Abstract
BackgroundPanel‐based targeted exome sequencing was applied to identify the pathogenic variants and genetic characteristics of retinitis pigmentosa (RP) in two Chinese families, and to gain a deeper understanding of the relationship between clinical manifestations and genotypes.MethodsA total of 17 subjects, comprising two probands (total patients: four subjects) and their family member, were recruited in this study. All subjects underwent comprehensive ophthalmic examinations and clinical evaluations, and the complete history and medical records were collected according to the standard procedures. All participants were screened using the multigene panel test (Target_Eye_792_V2 chip), and Sanger sequencing was used to confirm the candidate variants.ResultsAmong these two families, a total of three novel mutations in the EYS gene were identified in patients, including a homozygous frameshift mutation c.9252_9253insT detected in two patients in one family, and the compound heterozygous splicesite mutation c.5644+2T>C and frameshift mutation c.1920_1923delTGAG detected in two patients in the another family. All patients in both families had early onset of night blindness and poor visual acuity, and with typical posterior capsule opacification. The mutation co‐segregated within all recruited individuals. In addition, one patient with compound heterozygous mutations was found to have typical blue‐blindness symptoms and detected a previously reported disease‐causing mutation c.235G>A in OPN1SW gene, which caused blue blindness manifestations and was first discovered in patient combined with RP causative genes.ConclusionsPanel‐based targeted exome sequencing was used to identify three novel variants of RP causative gene, and we also detected a known pathogenic variants of blue‐blindness causative genes in two patients. Our finding will provide a powerful basis for genetic counseling and enhance our current understanding of the genetics factors for RP families.
Highlights
Hereditary retinal degeneration is an important neurodegenerative disease and the leading cause of genetic hereditary blindness in the world
Our finding will provide a powerful basis for genetic counseling and enhance our current understanding of the genetics factors for retinitis pigmentosa (RP) families
According to different clinical symptoms, hereditary retinal degeneration can be divided into: macular degeneration (MD), retinitis pigmentosa (RP), and cone-rod dystrophy etc., and the common feature of these diseases is that the structure or function of the retina is disordered and gradually leads to the death of photoreceptor cells (Berger, Kloeckener-Gruissem, & Neidhardt, 2010; Wright, Chakarova, Abd El-Aziz, & Bhattacharya, 2010)
Summary
This work was supported by the Science, Technology and Innovation Commission of Shenzhen Municipality under grant No KQJSCX20170322143848413, Shenzhen Municipal Government of China (No JCYJ20170412152854656), Shenyang Science and Technology Project Plan (No 17-600-9-00), and a grant from the Research Grants Council of the Hong Kong Special Administrative Region, China [CityU 11256116] and [CityU 11210119].
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