The effects of azole and polyene antifungals on the plasma membrane enzymes ofCandida albicans
- 1 January 1987
- journal article
- research article
- Published by Oxford University Press (OUP) in Medical Mycology
- Vol. 25 (6) , 403-413
- https://doi.org/10.1080/02681218780000491
Abstract
The two clinically important classes of antimycotic drugs, the polyenes and azoles, act on the plasma membrane of the cell. The primary modes of action are believed to be through interaction with sterols (polyenes) and alteration in sterol composition of the membrane (azoles). In this report we show that, at growth inhibitory concentrations, the polyenes (nystatin and amphotericin) and azoles (miconazole and ketoconazole) also inhibit plasma membrane enzymes. There was extensive (> 75%) inhibition of the Candida albicans plasma membrane enzymes. ATPase, glucan synthase, adenyl cyclase and 5''-nucleotidase, when assayed in situ. The antifungals papulacandin and echinocandin, which inhibit glucan synthesis, also inhibited plasma membrane enzymes in situ: glucan synthase (> 90%), 5''-nucleotidase (> 80%) and ATPase (70-80%). Purified plasma membrane was prepared from yeast cells of C. albicans by two different techniques: concanavalin A stabilization and coating of spheroplasts with silica microbeads. In the purified plasma membrane vesicles prepared from concanavalin A the adenyl cyclase and phosphodiesterase were extensively (> 90%) inhibited by the three different classes of antifungal drugs: variable inhibition was observed with ATPase (70-100%). The 3'',5''-cyclic phosphodiesterase of the plasma membrane purified by the microbeads method was almost completely inhibited by all of the antifungals tested and there was a partial inhibition of ATPase (20-85%) and adenyl cyclase (30-90%).This publication has 37 references indexed in Scilit:
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