Anti‐Candida activity and in vitro toxicity screening of antifungals complexed with β‐cyclodextrin

Author:

Moraes Gustavo Simão1ORCID,Tozetto Nathaly Mayer1,Pedroso Thaynara Aparecida Alves1,de Mattos Marcela Alves1,Urban Amanda Migliorini2,Paludo Katia Sabrina3,dos Santos Fábio André1,Neppelenbroek Karin Hermana4,Urban Vanessa Migliorini1

Affiliation:

1. Department of Dentistry State University of Ponta Grossa Ponta Grossa Brazil

2. Department of Pharmaceutical Sciences Federal University of Parana Curitiba Brazil

3. Department of Structural, Molecular, and Genetic Biology, State University of Ponta Grossa Ponta Grossa Brazil

4. Department of Prosthodontics and Periodontics, Bauru School of Dentistry University of São Paulo Bauru Brazil

Abstract

AbstractThe emergence of resistant fungal species and the toxicity of currently available antifungal drugs are relevant issues that require special consideration. Cyclodextrins inclusion complexes could optimize the antimicrobial activity of such drugs and create a controlled release system with few side effects. This study aimed to assess the in vitro toxicity and antifungal effectiveness of nystatin (Nys) and chlorhexidine (Chx) complexed or not with β‐cyclodextrin (βCD). First, a drug toxicity screening was performed through the Artemia salina bioassay. Then, the minimum inhibitory concentrations (MICs) against Candida albicans were determined with the broth microdilution test. After MICs determination, the cytotoxicity of the drugs was evaluated through the methyl‐thiazolyl‐tetrazolium (MTT) and neutral red (NR) assays and through cell morphology analysis. The PROBIT analysis was used to determine the median lethal concentration (LC50), and the cell viability values were submitted to one‐way analysis of variance(ANOVA)/Tukey (α = 0.05). Overall, the βCD‐complexed antifungals were less toxic against A. salina than their raw forms, suggesting that inclusion complexes can reduce the toxicity of drugs. The MICs obtained were as follows: Nys 0.5 mg/L; Nys:βCD 4 mg/L; Chx 4 mg/L; and Chx:βCD 8 mg/L. Chx showed significant cytotoxicity (MTT: 12.9 ± 9.6%; NR: 10.6 ± 12.5%) and promoted important morphological changes. Cells exposed to the other drugs showed viability above 70% with no cellular damage. These results suggest that antifungals complexed with βCD might be a biocompatible option for the treatment of Candida‐related infections.

Funder

Coordenação de Aperfeiçoamento de Pessoal de Nível Superior

Fundação de Amparo à Pesquisa do Estado de São Paulo

Publisher

Wiley

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