Literature DB >> 18725634

Inhibition of the fungal fatty acid synthase type I multienzyme complex.

Patrik Johansson1, Birgit Wiltschi, Preeti Kumari, Brigitte Kessler, Clemens Vonrhein, Janet Vonck, Dieter Oesterhelt, Martin Grininger.   

Abstract

Fatty acids are among the major building blocks of living cells, making lipid biosynthesis a potent target for compounds with antibiotic or antineoplastic properties. We present the crystal structure of the 2.6-MDa Saccharomyces cerevisiae fatty acid synthase (FAS) multienzyme in complex with the antibiotic cerulenin, representing, to our knowledge, the first structure of an inhibited fatty acid megasynthase. Cerulenin attacks the FAS ketoacyl synthase (KS) domain, forming a covalent bond to the active site cysteine C1305. The inhibitor binding causes two significant conformational changes of the enzyme. First, phenylalanine F1646, shielding the active site, flips and allows access to the nucleophilic cysteine. Second, methionine M1251, placed in the center of the acyl-binding tunnel, rotates and unlocks the inner part of the fatty acid binding cavity. The importance of the rotational movement of the gatekeeping M1251 side chain is reflected by the cerulenin resistance and the changed product spectrum reported for S. cerevisiae strains mutated in the adjacent glycine G1250. Platensimycin and thiolactomycin are two other potent inhibitors of KSs. However, in contrast to cerulenin, they show selectivity toward the prokaryotic FAS system. Because the flipped F1646 characterizes the catalytic state accessible for platensimycin and thiolactomycin binding, we superimposed structures of inhibited bacterial enzymes onto the S. cerevisiae FAS model. Although almost all side chains involved in inhibitor binding are conserved in the FAS multienzyme, a different conformation of the loop K1413-K1423 of the KS domain might explain the observed low antifungal properties of platensimycin and thiolactomycin.

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Year:  2008        PMID: 18725634      PMCID: PMC2529065          DOI: 10.1073/pnas.0805827105

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


  48 in total

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Journal:  Eur J Biochem       Date:  1993-01-15

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Journal:  J Bacteriol       Date:  1993-06       Impact factor: 3.490

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  29 in total

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Review 2.  The architectures of iterative type I PKS and FAS.

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4.  Direct structural insight into the substrate-shuttling mechanism of yeast fatty acid synthase by electron cryomicroscopy.

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6.  Triclosan inhibition of mycobacterial InhA in Saccharomyces cerevisiae: yeast mitochondria as a novel platform for in vivo antimycolate assays.

Authors:  A Gurvitz
Journal:  Lett Appl Microbiol       Date:  2010-01-27       Impact factor: 2.858

7.  Duplication and selection in β-ketoacyl-ACP synthase gene lineages in the sexually deceptive Chiloglottis (Orchidaceace).

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Journal:  Ann Bot       Date:  2019-06-24       Impact factor: 4.357

8.  Cryo-EM structure of fatty acid synthase (FAS) from Rhodosporidium toruloides provides insights into the evolutionary development of fungal FAS.

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Journal:  Protein Sci       Date:  2015-04-02       Impact factor: 6.725

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Authors:  Long Nam Nguyen; David Trofa; Joshua D Nosanchuk
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Authors:  Luis Gonzaga Heredia-Martínez; Ascensión Andrés-Garrido; Enrique Martínez-Force; María Esther Pérez-Pérez; José L Crespo
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