4.7 Article

A 69 kb Deletion in chr19q13.42 including PRPF31 Gene in a Chinese Family Affected with Autosomal Dominant Retinitis Pigmentosa

JOURNAL OF CLINICAL MEDICINE (2022)

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Journal

JOURNAL OF CLINICAL MEDICINE
Volume 11, Issue 22, Pages -

Publisher

MDPI
DOI: 10.3390/jcm11226682

Keywords

retinitis pigmentosa; PRPF31; deletion; whole-genome sequencing; RNA-seq

Categories

Medicine, General & Internal

Funding

  1. National Natural Science Foundation of China [81770968]
  2. Program of Shanghai Academic Research Leader [20XD1401100]
  3. Aging and women's and children's health Special project of Shanghai Municipal Health Commission [2020YJZX0102]
  4. Shanghai Municipal Science and Technology Major Projects [2018SHZDZX05]

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This study aimed to identify the genetic cause of autosomal dominant retinitis pigmentosa (adRP) in a Chinese family and investigate the molecular mechanisms of incomplete penetrance. Through whole-genome sequencing and RNA-seq analysis, a novel large deletion of a gene was identified in mutation carriers, leading to significant differential gene expression compared to healthy controls.
We aimed to identify the genetic cause of autosomal dominant retinitis pigmentosa (adRP) and characterize the underlying molecular mechanisms of incomplete penetrance in a Chinese family affected with adRP. All enrolled family members underwent ophthalmic examinations. Whole-genome sequencing (WGS), multiplex ligation-dependent probe amplification (MLPA), linkage analysis and haplotype construction were performed in all participants. RNA-seq was performed to analyze the regulating mechanism of incomplete penetrance among affected patients, mutation carriers and healthy controls. In the studied family, 14 individuals carried a novel heterozygous large deletion of 69 kilobase (kb) in 19q13.42 encompassing exon 1 of the PRPF31 gene and five upstream genes: TFPT, OSCAR, NDUFA3, TARM1, and VSTM1. Three family members were sequenced and diagnosed as non-penetrant carriers (NPCs). RNA-seq showed significant differential expression of genes in deletion between mutation carriers and healthy control. The RP11 pedigree in this study was the largest pedigree compared to other reported RP11 pedigrees with large deletions. Early onset in all affected members in this pedigree was considered to be a special phenotype and was firstly reported in a RP11 family for the first time. Differential expression of PRPF31 between affected and unaffected subjects indicates a haploinsufficiency to cause the disease in the family. The other genes with significant differential expression might play a cooperative effect on the penetrance of RP11.

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