Abstract

The respiration, membrane potential (Deltapsi), and oxidative phosphorylation of mitochondria in situ were determined in spheroplasts obtained from Candida albicans control strain ATCC 90028 by lyticase treatment. Mitochondria in situ were able to phosphorylate externally added ADP (200 microM) in the presence of 0.05% BSA. Mitochondria in situ generated and sustained stable mitochondrial Deltapsi respiring on 5 mM NAD-linked substrates, 5 mM succinate, or 100 microM N,N,N',N'-tetramethyl-p-phenylenediamine dihydrochloride plus 1 mM ascorbate. Rotenone (4 microM) inhibited respiration by 30% and 2 micro M antimycin A or myxothiazole and 1 mM cyanide inhibited it by 85%. Cyanide-insensitive respiration was partially blocked by 2 mM benzohydroxamic acid, suggesting the presence of an alternative oxidase. Candida albicans mitochondria in situ presented a carboxyatractyloside-insensitive increase of Deltapsi induced by 5 mM ATP and 0.5% BSA, and Deltapsi decrease induced by 10 microM linoleic acid, both suggesting the existence of an uncoupling protein. The presence of this protein was subsequently confirmed by immunodetection and respiration experiments with isolated mitochondria. In conclusion, Candida albicans ATCC 90028 possesses an alternative electron transfer chain and alternative oxidase, both absent in animal cells. These pathways can be exceptional targets for the design of new chemotherapeutic agents. Blockage of these respiratory pathways together with inhibition of the uncoupling protein (another potential target for drug design) could lead to increased production of reactive oxygen species, dysfunction of Candida mitochondria, and possibly to oxidative cell death.

Highlights

  • Candidiases are common infections of the skin, oral cavity, esophagus, gastrointestinal tract, vagina, and vascular system, and have become a major cause of mortality in immunocompromised patients, including those with AIDS [1,2,3] or debilitated in some other way [4]

  • (57%), C. tropicalis (13%), C. glabrata (10%), C. parapsilosis (6%), and C. krusei (3.4%), and 10.6% belonged to other yeast genera [5]

  • Most antifungal drugs react with ergosterol or inhibit its production [6]; there is an alarming increase in resistance to antifungal agents [3,7]

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Summary

Introduction

Candidiases are common infections of the skin, oral cavity, esophagus, gastrointestinal tract, vagina, and vascular system, and have become a major cause of mortality in immunocompromised patients, including those with AIDS [1,2,3] or debilitated in some other way [4]. We demonstrated that spheroplasts obtained from cultures of C. albicans in the middle of their exponential phase of growth possess intact mitochondria able to phosphorylate ADP and an uncoupling protein (CaUCP) homologous to the previously described C. parapsilosis UCP (CpUCP) [28].

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