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2023 OMIG Abstract
Purpose: Staphylococcus aureus and Pseudomonas aeruginosa are major causes of severe bacterial corneal infections (keratitis). Unfortunately, current therapeutics are increasingly ineffective in the face of significant multi (MDR)-drug resistance, and novel treatments are urgently needed. We sought to evaluate the in vitro efficacy of the novel drug combination polymyxin B/trimethoprim (PT) + rifampin to eradicate MDR clinical keratitis isolates.
Methods: 20 S. aureus, and 19 P. aeruginosa clinical keratitis isolates were collected from the LV Prasad Eye Institute and underwent extensive minimum inhibitory concentration (MIC) testing. S. aureus isolates were tested against 22 antibiotics from 11 distinct classes, while P. aeruginosa isolates were tested with 25 antibiotics from 16 classes. MDR was defined as resistance to > 3 classes. Fractional inhibitory concentration (FIC) testing was performed with PT + rifampin. The FIC index (FICI) was calculated: FICI = (MIC drug A in combination/MIC drug A alone) + (MIC drug B in combination/MIC drug B alone). The averaged FICI from three biological replicates was defined as synergistic (FICI < 0.5), additive (0.5-1), indifference (1-4), or antagonistic (FICI > 4).
Results: Among P. aeruginosa isolates, 100% were classified as MDR. Among S. aureus isolates, 100% were resistant to at least 1 antibiotic class, 12 (60%) were MDR, and 14 (70%) were classified as methicillin-resistant (MRSA). FIC testing revealed that PT + rifampin was effective at eradicating 100% of all isolates, displaying additive or synergistic activity towards approximately 70% of strains. Mean FICI values were Disclosure:
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