International Journal of Ophthalmology (Dec 2015)

A novel CRX mutation by whole-exome sequencing in an autosomal dominant cone-rod dystrophy pedigree

  • Qin-Kang Lu,
  • Na Zhao,
  • Ya-Su Lv,
  • Wei-Kun Gong,
  • Hui-Yun Wang,
  • Qi-Hu Tong,
  • Xiao-Ming Lai,
  • Rong-Rong Liu,
  • Ming-Yan Fang,
  • Jian-Guo Zhang,
  • Zhen-Fang Du,
  • Xian-Ning Zhang

DOI
https://doi.org/10.3980/j.issn.2222-3959.2015.06.06
Journal volume & issue
Vol. 8, no. 6
pp. 1112 – 1117

Abstract

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AIM: To identify the disease-causing gene mutation in a Chinese pedigree with autosomal dominant cone-rod dystrophy (adCORD). METHODS: A southern Chinese adCORD pedigree including 9 affected individuals was studied. Whole-exome sequencing (WES), coupling the Agilent whole-exome capture system to the Illumina HiSeq 2000 DNA sequencing platform was used to search the specific gene mutation in 3 affected family members and 1 unaffected member. After a suggested variant was found through the data analysis, the putative mutation was validated by Sanger DNA sequencing of samples from all available family members. RESULTS: The results of both WES and Sanger sequencing revealed a novel nonsense mutation c.C766T (p.Q256X) within exon 5 of CRX gene which was pathogenic for adCORD in this family. The mutation could affect photoreceptor-specific gene expression with a dominant-negative effect and resulted in loss of the OTX tail, thus the mutant protein occupies the CRX-binding site in target promoters without establishing an interaction and, consequently, may block transactivation. CONCLUSION: All modes of Mendelian inheritance in CORD have been observed, and genetic heterogeneity is a hallmark of CORD. Therefore, conventional genetic diagnosis of CORD would be time-consuming and labor-intensive. Our study indicated the robustness and cost-effectiveness of WES in the genetic diagnosis of CORD.

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