Abstract
To evaluate the safety and efficacy of topical bevacizumab in the treatment of corneal neovascularization. Prospective, nonrandomized, interventional case series. setting: Institutional, multicenter clinical trial. study population: Twenty eyes from 20 patients with stable corneal neovascularization. intervention procedures: Patients were treated with topical 1.0% bevacizumab for 3 weeks and were monitored for a total of 24 weeks. main outcome measures: Primary outcome measures included: neovascular area, defined as the area of the corneal vessels themselves; vessel caliber, defined as the mean corneal vessel diameter; and invasion area, defined as the fraction of the total cornea into which the vessels extended. The occurrence of ocular and systemic adverse events was monitored closely. As compared with the baseline visit, patients exhibited a statistically significant improvement in neovascular area by week 6 (P = .007) and in vessel caliber by week 12 (P = .006). At the final visit, neovascular area, vessel caliber, and invasion area were reduced by 47.5%, 36.2%, and 20%, respectively. The decreases in neovascular area and vessel caliber were statistically significant (P < .001 and P = .003, respectively); however, the reduction in invasion area did not reach statistical significance (P = .06). There were no significant changes in the secondary outcomes, and there were no adverse events. Short-term topical bevacizumab treatment reduced the extent of stable corneal neovascularization as measured by neovascular area and vessel caliber with no associated adverse events. Interestingly, the degree of treatment efficacy was inversely proportional to the baseline invasion area.
Highlights
The healthy cornea is a unique tissue devoid of blood and lymphatic vessels
Neovascular area, vessel caliber, and invasion area were reduced by 47.5%, 36.2%, and 20%, respectively
Short-term topical bevacizumab treatment reduced the extent of stable corneal NV as measured by neovascular area and vessel caliber with no associated adverse events
Summary
The healthy cornea is a unique tissue devoid of blood and lymphatic vessels. This feature is necessary for the maintenance of corneal transparency and visual acuity. The presence of corneal vessels can influence corneal inflammation, scarring, edema, and lipid deposition, all of which serve to decrease corneal transparency.[4] In the case of corneal transplantation, ocular immune privilege, which helps extend the survival of corneal allografts,[5] can be abrogated by corneal NV.[6] the presence of stromal vessels in the host cornea is one of the strongest risk factors for subsequent graft failure.[7]
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