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Designed biosynthesis of 36-methyl-FK506 by polyketide precursor pathway engineering.


ABSTRACT: The polyketide synthase (PKS) biosynthetic code has recently expanded to include a newly recognized group of extender unit substrates derived from ?,?-unsaturated acyl-CoA molecules that deliver diverse side chain chemistry to polyketide backbones. Herein we report the identification of a three-gene operon responsible for the biosynthesis of the PKS building block isobutyrylmalonyl-CoA associated with the macrolide ansalactam A from the marine bacterium Streptomyces sp. CNH189. Using a synthetic biology approach, we engineered the production of unnatural 36-methyl-FK506 in Streptomyces sp. KCTC 11604BP by incorporating the branched extender unit into FK506 biosynthesis in place of its natural C-21 allyl side chain, which has been shown to be critical for FK506's potent immunosuppressant and neurite outgrowth activities.

SUBMITTER: Lechner A 

PROVIDER: S-EPMC3716868 | biostudies-literature | 2013 Jul

REPOSITORIES: biostudies-literature

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Designed biosynthesis of 36-methyl-FK506 by polyketide precursor pathway engineering.

Lechner Anna A   Wilson Micheal C MC   Ban Yeon Hee YH   Hwang Jae-Yeon JY   Yoon Yeo Joon YJ   Moore Bradley S BS  

ACS synthetic biology 20121105 7


The polyketide synthase (PKS) biosynthetic code has recently expanded to include a newly recognized group of extender unit substrates derived from α,β-unsaturated acyl-CoA molecules that deliver diverse side chain chemistry to polyketide backbones. Herein we report the identification of a three-gene operon responsible for the biosynthesis of the PKS building block isobutyrylmalonyl-CoA associated with the macrolide ansalactam A from the marine bacterium Streptomyces sp. CNH189. Using a synthetic  ...[more]

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