Abstract

The corneal endothelium located on the posterior corneal surface is responsible for regulating stromal hydration. This is contributed by a monolayer of corneal endothelial cells (CECs), which are metabolically active in a continuous fluid-coupled efflux of ions from the corneal stroma into the aqueous humor, preventing stromal over-hydration and preserving the orderly arrangement of stromal collagen fibrils, which is essential for corneal transparency. Mature CECs do not have regenerative capacity and cell loss due to aging and diseases results in irreversible stromal edema and a loss of corneal clarity. The current gold standard of treatment for this worldwide blindness caused by corneal endothelial failure is the corneal transplantation using cadaveric donor corneas. The top indication is Fuchs corneal endothelial dystrophy/degeneration, which represents 39% of all corneal transplants performed. However, the global shortage of transplantable donor corneas has restricted the treatment outcomes, hence instigating a need to research for alternative therapies. One such avenue is the CEC regeneration from endothelial progenitors, which have been identified in the peripheral endothelium and the adjacent transition zone. This review examines the evidence supporting the existence of endothelial progenitors in the posterior limbus and summarizes the existing knowledge on the microanatomy of the transitional zone. We give an overview of the isolation and ex vivo propagation of human endothelial progenitors in the transition zone, and their growth and differentiation capacity to the corneal endothelium. Transplanting these bioengineered constructs into in vivo models of corneal endothelial degeneration will prove the efficacy and viability, and the long-term maintenance of functional endothelium. This will develop a novel regenerative therapy for the management of corneal endothelial diseases.

Highlights

  • The corneal endothelium located on the posterior corneal surface is responsible for regulating stromal hydration

  • Loss of stromal deturgescence may be accompanied by frank corneal epithelial edema and the formation of bullous epithelial cysts, the rupture of which results in severe pain, in a condition known as bullous keratopathy [14]

  • Penetrating keratoplasty (PK) was previously the most commonly performed procedure, innovations in surgical techniques have led to the development of endothelial keratoplasty (EK) techniques, including Descemet’s stripping automated endothelial keratoplasty (DSAEK) and Descemet’s membrane endothelial keratoplasty (DMEK) [15, 16]

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Summary

Introduction

The corneal endothelium located on the posterior corneal surface is responsible for regulating stromal hydration. While the entire corneal endothelium, TM, and TZ were positively labeled with different stem cell markers, including ABCG2, nestin, Oct4, Pax6, Sox2, STRO-1, and telomerase, the TZ exclusively expressed ankyrin G, a marker of TM insert cells [68].

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