Literature DB >> 15616276

Surface-active fungicidal D-peptide inhibitors of the plasma membrane proton pump that block azole resistance.

Brian C Monk1, Kyoko Niimi, Susan Lin, Allison Knight, Thomas B Kardos, Richard D Cannon, Rekha Parshot, Amanda King, David Lun, David R K Harding.   

Abstract

A 1.8-million-member D-octapeptide combinatorial library was constructed in which each member comprised a diversity-containing N-terminal pentapeptide and a C-terminal amidated triarginine motif. The C-terminal motif concentrated the library members at the fungal cell surface. A primary screen for inhibitors of Saccharomyces cerevisiae and Candida albicans growth, together with an in vitro secondary screen with the S. cerevisiae plasma membrane ATPase (Pma1p) as a target, identified the antifungal D-octapeptide BM0 (D-NH(2)-RFWWFRRR-CONH(2)). Optimization of BM0 led to the construction of BM2 (D-NH(2)-RRRFWWFRRR-CONH(2)), which had broad-spectrum fungicidal activity against S. cerevisiae, Candida species, and Cryptococcus neoformans; bound strongly to the surfaces of fungal cells; inhibited the physiological activity of Pma1p; and appeared to target Pma1p, with 50% inhibitory concentrations in the range of 0.5 to 2.5 microM. At sub-MICs (<5 microM), BM2 chemosensitized to fluconazole (FLC) S. cerevisiae strains functionally hyperexpressing fungal lanosterol 14alpha-demethylase and resistance-conferring transporters of azole drugs. BM2 chemosensitized to FLC some FLC-resistant clinical isolates of C. albicans and C. dubliniensis and chemosensitized to itraconazole clinical isolates of C. krusei that are intrinsically resistant to FLC. The growth-inhibitory concentrations of BM2 did not cause fungal cell permeabilization, significant hemolysis of red blood cells, or the death of cultured HEp-2 epithelial cells. BM2 represents a novel class of broad-spectrum, surface-active, Pma1p-targeting fungicides which increases the potencies of azole drugs and circumvents azole resistance.

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Year:  2005        PMID: 15616276      PMCID: PMC538910          DOI: 10.1128/AAC.49.1.57-70.2005

Source DB:  PubMed          Journal:  Antimicrob Agents Chemother        ISSN: 0066-4804            Impact factor:   5.191


  41 in total

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Journal:  Antimicrob Agents Chemother       Date:  1999-01       Impact factor: 5.191

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8.  The effect of charge increase on the specificity and activity of a short antimicrobial peptide.

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  21 in total

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2.  Studies on the mode of action of the antifungal hexapeptide PAF26.

Authors:  Alberto Muñoz; Belén López-García; Jose F Marcos
Journal:  Antimicrob Agents Chemother       Date:  2006-11       Impact factor: 5.191

3.  Overexpression of Candida albicans CDR1, CDR2, or MDR1 does not produce significant changes in echinocandin susceptibility.

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Journal:  Antimicrob Agents Chemother       Date:  2006-04       Impact factor: 5.191

4.  Involvement of PDK1, PKC and TOR signalling pathways in basal fluconazole tolerance in Cryptococcus neoformans.

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5.  A genomic approach highlights common and diverse effects and determinants of susceptibility on the yeast Saccharomyces cerevisiae exposed to distinct antimicrobial peptides.

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Journal:  BMC Microbiol       Date:  2010-11-15       Impact factor: 3.605

6.  Antifungal Mechanism of Action of Lactoferrin: Identification of H+-ATPase (P3A-Type) as a New Apoptotic-Cell Membrane Receptor.

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7.  Heterologous expression of Candida albicans Pma1p in Saccharomyces cerevisiae.

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8.  Characterization of three classes of membrane proteins involved in fungal azole resistance by functional hyperexpression in Saccharomyces cerevisiae.

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Review 9.  Efflux-mediated antifungal drug resistance.

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Review 10.  Cryptococcosis: epidemiology, fungal resistance, and new alternatives for treatment.

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