Microbial Synthesis of the Forskolin Precursor Manoyl Oxide in an Enantiomerically Pure Form
Author(s) -
Morten T. Nielsen,
Johan AndersenRanberg,
Ulla Christensen,
Hanne Bjerre Christensen,
Scott J. Harrison,
Carl Erik Olsen,
Björn Hamberger,
Birger Lindberg Møller,
Morten H. H. Nørholm
Publication year - 2014
Publication title -
applied and environmental microbiology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.552
H-Index - 324
eISSN - 1070-6291
pISSN - 0099-2240
DOI - 10.1128/aem.02301-14
Subject(s) - yield (engineering) , forskolin , metabolite , fermentation , terpenoid , pipeline (software) , corynebacterium glutamicum , de novo synthesis , biology , chemistry , biochemical engineering , microbiology and biotechnology , botany , biochemistry , computer science , enzyme , engineering , materials science , receptor , gene , metallurgy , programming language
Forskolin is a promising medicinal compound belonging to a plethora of specialized plant metabolites that constitute a rich source of bioactive high-value compounds. A major obstacle for exploitation of plant metabolites is that they often are produced in small amounts and in plants difficult to cultivate. This may result in insufficient and unreliable supply leading to fluctuating and high sales prices. Hence, substantial efforts and resources have been invested in developing sustainable and reliable supply routes based on microbial cell factories. Here, we report microbial synthesis of (13R)-manoyl oxide, a proposed intermediate in the biosynthesis of forskolin and other medically important labdane-type terpenoids. Process optimization enabled synthesis of enantiomerically pure (13R)-manoyl oxide as the sole metabolite, providing a pure compound in just two steps with a yield of 10 mg/liter. The work presented here demonstrates the value of a standardized bioengineering pipeline and the large potential of microbial cell factories as sources for sustainable synthesis of complex biochemicals.
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