Biosynthesis of antibacterial iron-chelating tropolones in Aspergillus nidulans 
as response to glycopeptide-producing Streptomycetes

Gerke, Jennifer; Köhler, Anna M.; Wennrich, Jan-Peer; Große, Verena; Shao, Lulu; Heinrich, Antje K.; Bode, Helge B.; Chen, Wanping; Surup, Frank; Braus, Gerhard H.

doi:10.3389/ffunb.2021.777474

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Biosynthesis of antibacterial iron-chelating tropolones in Aspergillus nidulans as response to glycopeptide-producing Streptomycetes

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Bode, Helge B.
Natural Product Function and Engineering, Department of Natural Products in Organismic Interactions, Max Planck Institute for Terrestrial Microbiology, Max Planck Society;
Molecular Biotechnology, Department of Biosciences, Goethe University Frankfurt, Frankfurt, Germany, External Organizations;

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https://doi.org/10.3389/ffunb.2021.777474
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Citation

Gerke, J., Köhler, A. M., Wennrich, J.-P., Große, V., Shao, L., Heinrich, A. K., et al. (2022). Biosynthesis of antibacterial iron-chelating tropolones in Aspergillus nidulans as response to glycopeptide-producing Streptomycetes. Frontiers in Fungal Biology, 2: 777474. doi:10.3389/ffunb.2021.777474.

Cite as: https://hdl.handle.net/21.11116/0000-000E-0534-2

Abstract

The soil microbiome comprises numerous filamentous fungi and bacteria that mutually react and challenge each other by the production of bioactive secondary metabolites. Herein, we show in liquid co-cultures that the presence of filamentous Streptomycetes producing antifungal glycopeptide antibiotics induces the production of the antibacterial and iron-chelating tropolones anhydrosepedonin (1) and antibiotic C (2) in the mold Aspergillus nidulans. Additionally, the biosynthesis of the related polyketide tripyrnidone (5) was induced, whose novel tricyclic scaffold we elucidated by NMR and HRESIMS data. The corresponding biosynthetic polyketide synthase-encoding gene cluster responsible for the production of these compounds was identified. The tropolones as well as tripyrnidone (5) are produced by genes that belong to the broad reservoir of the fungal genome for the synthesis of different secondary metabolites, which are usually silenced under standard laboratory conditions. These molecules might be part of the bacterium-fungus competition in the complex soil environment, with the bacterial glycopeptide antibiotic as specific environmental trigger for fungal induction of this cluster.