The Organochalcogen Compound (MeOPhSe)2 Inhibits Both Formation and the Viability of the Biofilm Produced by Candida albicans, at Different Stages of Development.

CURRENT PHARMACEUTICAL DESIGN(2019)

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摘要
Background: Candida albicans is a commensal and opportunistic fungus which is able to produce both local and systemic infections in immunocompromised patients. A correlation has been demonstrated between the resistance to conventional antifungal drugs and C. albicans ability to produce biofilms. Therefore, the potential of the organochalcogen compounds as antifungal therapy has been demonstrated. Method: In this work, we studied the effect of the organochalcogen compound (MeOPhSe)(2) on both formation and the viability of the biofilm produced by C. albicans, at different stages of development. Biofilm formation and viability were determined by a metabolic assay based on the reduction of XTT assay. In addition, the morphology of the biofilm was observed using light microscopy. Results: A significant reduction was observed in both growth and biofilm formation by C. albicans, in a dependent manner of cell density. In the presence of 2 mu M (MeOPhSe)(2) it was observed an inhibition of 87, 72, 69 and 56 % in C. albicans growth, using cell densities of 10(4), 10(5), 10(6) and 10(7) cells/mL, respectively. C. albicans growth was inhibited >90 % in the presence of 10 mu M (MeOPhSe) 2 in all cell densities used. Also, (MeOPhSe)(2) was found to be able to decrease the viability of the biofilm produced by C. albicans at different stages of development. This effect was more pronounced in early biofilms as compared to mature biofilms. Biofilms forming at 6 and 12 hours was inhibited similar to 80% in the presence of 10 mu M (MeOPhSe)(2). However, mature biofilms presented an inhibition of similar to 40 % in the presence of 10 mu M (MeOPhSe)(2). The analyses of the structure of the biofilm have shown a significant reduction in the number of both yeast and filamentous form after treatment with (MeOPhSe)(2). In addition, the organochalcogen compound (MeOPhSe)(2) did not modify the viability of Fibroblastic cells. Conclusion: Taken together, these results demonstrated the potential of the organochalcogen compound (MeOPhSe)(2) as a promising antifungal therapy.
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Candida albicans,biofilm formation,biofilm viability,(MeOPhSe)(2),antifungal therapy,organochalcogen compounds
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