Abstract
BackgroundTo determine the clinical characteristics and molecular genetic background responsible for USH2A mutations associated with nonsyndromic retinitis pigmentosa (RP) in five Chinese families, a retrospective cross‐sectional study was performed.MethodsData on detailed history and comprehensive ophthalmological examinations were extracted from medical charts. Genomic DNA was sequenced by whole‐exome sequencing. The pathogenicity predictions were evaluated by in silico analysis. The structural modeling of the wide‐type and mutant USH2A proteins was displayed based on the I‐Tasser software.ResultsThe ultra‐wide‐field fundus imaging showed a distinctive pattern of hyperautofluorescence in the parafoveal ring with macular sparing. Ten USH2A variants were detected, including seven missense mutations, two splicing mutations, and one insertion mutation. Six of these variants have already been reported, and the remaining four were novel. Of the de novo mutations, the p.C931Y and p.G4489S mutations were predicted to be deleterious or probably damaging; the p.M4853V mutation was predicted to be neutral or benign; and the IVS22+3A>G mutation was a splicing mutation that could influence mRNA splicing and affect the formation of the hairpin structure of the USH2A protein.ConclusionsOur data further confirm that USH2A protein plays a pivotal role in the maintenance of photoreceptors and expand the spectrum of USH2A mutations that are associated with nonsyndromic RP in Chinese patients.
Highlights
To determine the clinical characteristics and molecular genetic background responsible for Usher syndrome 2A (USH2A) mutations associated with nonsyndromic retinitis pigmentosa (RP) in five Chinese families, a retrospective cross-sectional study was performed
Our data further confirm that USH2A plays a pivotal role in the maintenance of photoreceptors and expand the spectrum of USH2A mutations that are associated with nonsyndromic RP in Chinese patients
Among 25 patients clinically diagnosed with RP, 10 eyes of 5 probands from 5 pedigrees with nonsyndromic RP resulting from USH2A mutations were included (Figure 1)
Summary
To determine the clinical characteristics and molecular genetic background responsible for USH2A mutations associated with nonsyndromic retinitis pigmentosa (RP) in five Chinese families, a retrospective cross-sectional study was performed. Retinitis pigmentosa (RP) is the most common inherited retinal degeneration and occurs in approximately 1 in 4000 individuals worldwide [1]. The typical clinical signs of RP include retinal arteriolar attenuation and a generalized and diffuse pattern of mottled and moth-eaten retinal pigment epithelium (RPE). The disease onset, progression, retinal characteristics, and visual prognosis may vary remarkably among patients, even within the same family [4, 5]. Sporadic cases account for approximately 40% of all cases, these data vary between different populations [6]
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