Enhancement of the antifungal activity of some antimycotics by farnesol and reduction of Candida albicans pathogenicity in a quail model experiment

BACKGROUND AND AIM: Clinical strains of microorganisms, including pathogenic yeast-like fungi (YLF), are resistant to currently used antifungal agents. Thus, it is relevant to study the combinations of existing antimicrobial drugs and a medicinal extract of plant origin (farnesol). In previous studi...

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Autores principales: Sachivkina, Nadezhda, Senyagin, Alexander, Podoprigora, Irina, Vasilieva, Elena, Kuznetsova, Olga, Karamyan, Arfenia, Ibragimova, Alfia, Zhabo, Natalia, Molchanova, Maria
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Veterinary World 2022
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9178579/
https://www.ncbi.nlm.nih.gov/pubmed/35698495
http://dx.doi.org/10.14202/vetworld.2022.848-854
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author Sachivkina, Nadezhda
Senyagin, Alexander
Podoprigora, Irina
Vasilieva, Elena
Kuznetsova, Olga
Karamyan, Arfenia
Ibragimova, Alfia
Zhabo, Natalia
Molchanova, Maria
author_facet Sachivkina, Nadezhda
Senyagin, Alexander
Podoprigora, Irina
Vasilieva, Elena
Kuznetsova, Olga
Karamyan, Arfenia
Ibragimova, Alfia
Zhabo, Natalia
Molchanova, Maria
author_sort Sachivkina, Nadezhda
collection PubMed
description BACKGROUND AND AIM: Clinical strains of microorganisms, including pathogenic yeast-like fungi (YLF), are resistant to currently used antifungal agents. Thus, it is relevant to study the combinations of existing antimicrobial drugs and a medicinal extract of plant origin (farnesol). In previous studies, farnesol showed a relatively strong anti-biofilm effect against Candida albicans. This study aimed to determine how much the resistance profile of non-biofilm microorganisms can change. MATERIALS AND METHODS: Six clinical isolates of C. albicans and one reference strain were used to study the interaction of farnesol with the most used antimycotics. To determine the sensitivity of YLF to antimycotic drugs, such as nystatin (50 μg), amphotericin B (10 μg), ketoconazole (10 μg), clotrimazole (10 μg), voriconazole (10 μg), fluconazole (25 μg), miconazole (10 μg), and intraconazole (10 μg), the classic disk diffusion method was used. In the second stage, one of the six strains was used to simulate candidiasis of the gastrointestinal tract in an in vivo quail model. As an unusual experimental design, this study investigated the effects of pretreated C. albicans in quails, not the in vivo pathogenicity of C. albicans, after treatment with farnesol. RESULTS: The resistance profiles of Candida strains did not improve with farnesol in all strains. All concentrations of farnesol (100, 50, and 25 μM) demonstrated a fungistatic effect (i.e., an increase in drug sensitivity) in 23 of 56 (7×8) cases (41%). The remaining 54% demonstrated no changes in the resistance to antifungal drugs or deterioration of the indicators in rare cases (5%). At 100 μM farnesol, sensitivity improved in 33 of 56 cases (59%). Candidiasis or the severity of clinical disease of the quail digestive tract developed to a lesser extent if fungi were treated with farnesol. CONCLUSION: Farnesol does not always show a positive result on single cells without biofilm in the laboratory. However, in a biofilm or an in vivo model with biofilms, farnesol can be considered a new antimycotic drug or an additive to existing antimycotics.
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spelling pubmed-91785792022-06-12 Enhancement of the antifungal activity of some antimycotics by farnesol and reduction of Candida albicans pathogenicity in a quail model experiment Sachivkina, Nadezhda Senyagin, Alexander Podoprigora, Irina Vasilieva, Elena Kuznetsova, Olga Karamyan, Arfenia Ibragimova, Alfia Zhabo, Natalia Molchanova, Maria Vet World Research Article BACKGROUND AND AIM: Clinical strains of microorganisms, including pathogenic yeast-like fungi (YLF), are resistant to currently used antifungal agents. Thus, it is relevant to study the combinations of existing antimicrobial drugs and a medicinal extract of plant origin (farnesol). In previous studies, farnesol showed a relatively strong anti-biofilm effect against Candida albicans. This study aimed to determine how much the resistance profile of non-biofilm microorganisms can change. MATERIALS AND METHODS: Six clinical isolates of C. albicans and one reference strain were used to study the interaction of farnesol with the most used antimycotics. To determine the sensitivity of YLF to antimycotic drugs, such as nystatin (50 μg), amphotericin B (10 μg), ketoconazole (10 μg), clotrimazole (10 μg), voriconazole (10 μg), fluconazole (25 μg), miconazole (10 μg), and intraconazole (10 μg), the classic disk diffusion method was used. In the second stage, one of the six strains was used to simulate candidiasis of the gastrointestinal tract in an in vivo quail model. As an unusual experimental design, this study investigated the effects of pretreated C. albicans in quails, not the in vivo pathogenicity of C. albicans, after treatment with farnesol. RESULTS: The resistance profiles of Candida strains did not improve with farnesol in all strains. All concentrations of farnesol (100, 50, and 25 μM) demonstrated a fungistatic effect (i.e., an increase in drug sensitivity) in 23 of 56 (7×8) cases (41%). The remaining 54% demonstrated no changes in the resistance to antifungal drugs or deterioration of the indicators in rare cases (5%). At 100 μM farnesol, sensitivity improved in 33 of 56 cases (59%). Candidiasis or the severity of clinical disease of the quail digestive tract developed to a lesser extent if fungi were treated with farnesol. CONCLUSION: Farnesol does not always show a positive result on single cells without biofilm in the laboratory. However, in a biofilm or an in vivo model with biofilms, farnesol can be considered a new antimycotic drug or an additive to existing antimycotics. Veterinary World 2022-04 2022-04-08 /pmc/articles/PMC9178579/ /pubmed/35698495 http://dx.doi.org/10.14202/vetworld.2022.848-854 Text en Copyright: © Sachivkina, et al. https://creativecommons.org/licenses/by/4.0/Open Access. This article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) ), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/ (https://creativecommons.org/publicdomain/zero/1.0/) ) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research Article
Sachivkina, Nadezhda
Senyagin, Alexander
Podoprigora, Irina
Vasilieva, Elena
Kuznetsova, Olga
Karamyan, Arfenia
Ibragimova, Alfia
Zhabo, Natalia
Molchanova, Maria
Enhancement of the antifungal activity of some antimycotics by farnesol and reduction of Candida albicans pathogenicity in a quail model experiment
title Enhancement of the antifungal activity of some antimycotics by farnesol and reduction of Candida albicans pathogenicity in a quail model experiment
title_full Enhancement of the antifungal activity of some antimycotics by farnesol and reduction of Candida albicans pathogenicity in a quail model experiment
title_fullStr Enhancement of the antifungal activity of some antimycotics by farnesol and reduction of Candida albicans pathogenicity in a quail model experiment
title_full_unstemmed Enhancement of the antifungal activity of some antimycotics by farnesol and reduction of Candida albicans pathogenicity in a quail model experiment
title_short Enhancement of the antifungal activity of some antimycotics by farnesol and reduction of Candida albicans pathogenicity in a quail model experiment
title_sort enhancement of the antifungal activity of some antimycotics by farnesol and reduction of candida albicans pathogenicity in a quail model experiment
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9178579/
https://www.ncbi.nlm.nih.gov/pubmed/35698495
http://dx.doi.org/10.14202/vetworld.2022.848-854
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