Mechanism of Fluconazole Resistance in Candida krusei

Author:

Orozco Alison S.1,Higginbotham Lindsey M.1,Hitchcock Christopher A.2,Parkinson Tanya2,Falconer Derek2,Ibrahim Ashraf S.1,Ghannoum Mahmoud A.13,Filler Scott G.13

Affiliation:

1. St. John’s Cardiovascular Research Center, Division of Infectious Diseases, Harbor-UCLA Research and Education Institute, Torrance, California 905021;

2. Pfizer Central Research, Sandwich, Kent, United Kingdom2; and the

3. UCLA School of Medicine, Los Angeles, California 900243

Abstract

ABSTRACT The mechanisms of fluconazole resistance in three clinical isolates of Candida krusei were investigated. Analysis of sterols of organisms grown in the absence and presence of fluconazole demonstrated that the predominant sterol of C. krusei is ergosterol and that fluconazole inhibits 14α-demethylase in this organism. The 14α-demethylase activity in cell extracts of C. krusei was 16- to 46-fold more resistant to inhibition by fluconazole than was 14α-demethylase activity in cell extracts of two fluconazole-susceptible strains of Candida albicans . Comparing the carbon monoxide difference spectra of microsomes from C. krusei with those of microsomes from C. albicans indicated that the total cytochrome P-450 content of C. krusei is similar to that of C. albicans . The Soret absorption maximum in these spectra was located at 448 nm for C. krusei and at 450 nm for C. albicans . Finally, the fluconazole accumulation of two of the C. krusei isolates was similar to if not greater than that of C. albicans . Thus, there are significant qualitative differences between the 14α-demethylase of C. albicans and C. krusei . In addition, fluconazole resistance in these strains of C. krusei appears to be mediated predominantly by a reduced susceptibility of 14α-demethylase to inhibition by this drug.

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Pharmacology (medical),Pharmacology

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