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2023 OMIG Abstract
Purpose: To assess the safety of miltefosine to corneal cells and tissues and to evaluate its efficacy to eliminate Acanthamoeba cysts and trophozoites.
Methods: Clinical isolates of Acanthamoeba spp. from corneal scrapings of patients with keratitis (n=17) were grown axenically, subjected to genotyping and tested against miltefosine for minimum cysticidal and trophozoiticidal concentrations (MCC, MTC). Cytotoxicity of miltefosine was assessed on human corneal epithelial cells (HCEC) at four incubation time points at different concentrations. Confluent monolayers of HCEC and ex-vivo human corneal models were challenged with A. castellanii (T4) trophozoites and cysts in the presence and absence of miltefosine for 24hrs. Cytopathic effects and changes in the corneal morphology were evaluated using microscopy and histopathology analysis.
Results: Majority of Acanthamoeba isolates tested were T4 genotype (82.3%). MTC90 and MCC90 values of miltefosine were 125 µg/mL and 4 mg/mL respectively. Miltefosine was found to be safe at 62.5 µg/mL and 125 µg/mL on HCE for 4 hours and 15 minutes, respectively. Without miltefosine, A.castellani trophozoites and cysts destroyed the cellular structures and corneal architecture within 24 hours while miltefosine pre-treatment completely prevented the infection at both the tested concentrations (62.5µg/mL, 125µg/mL). Disclosure:
N
Support:
Hyderabad Eye Research Foundation
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