AI Article Synopsis

  • The corneal endothelium is crucial for maintaining corneal transparency, and its dysfunction can lead to significant vision issues.
  • Tissue engineering, specifically cell-based therapies using monkey and human corneal endothelial cells, shows promise as a less invasive alternative to traditional corneal transplants.
  • The incorporation of a ROCK inhibitor enhances the engraftment of these cells, suggesting potential for effective treatment of corneal endothelial dysfunction in future clinical applications.

Article Abstract

The corneal endothelium maintains corneal transparency; consequently, its dysfunction causes severe vision loss. Tissue engineering-based therapy, as an alternative to conventional donor corneal transplantation, is anticipated to provide a less invasive and more effective therapeutic modality. We conducted a preclinical study for cell-based therapy in a primate model and demonstrated regeneration of the corneal endothelium following injection of cultured monkey corneal endothelial cells (MCECs) or human CECs (HCECs), in combination with a Rho kinase (ROCK) inhibitor, Y-27632, into the anterior chamber. We also evaluated the safety and efficacy of Good Manufacturing Practice (GMP)-grade HCECs, similar to those planned for use as transplant material for human patients in a clinical trial, and we showed that the corneal endothelium was regenerated without adverse effect. We also showed that CEC engraftment is impaired by limited substrate adhesion, which is due to actomyosin contraction induced by dissociation-induced activation of ROCK/MLC signaling. Inclusion of a ROCK inhibitor improves efficiency of engraftment of CECs and enables cell-based therapy for treating corneal endothelial dysfunction as a clinically relevant therapy.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4870691PMC
http://dx.doi.org/10.1038/srep26113DOI Listing

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