Metabolic engineering of yeast forde novoproduction of kratom monoterpene indole alkaloids

Author:

Holtz MaxenceORCID,Rago DanielaORCID,Nedermark Ida,Hansson Frederik G.ORCID,Lehka Beata J.ORCID,Hansen Lea G.ORCID,Marcussen Nils E. J.,Veneman Wouter J.ORCID,Ahonen LindaORCID,Wungsintaweekul JuraithipORCID,Dirks Ron P.ORCID,Acevedo-Rocha Carlos G.ORCID,Zhang JieORCID,Keasling Jay D.ORCID,Jensen Michael K.ORCID

Abstract

AbstractMonoterpene indole alkaloids (MIAs) fromMitragyna speciosa(“kratom”), such as mitragynine and speciogynine, are promising novel scaffolds for opioid receptor ligands for treatment of pain, addiction, and depression. While kratom leaves have been used for centuries in South-East Asia as stimulant and pain management substance, the biosynthetic pathway of these psychoactives have only recently been partially elucidated. Here, we demonstrate thede novoproduction of mitragynine and speciogynine inSaccharomyces cerevisiaethrough the reconstruction of a five-step synthetic pathway from common MIA precursor strictosidine comprising fungal tryptamine 4-monooxygenase to bypass an unknown kratom hydroxylase. Upon optimizing cultivation conditions, a titer of ∼290 µg/L kratom MIAs from glucose was achieved. Untargeted metabolomics analysis of lead production strains led to the identification of numerous shunt products derived from the activity of strictosidine synthase (STR) and dihydrocorynantheine synthase (DCS), highlighting them as candidates for enzyme engineering to further improve kratom MIAs production in yeast. Finally, by feeding fluorinated tryptamine and expressing a human tailoring enzyme, we further demonstrate production of fluorinated and hydroxylated mitragynine derivatives with potential applications in drug discovery campaigns. Altogether, this study introduces a yeast cell factory platform for the biomanufacturing of complex natural and new-to-nature kratom MIAs derivatives with therapeutic potential.

Publisher

Cold Spring Harbor Laboratory

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