Synthesis and biological activity of tripeptidyl polyoxins as antifungal agents

Author:

Naider F,Shenbagamurthi P,Steinfeld A S,Smith H A,Boney C,Becker J M

Abstract

Three tripeptidyl polyoxins were synthesized and found to inhibit Candida albicans. Compared with the naturally occurring polyoxin D, the three synthetic polyoxins had little effect on chitin synthetase when assayed with a C. albicans membrane preparation. However, all the compounds inhibited growth, affected cell morphology in a manner similar to that of polyoxin D, and were hydrolyzed by cell extracts of C. albicans. Hydrolysis did not occur extracellularly, and at least one of the synthetic polyoxins, leucyl-norleucyl-uracil polyoxin C, inhibited peptide uptake, suggesting entrance into the cell via the peptide transport system. Thus, the intact tripeptidyl polyoxins are inactive prodrugs that are converted to active moieties by cellular enzymes.

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Pharmacology (medical),Pharmacology

Reference14 articles.

1. Polyoxin D inhibits growth of zoopathogenic fungi;Becker J. M.;Antimicrob. Agents Chemother.,1983

2. Becker J. M. and F. Naider. 1980. Transport and utilization of peptides by yeast. p. 257-280. In J. W. Payne (ed.) Microorganisms and nitrogen sources. John Wiley & Sons Inc. New York.

3. Effect of polyoxin D on chitin synthetase and septum formation in Saccharomyces cerevisiae;Bowers B.;J. Bacteriol.,1974

4. Regulation of chitin synthesis during germ-tube formation in Candida albicans;Chiew Y.;Arch. Microbiol.,1980

5. Synthesis of the basic nucleotide skeleton of the polyoxin complex;Damadoran N. P.;J. Am. Chem. Soc.,1971

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