Origin of the 3-methylglutaryl moiety in caprazamycin biosynthesis

Daniel Bär; Benjamin Konetschny; Andreas Kulik; Houchao Xu; Davide Paccagnella; Patrick Beller; Nadine Ziemert; Jeroen S. Dickschat; Bertolt Gust

doi:10.1186/s12934-022-01955-6

Microbial Cell Factories (Nov 2022)

Origin of the 3-methylglutaryl moiety in caprazamycin biosynthesis

Daniel Bär,
Benjamin Konetschny,
Andreas Kulik,
Houchao Xu,
Davide Paccagnella,
Patrick Beller,
Nadine Ziemert,
Jeroen S. Dickschat,
Bertolt Gust

Affiliations

Daniel Bär: Department of Pharmaceutical Biology, Eberhard-Karls University Tübingen
Benjamin Konetschny: Department of Pharmaceutical Biology, Eberhard-Karls University Tübingen
Andreas Kulik: Department of Microbial Bioactive Compounds, Interfaculty Institute of Microbiology and Infection Medicine, Eberhard-Karls University Tübingen
Houchao Xu: Kekulé-Institute for Organic Chemistry and Biochemistry, University of Bonn
Davide Paccagnella: Interfaculty Institute of Microbiology and Infection Medicine, Institute for Bioinformatics and Medical Informatics, Eberhard-Karls University Tübingen
Patrick Beller: Department of Pharmaceutical Biology, Eberhard-Karls University Tübingen
Nadine Ziemert: Interfaculty Institute of Microbiology and Infection Medicine, Institute for Bioinformatics and Medical Informatics, Eberhard-Karls University Tübingen
Jeroen S. Dickschat: Kekulé-Institute for Organic Chemistry and Biochemistry, University of Bonn
Bertolt Gust: Department of Pharmaceutical Biology, Eberhard-Karls University Tübingen

DOI: https://doi.org/10.1186/s12934-022-01955-6
Journal volume & issue: Vol. 21, no. 1
pp. 1 – 15

Abstract

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Abstract Background Caprazamycins are liponucleoside antibiotics showing bioactivity against Gram-positive bacteria including clinically relevant Mycobacterium tuberculosis by targeting the bacterial MraY-translocase. Their chemical structure contains a unique 3-methylglutaryl moiety which they only share with the closely related liposidomycins. Although the biosynthesis of caprazamycin is understood to some extent, the origin of 3-methylglutaryl-CoA for caprazamycin biosynthesis remains elusive. Results In this work, we demonstrate two pathways of the heterologous producer Streptomyces coelicolor M1154 capable of supplying 3-methylglutaryl-CoA: One is encoded by the caprazamycin gene cluster itself including the 3-hydroxy-3-methylglutaryl-CoA synthase Cpz5. The second pathway is part of primary metabolism of the host cell and encodes for the leucine/isovalerate utilization pathway (Liu-pathway). We could identify the liu cluster in S. coelicolor M1154 and gene deletions showed that the intermediate 3-methylglutaconyl-CoA is used for 3-methylglutaryl-CoA biosynthesis. This is the first report of this intermediate being hijacked for secondary metabolite biosynthesis. Furthermore, Cpz20 and Cpz25 from the caprazamycin gene cluster were found to be part of a common route after both individual pathways are merged together. Conclusions The unique 3-methylglutaryl moiety in caprazamycin originates both from the caprazamycin gene cluster and the leucine/isovalerate utilization pathway of the heterologous host. Our study enhanced the knowledge on the caprazamycin biosynthesis and points out the importance of primary metabolism of the host cell for biosynthesis of natural products.

Published in Microbial Cell Factories

ISSN: 1475-2859 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Science: Microbiology
Website: https://microbialcellfactories.biomedcentral.com/

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