retina. Mutations in USH2A are linked to Usher syndrome type II (USH II) and non-syndromic retinitis pigmentosa (RP). Molecular diagnosis can provide insight into the pathogenesis of these diseases, facilitate clinical diagnosis, and identify individuals who can most benefit from gene or cell replacement therapy. Here, we report 21 pathogenic mutations in the USH2A gene identified in 11 Chinese families by using the targeted next-generation sequencing (NGS) technology.Methods: In all, 11 unrelated Chinese families were enrolled, and NGS was performed to identify mutations in the USH2A gene. Variant analysis, Sanger validation, and segregation tests were utilized to validate the disease-causing mutations in these families.Results: We identified 21 pathogenic mutations, of which 13, including 5 associated with non-syndromic RP and 8 with USH II, have not been previously reported. The novel variants segregated with disease phenotype in the affected families and were absent from the control subjects. In general, visual impairment and retinopathy were consistent between the USH II and non-syndromic RP patients with USH2A mutations.Conclusions: These findings provide a basis for investigating genotype–phenotype relationships in Chinese USH II and RP patients and for clarifying the pathophysiology and molecular mechanisms of the diseases associated with USH2A mutations.

Highlights

  • Retinitis pigmentosa (RP; OMIM 226800) is one of the most common incurable ocular diseases and can lead to severe visual impairment

  • The Usher syndrome type II (USH II) patients tended to be younger than the retinitis pigmentosa (RP) patients at the time of symptom onset, the two groups were diagnosed at a similar age

  • We performed genetic diagnosis for Usher syndrome (USH) II and non-syndromic RP cases arising from mutations in Usher syndrome 2A (USH2A) in 11 unrelated Chinese families by next-generation sequencing (NGS) and identified 21 associated mutations, of which 13 were novel and definitively pathogenic

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Summary

Introduction

Retinitis pigmentosa (RP; OMIM 226800) is one of the most common incurable ocular diseases and can lead to severe visual impairment. It is characterized by clinical and genetic heterogeneity. The most common of these is Usher syndrome (USH) [2], an autosomal recessive disorder that has a prevalence of 3.2–6.2/100000 and is characterized by sensorineural hearing loss (HL), visual impairment due to RP, and variable vestibular dysfunction with heterogeneous clinical and genetic manifestations [3,4]. Visual impairment and retinopathy were consistent between the USH II and non-syndromic RP patients with USH2A mutations. Conclusions: These findings provide a basis for investigating genotype–phenotype relationships in Chinese USH II and RP patients and for clarifying the pathophysiology and molecular mechanisms of the diseases associated with USH2A mutations

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