Potential Activity of Micafungin and Amphotericin B Co-Encapsulated in Nanoemulsion against Systemic Candida auris Infection in a Mice Model

Author:

Marena Gabriel Davi12ORCID,Carvalho Gabriela Corrêa12ORCID,Ruiz-Gaitán Alba34ORCID,Onisto Giovana Scaramal1,Bugalho Beatriz Chiari Manzini1,Genezini Letícia Maria Valente1,Santos Maíra Oliveira Dos1,Blanco Ana Lígia1,Chorilli Marlus2ORCID,Bauab Tais Maria1

Affiliation:

1. Department of Biological Sciences, School of Pharmaceutical Sciences, São Paulo State University (UNESP), Araraquara 14800-903, Brazil

2. Department of Drug and Medicines, School of Pharmaceutical Sciences, São Paulo State University (UNESP), Araraquara 14800-903, Brazil

3. Severe Infection Research Group, Health Research Institute La Fe, 46026 Valencia, Spain

4. Department of Medical Microbiology, University and Polytechnic La Fe Hospital, 46026 Valencia, Spain

Abstract

The Candida auris species is a multidrug-resistant yeast capable of causing systemic and lethal infections. Its virulence and increase in outbreaks are a global concern, especially in hospitals where outbreaks are more recurrent. In many cases, monotherapy is not effective, and drug combinations are opted for. However, resistance to antifungals has increased over the years. In view of this, nanoemulsions (NEs) may represent a nanotechnology strategy in the development of new therapeutic alternatives. Therefore, this study developed a co-encapsulated nanoemulsion with amphotericin B (AmB) and micafungin (MICA) (NEMA) for the control of infections caused by C. auris. NEs were developed in previous studies. Briefly, the NEs were composed of a mixture of 10% sunflower oil and cholesterol as the oil phase (5:1), 10% Polyoxyethylene (20) cetyl ether (Brij® 58) and soy phosphatidylcholine as surfactant/co-surfactant (2:1), and 80% PBS as the aqueous phase. The in vivo assay used BALB/c mice weighing between 25 and 28 g that were immunosuppressed (CEUA/FCF/CAr n° 29/2021) and infected with Candida auris CDC B11903. The in vivo results show the surprising potentiate of the antifungal activity of the co-encapsulated drugs in NE, preventing yeast from causing infection in the lung and thymus. Biochemical assays showed a higher concentration of liver and kidney enzymes under treatment with AmB and MICAmB. In conclusion, this combination of drugs to combat the infection caused by C. auris can be considered an efficient therapeutic option, and nanoemulsions contribute to therapeutic potentiate, proving to be a promising new alternative.

Funder

São Paulo Research Foundation—FAPESP

Publisher

MDPI AG

Reference29 articles.

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2. (2024, January 20). CDC Tracking Candida auris: Candida auris Fungal Diseases CDC, Available online: https://www.cdc.gov/fungal/candida-auris/index.html.

3. Candida auris: A Review of the Literature;Taori;Clin. Microbiol. Rev.,2018

4. Simultaneous Emergence of Multidrug-Resistant Candida auris on 3 Continents Confirmed by Whole-Genome Sequencing and Epidemiological Analyses;Lockhart;Clin. Infect. Dis.,2017

5. Role of Microbiota in the Skin Colonization of Candida auris;Tharp;mSphere,2023

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