Gallic acid triphenylphosphonium derivatives TPP+-C10 and TPP+-C12 inhibit mitochondrial function in Candida albicans exerting antifungal and antibiofilm effects

Author:

Valderrama Victoria1,Sánchez Paula1,Delso Macarena1,Díaz-Dosque Mario12,Escobar Alejandro3,Budini Mauricio4,Catalán Mabel5,Vivar Raúl5,López-Muñoz Rodrigo6,Jara José A1ORCID,Molina-Berríos Alfredo1ORCID

Affiliation:

1. Laboratory of Applied Pharmacology for the Development of Anticancer and Antifungal Drugs, Institute for Research in Dental Sciences (ICOD), Faculty of Dentistry, University of Chile , Santiago, 8380544 , Chile

2. Laboratory of Nanobiomaterials, Institute for Research in Dental Sciences (ICOD), Faculty of Dentistry, University of Chile , Santiago, 8380544 , Chile

3. Laboratory of Cellular Biology, Institute for Research in Dental Sciences (ICOD), Faculty of Dentistry, University of Chile , Santiago, 8380544 , Chile

4. Cellular and Molecular Pathology Laboratory, Institute for Research in Dental Sciences (ICOD), Faculty of Dentistry, University of Chile , Santiago, 8380544 , Chile

5. Clinical and Molecular Pharmacology Program, Institute of Biomedical Sciences (ICBM), Faculty of Medicine, University of Chile , Santiago, 8380453 , Chile

6. Instituto de Farmacología y Morfofisiología, Facultad de Ciencias Veterinarias, Universidad Austral de Chile , Valdivia, 5110566 , Chile

Abstract

Abstract Aims To evaluate the antifungal and antibiofilm activity of gallic acid derivatives TPP+-C10 and TPP+-C12 and their effects on mitochondrial function on two Candida albicans reference strains (ATCC 90029 and ATCC 10231). Methods and results First, we determined minimal inhibitory concentration (MIC) using a microdilution assay. Both compounds exerted antifungal effects, and their MICs ranged from 3.9 to 13 µM, with no statistically significant differences between them (P > 0.05, t-test). These concentrations served as references for following assays. Subsequently, we measured oxygen consumption with a Clark electrode. Our observations revealed that both drugs inhibited oxygen consumption in both strains with TPP+-C12 exerting a more pronounced inhibitory effect. We then employed flow cytometry with TMRE as a probe to assess mitochondrial membrane potential. For each strain assayed, the compounds induced a decay in transmembrane potential by 75%–90% compared to the control condition (P < 0.05, ANOVA). Then, we measured ATP levels using a commercial kit. TPP+-C12 showed a 50% decrease of ATP content (P < 0.05 ANOVA), while TPP+-C10 exhibited a less pronounced effect. Finally, we assessed the antibiofilm effect using the MTT reduction assay. Both compounds were effective, but TPP+-C12 displayed a greater potency, requiring a lower concentration to inhibit 50% of biofilms viability (P < 0.05, t-test). Conclusions Derivatives of gallic acid linked to a TPP+ group exert antifungal and antibiofilm activity through impairment of mitochondrial function in C. albicans.

Funder

Dirección de Investigación de la Facultad de Odontología de la Universidad de Chile

Agencia Nacional de investigación y Desarrollo

Publisher

Oxford University Press (OUP)

Subject

Applied Microbiology and Biotechnology,General Medicine,Biotechnology

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