PLoS ONE (Jan 2012)

Telomerase immortalization of human corneal endothelial cells yields functional hexagonal monolayers.

  • Thore Schmedt,
  • Yuming Chen,
  • Tracy T Nguyen,
  • Shimin Li,
  • Joseph A Bonanno,
  • Ula V Jurkunas

DOI
https://doi.org/10.1371/journal.pone.0051427
Journal volume & issue
Vol. 7, no. 12
p. e51427

Abstract

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Human corneal endothelial cells (HCEnCs) form a monolayer of hexagonal cells whose main function is to maintain corneal clarity by regulating corneal hydration. HCEnCs are derived from neural crest and are arrested in the post-mitotic state. Thus cell loss due to aging or corneal endothelial disorders leads to corneal edema and blindness-the leading indication for corneal transplantation. Here we show the existence of morphologically distinct subpopulations of HCEnCs that are interspersed among primary cells and exhibit enhanced self-renewal competence and lack of phenotypic signs of cellular senescence. Colonies of these uniform and hexagonal HCEnCs (HCEnC-21) were selectively isolated and demonstrated high proliferative potential that was dependent on endogenous upregulation of telomerase and cyclin D/CDK4. Further transduction of HCEnC-21 with telomerase yielded a highly proliferative corneal endothelial cell line (HCEnT-21T) that was devoid of oncogenic transformation and retained critical corneal endothelial cell characteristics and functionality. This study will significantly impact the fields of corneal cell biology and regenerative medicine.