Thioesterase-mediated side chain transesterification generates potent Gq signaling inhibitor FR900359

Author:

Hermes CorneliaORCID,Richarz René,Wirtz Daniel A.,Patt JulianORCID,Hanke Wiebke,Kehraus Stefan,Voß Jan HendrikORCID,Küppers Jim,Ohbayashi Tsubasa,Namasivayam VigneshwaranORCID,Alenfelder Judith,Inoue Asuka,Mergaert PeterORCID,Gütschow Michael,Müller Christa E.ORCID,Kostenis EviORCID,König Gabriele M.,Crüsemann MaxORCID

Abstract

AbstractThe potent and selective Gq protein inhibitor depsipeptide FR900359 (FR), originally discovered as the product of an uncultivable plant endosymbiont, is synthesized by a complex biosynthetic system comprising two nonribosomal peptide synthetase (NRPS) assembly lines. Here we characterize a cultivable bacterial FR producer, enabling detailed investigations into biosynthesis and attachment of the functionally important FR side chain. We reconstitute side chain assembly by the monomodular NRPS FrsA and the non-heme monooxygenase FrsH, and characterize intermolecular side chain transesterification to the final macrocyclic intermediate FR-Core, mediated by the FrsA thioesterase domain. We harness FrsA substrate promiscuity to generate FR analogs with altered side chains and demonstrate indispensability of the FR side chain for efficient Gq inhibition by comparative bioactivity, toxicity and docking studies. Finally, evolution of FR and side chain biosynthesis is discussed based on bioinformatics analyses. Side chain transesterification boosts potency and target affinity of selective Gq inhibitor natural products.

Funder

Deutsche Bundesstiftung Umwelt

Japan Agency for Medical Research and Development

Deutsche Forschungsgemeinschaft

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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