Recombinant Human MG53 Protein Protects Against Alkaline-Induced Corneal Injuries in Mice

Author:

Guo Owen12,Ju Brent32,Shawver McKinley H2,Geng Bingchuan2,Wei Siqi2,Early Terriah2,Yi Frank2,Tan Tao24,Chandler Heather L5,Ma Jianjie21,Zhu Hua21

Affiliation:

1. Dublin Jerome High School, Dublin, OH 43016, USA

2. Department of Surgery, Davis Heart and Lung Research Institute, The Ohio State University, Columbus, OH 43210, USA

3. Upper Arlington High School, Upper Arlington, OH 43221, USA

4. TRIM-edicine, Inc, Columbus, OH 43212, USA

5. College of Optometry, The Ohio State University, Columbus, OH 43210, USA

Abstract

ABSTRACT Introduction The current study was designed to test the potential role of recombinant human MG53 (rhMG53) protein on protecting against alkaline-induced corneal injury in mice. Materials and Methods A round filter paper with 2-mm diameter was soaked in 1 mol/L of NaOH solution. The mouse alkaline injury was generated by placing the filter paper directly on the cornea for 30 seconds and washed with 30-mL saline; 10 µL of rhMG53 solution (20 µg/mL) or saline control was topically administrated on the mouse corneas (twice per day for 10 days). Re-epithelialization was measured by fluorescein staining and imaged by a slit lamp equipped with a digital camera. Clinical neovascularization and opacity scores were measured every day after injury. Ten days after injury, mice were sacrificed and corneas were dissected out for flat mount staining of CD31 for neovascularization. Results MG53 was present in both dog aqueous humor and human tears. mg53-/- corneas were more susceptible to alkaline-induced corneal injury. Topical treatment of rhMG53 improved re-epithelialization, suppressed neovascularization, and fibrosis induced by alkaline injury. Conclusions rhMG53 may be an effective means to treat corneal wounding.

Funder

U.S. Department of Defense

NIH

Publisher

Oxford University Press (OUP)

Subject

Public Health, Environmental and Occupational Health,General Medicine

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