Inhibition of Inositol Phosphorylceramide Synthase by Aureobasidin A in Candida and Aspergillus Species

doi:10.1128/AAC.44.3.651-653.2000

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Antimicrobial Agents and Chemotherapy, March 2000, p. 651-653, Vol. 44, No. 3
0066-4804/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.

Inhibition of Inositol Phosphorylceramide Synthase by Aureobasidin A in Candida and Aspergillus Species

Wenyan Zhong, Matthew W. Jeffries, and Nafsika H. Georgopapadakou^*

Experimental Station, DuPont Pharmaceuticals Company, Wilmington, Delaware 19880-0400

Received 25 October 1999/Returned for modification 30 November 1999/Accepted 20 December 1999

Inositol phosphorylceramide (IPC) synthase is an enzyme common to fungi and plants that catalyzes the transfer of phosphoinositolfrom phosphatidylinositol to ceramide to form IPC. The reactionis a key step in fungal sphingolipid biosynthesis and the targetof the antibiotics galbonolide A, aureobasidin A, and khafrefungin.As a first step toward understanding the antifungal spectrum ofIPC synthase inhibitors, we examined the sensitivity of IPC synthaseto aureobasidin A in membrane preparations of Candida species(Candida albicans, C. glabrata, C. tropicalis, C. parapsilosis,and C. krusei) and Aspergillus species (Aspergillus fumigatus,A. flavus, A. niger, and A. terreus). As expected, preparationsfrom the five Candida species, all exquisitely susceptible toaureobasidin A (MICs, <2 µg/ml), had IPC synthase activity (specificactivity, 50 to 400 pmol/min/mg of protein) sensitive to aureobasidinA (50% inhibitory concentrations [IC₅₀s], 2 to 4 ng/ml). Surprisingly,preparations from the four Aspergillus species, including A. fumigatusand A. flavus, which are intrinsically resistant to aureobasidinA (MICs, >50 µg/ml), had IPC synthase activity (specific activity,1 to 3 pmol/min/mg of protein) also sensitive to aureobasidinA (IC₅₀s, 3 to 5 ng/ml). The mammalian multidrug resistance modulatorsverapamil, chlorpromazine, and trifluoperazine lowered the MICof aureobasidin A for A. fumigatus from >50 µg/ml to 2 to 3 µg/ml,suggesting that the resistance of this major fungal pathogen isthe result of increasedefflux.

^* Corresponding author. Mailing address: DuPont Pharmaceuticals Company, Experimental Station, E400/3456A, P.O. Box 80400, Wilmington,DE 19880-0400. Phone: (302) 695-8525. Fax: (302) 695-7407. E-mail:nafsika.h.dakou{at}dupontpharma.com.

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