Glutathione metabolism in Candida albicans resistant strains to fluconazole and micafungin

Glutathione metabolism in Candida albicans resistant strains to fluconazole and micafungin

Currently available therapies for candidiasis are based on antifungal drugs belonging to azole and echinocandin families that interfere with different aspects of fungal metabolism. These drugs, beyond their specific effects, elicit also a cellular stress including an unbalance of redox state that is...

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Veröffentlicht in:PloS one 2014-06, Vol.9 (6), p.e98387
Hauptverfasser: Maras, Bruno, Angiolella, Letizia, Mignogna, Giuseppina, Vavala, Elisabetta, Macone, Alberto, Colone, Marisa, Pitari, Giuseppina, Stringaro, Annarita, Dupré, Silvestro, Palamara, Anna Teresa
Format: Artikel
Sprache:eng
Schlagworte:
Analysis
Antifungal agents
Antifungal Agents - pharmacology
Antioxidants
Biology and Life Sciences
Candida albicans
Candida albicans - drug effects
Candida albicans - metabolism
Candida glabrata
Candidiasis
Candidiasis - drug therapy
Candidiasis - microbiology
Drug metabolism
Drug resistance
Drug Resistance, Fungal - physiology
Drugs
Echinocandins
Echinocandins - pharmacology
Enzymes
Fluconazole
Fluconazole - pharmacology
Fungicides
Glutathione
Glutathione - metabolism
Kinases
Ligases
Lipopeptides - pharmacology
Metabolism
Metabolites
Micafungin
Microbial Sensitivity Tests
Mycoses
Oxidation-Reduction
Oxidative stress
Physiological aspects
Proteins
Redox properties
Rodents
Stress response
Substance abuse treatment
Thiols
Transcription factors
Yeast
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Zusammenfassung:Currently available therapies for candidiasis are based on antifungal drugs belonging to azole and echinocandin families that interfere with different aspects of fungal metabolism. These drugs, beyond their specific effects, elicit also a cellular stress including an unbalance of redox state that is counteracted not only utilizing antioxidant species but also increasing the outcome export by transporters to detoxify the internal environment. These cellular actions are both based on the cytosolic concentration of reduced glutathione (GSH). In this paper we investigated the effects of two antifungal drugs fluconazole and micafungin on the redox state of the cell in C. albicans to understand if the resistance to these drugs is accompanied by variation of glutathione metabolism. Analyses of resistant strains showed a marked difference in glutathione contents in strains resistant to fluconazole (CO23RFLC) or micafungin (CO23RFK). In CO23RFLC, the total amount of glutathione was more than doubled with respect to CO23RFK thanks to the increased activity of γ-glutamilcysteine synthetase, the key enzyme involved in GSH synthesis. We demonstrated that the GSH increase in CO23RFLC conferred to this strain a clear advantage in counteracting oxidative toxic agents while assignment of other roles, such as a more efficient elimination of the drug from the cell, should be considered more speculative. As far as MCFG resistance is concerned, from our data a role of glutathione metabolism in supporting this condition is not evident. Overall our data indicate that glutathione metabolism is differently affected in the two resistant strains and that glutathione system may play an important role in the global organization of C.albicans cells for resistance to fluconazole. Such scenario may pave the way to hypothesize the use of oxidant drugs or inhibitors able to deplete reduced glutathione level as a novel approach, for counteracting the resistance to this specific antifungal drug.
ISSN:1932-6203
1932-6203
DOI:10.1371/journal.pone.0098387