Challenge of Corneal Ulcer Healing: A Novel Conceptual Framework, the "Triad" of Corneal Ulcer Healing/Corneal Neovascularization/Intraocular Pressure, and Avascular Tendon Healing, for Evaluation of Corneal Ulcer Therapy, Therapy of Neovascularization, Glaucoma Therapy, and Pentadecapeptide BPC 157 Efficacy.

Pharmaceuticals (Basel, Switzerland)2025PMID: 41471311

ReviewAnimal StudyBPC-157

Plain Language Summary

Proposes a novel conceptual framework—a 'triad' of corneal ulcer healing, corneal neovascularization, and intraocular pressure—for evaluating therapies including BPC 157 for corneal ulcers and glaucoma. Preclinical studies showed BPC 157 accelerated corneal healing, modulated neovascularization, and maintained intraocular pressure. Extends the analysis to avascular tissues like tendon where similar healing principles apply.

Abstract

To better address the challenge of corneal ulcer healing, with already available standard agents, and those recently introduced, such as stable gastric pentadecapeptide BPC 157, we introduced a novel conceptual framework-the "triad" of corneal ulcer healing↔corneal neovascularization↔intraocular pressure-and extended it to avascular tissues such as tendon. Within this framework, cytoprotection serves as the unifying principle, underscoring that therapeutic effects are not isolated but interconnected. Preclinical studies with BPC 157 therapy, as a cytoprotection agent, illustrate this integration. BPC 157 rapidly normalizes elevated intraocular pressure in glaucomatous rats, preserves retinal integrity, restores pupil function, maintains corneal transparency during ulcer or abrasion healing, and counteracts both corneal neovascularization and dry eye. In parallel, its consistent efficacy in tendon injury models highlights a cytoprotective specificity across avascular tissues. The cornea's "angiogenic privilege," preserved during healing and tendon recovery together, provides strong proof of concept. Furthermore, mapping standard therapeutic agents used for corneal ulcers, neovascularization, or glaucoma onto this triad, and linking them with tendon healing, reveals both shared pathways and inconsistencies across existing drug classes. Analyzed were the ascorbate, fibronectin, hyaluronic acid, metalloproteinase inhibitors, EGF, FGF, NGF, insulin, and IGF-1 (corneal ulcer healing), the antiangiogenic agents (endostatin, PAI-1, PEDF, angiostatin, TSP-1, TSP-2, IFN-α), corticosteroids, NSAIDs, cyclosporine A, anti-VEGF drops (treatment of corneal neovascularization), and alpha 2-agonists, beta-blockers, carboanhydrase inhibitors, muscarinic agonists, Rho-kinase inhibitors, and prostaglandin analogs (glaucoma). Taken together, these findings advance cytoprotection as a unifying therapeutic paradigm, with BPC 157 emerging as its first exemplar, and encourage further translational research toward clinical application.

Authors

Masnec, Sanja; Kokot, Antonio; Kralj, Tamara; Zlatar, Mirna; Loncaric, Kristina; Sablic, Marko; Kalauz, Miro; Beslic, Iva; Oroz, Katarina; Mrvelj, Bozana; Beketic Oreskovic, Lidija; Oreskovic, Ivana; Strbe, Sanja; Staresinic, Borna; Slivsek, Goran; Boban Blagaic, Alenka; Seiwerth, Sven; Skrtic, Anita; Sikiric, Predrag

Keywords

corneal neovascularizationcorneal ulcer healingcorneal ulcer therapyevaluationglaucoma therapyintraocular pressurepentadecapeptide BPC 157tendon healingtherapy of neovascularization