Journal of Clinical Medicine (Aug 2019)

A Mutation in <i>ZNF143</i> as a Novel Candidate Gene for Endothelial Corneal Dystrophy

  • Yonggoo Kim,
  • Hye Jin You,
  • Shin Hae Park,
  • Man Soo Kim,
  • Hyojin Chae,
  • Joonhong Park,
  • Dong Wook Jekarl,
  • Jiyeon Kim,
  • Ahlm Kwon,
  • Hayoung Choi,
  • Yeojae Kim,
  • A Rome Paek,
  • Ahwon Lee,
  • Jung Min Kim,
  • Seon Young Park,
  • Yonghwan Kim,
  • Keehyoung Joo,
  • Jooyoung Lee,
  • Jongsun Jung,
  • So-Hyang Chung,
  • Jee Won Mok,
  • Myungshin Kim

DOI
https://doi.org/10.3390/jcm8081174
Journal volume & issue
Vol. 8, no. 8
p. 1174

Abstract

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Corneal dystrophies (CDs) are a diverse group of inherited disorders with a heterogeneous genetic background. Here, we report the identification of a novel ZNF143 heterozygous missense mutation in three individuals of the same family with clinical and pathological features that are consistent with endothelial CD. Ophthalmologic examination revealed diffuse corneal clouding and edema with decreased endothelial cell density. Pathological findings showed increased corneal thickness due to edema of basal epithelial cells and stroma, and abnormal metaplastic endothelium with stratified epithelium-like changes. Patients’ metaplastic corneal endothelial cells expressed predominantly cytokerain 7, cytokeratin 19, and E-cadherin. Although Sanger sequencing did not detect any mutation associated with endothelial CDs, whole exome sequencing identified the ZNF143 c.937G>C p.(Asp313His) mutation as a candidate gene for our patients’ endothelial CD. In-vitro functional studies demonstrated that mutant ZNF143 promoted the mesenchymal-to-epithelial transition; it upregulated the expression of genes associated with epithelialization in human corneal endothelial cells. Additionally, proinflammatory cytokine responsive genes were significantly enriched after mutant ZNF143 transfection, which may contribute to the severe phenotype of the three patients. These findings link a mutation in ZNF143 with endothelial CD for the first time.

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