Literature DB >> 22733749

Polyene antibiotic that inhibits membrane transport proteins.

Yvonne Maria te Welscher1, Martin Richard van Leeuwen, Ben de Kruijff, Jan Dijksterhuis, Eefjan Breukink.   

Abstract

The limited therapeutic arsenal and the increase in reports of fungal resistance to multiple antifungal agents have made fungal infections a major therapeutic challenge. The polyene antibiotics are the only group of antifungal antibiotics that directly target the plasma membrane via a specific interaction with the main fungal sterol, ergosterol, often resulting in membrane permeabilization. In contrast to other polyene antibiotics that form pores in the membrane, the mode of action of natamycin has remained obscure but is not related to membrane permeabilization. Here, we demonstrate that natamycin inhibits growth of yeasts and fungi via the immediate inhibition of amino acid and glucose transport across the plasma membrane. This is attributable to ergosterol-specific and reversible inhibition of membrane transport proteins. It is proposed that ergosterol-dependent inhibition of membrane proteins is a general mode of action of all the polyene antibiotics, of which some have been shown additionally to permeabilize the plasma membrane. Our results imply that sterol-protein interactions are fundamentally important for protein function even for those proteins that are not known to reside in sterol-rich domains.

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Year:  2012        PMID: 22733749      PMCID: PMC3396478          DOI: 10.1073/pnas.1203375109

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  34 in total

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8.  Natamycin blocks fungal growth by binding specifically to ergosterol without permeabilizing the membrane.

Authors:  Yvonne M te Welscher; Hendrik H ten Napel; Miriam Masià Balagué; Cleiton M Souza; Howard Riezman; Ben de Kruijff; Eefjan Breukink
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4.  Ethylzingerone, a Novel Compound with Antifungal Activity.

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Review 7.  Targeting Candida albicans filamentation for antifungal drug development.

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Review 8.  Biosynthesis and pathway engineering of antifungal polyene macrolides in actinomycetes.

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9.  Sterol Sponge Mechanism Is Conserved for Glycosylated Polyene Macrolides.

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