Fenbendazole controlsin vitrogrowth, virulence potential and animal infection in theCryptococcusmodel

Author:

de Oliveira Haroldo C.,Joffe Luna S.,Simon Karina S.,Castelli Rafael F.,Reis Flavia C. G.,Bryan Arielle M.,Borges Beatriz S.,Medeiros Lia C. Soares,Bocca Anamelia L.ORCID,Del Poeta Maurizio,Rodrigues Marcio L.ORCID

Abstract

AbstractThe human diseases caused by the fungal pathogensCryptococcus neoformansandC. gattiiare associated with high indices of mortality, and toxic and/or cost-prohibitive therapeutic protocols. The need for affordable antifungals to combat cryptococcal disease is unquestionable. Previous studies suggested benzimidazoles as promising anti-cryptococcal agents combining low cost and high antifungal efficacy, but their therapeutic potential has not been demonstrated so far. In this study, we investigated the antifungal potential of fenbendazole, the most effective anti-cryptococcal benzimidazole. Fenbendazole was inhibitory against 30 different isolates ofC. neoformansandC. gattiiat a low concentration. The mechanism of anti-cryptococcal activity of fenbendazole involved microtubule disorganization, as previously described for human parasites. In combination with fenbendazole, the concentrations of the standard antifungal amphotericin B required to control cryptococcal growth were lower than those required when this antifungal was used alone. Fenbendazole was not toxic to mammalian cells. During macrophage infection, the anti-cryptococcal effects of fenbendazole included inhibition of intracellular proliferation rates and reduced phagocytic escape through vomocytosis. Fenbendazole deeply affected the cryptococcal capsule. In a mice model of cryptococcosis, the efficacy of fenbendazole to control animal mortality was similar to that observed for amphotericin B. These results indicate that fenbendazole is a promising candidate for the future development of an efficient and affordable therapeutic tool to combat cryptococcosis.

Publisher

Cold Spring Harbor Laboratory

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