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Corneal edema following Photorefractive Keratectomy (PRK) Gerald W Zaidman, MD, FAAO,FACS Professor of Ophthalmology Sarah E. Eccles Brown, BA Westchester Medical Center New York Medical College Valhalla, NY
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THE AUTHORS DO NOT HAVE ANY FINANCIAL INTEREST IN THIS PRESENTATION
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The purpose of this poster is to present a case of a patient with nearly total loss of endothelial cells and subsequent corneal edema following PRK with mitomycin
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Case Report A 49 year old fireman underwent refractive surgery in May 2005 He had had flash burns to his eyes so he had no eyelashes or eyebrows His preoperative refraction was OD -4.75 – 2.50 x 40 OS -5.50 – 1.00 x 110
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Case Report Corneal pachymetry was 503 OD and 502 OS Therefore his surgeon chose PRK + mitomycin – surgery completed without complication His exam in November, 2005 – VA, OD 20/40; Rx +0.75 – 0.75 x 30 VA, OS 20/25+; Rx plano PRK enhancement + mitomycin was performed
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Case Report 5 days after enhancement cornea OD became acutely inflamed Patient referred-exam showed corneal stromal edema without ulceration – Figure 1 Eye healed; residual scarring and corneal thinning – VA = 20/200 Pacyhmetry = 391 OD, 467 OS; endo cell count OS=2700 PKP performed OD 5 months later
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Figure 1
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Pathology Excised corneal button demonstrated chronic stromal keratitis, loss of Bowman’s membrane, intact Descemet’s membrane, severe hypocellularity (almost complete absence) of endothelial cells
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Discussion ► Myopic PRK may induce corneal scarring ► Mitomycin – C used since 2000 to prevent corneal haze following PRK ► Mitomycin toxicity has been reported after pterygium surgery but rarely after PRK
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Mitomycin toxicity after PTK/PRK Pfister-after PTK, 6 day use of topical mito-C led to corneal edema Torres- mito-C seen in AC after PRK, after epithelial debridement Chang-rabbit study demonstrated dose dependent increase of corneal thickness after mito-c applied to corneas debrided of epithelium Morales-patients treated with mito-C after PRK had a significant loss of endothelial cells
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Conclusions ► Mitomycin – C can penetrate into the anterior chamber ► Mitomycin – C in the anterior chamber can be toxic to endothelial cells ► Ophthalmologists should be careful about the use of Mitomycin – C in thin corneas with debrided epithelium because of an increased risk of endothelial toxicity
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References ► Pfister RR. Cornea 2004; 23: 744-7. ► Torres RM, et al. JCRS 2006; 32: 67-71. ► Chang SW. JCRS 2004; 30: 1742-1750. ► Morales AJ, et al. AJO 2006; 142: 400-4.
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