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Engineering anthracycline biosynthesis toward angucyclines.


ABSTRACT: The biosynthesis pathways of two anthracyclines, nogalamycin and aclacinomycin, were directed toward angucyclines by using an angucycline-specific cyclase, pgaF, isolated from a silent antibiotic biosynthesis gene cluster. Addition of pgaF to a gene cassette that harbored the early biosynthesis genes of nogalamycin resulted in the production of two known angucyclinone metabolites, rabelomycin and its precursor, UWM6. Substrate flexibility of pgaF was demonstrated by replacement of the nogalamycin minimal polyketide synthase genes in the gene cassette with the equivalent aclacinomycin genes together with aknE2 and aknF, which specify the unusual propionate starter unit in aclacinomycin biosynthesis. This modification led to the production of a novel angucyclinone, MM2002, in which the expected ethyl side chain was incorporated into the fourth ring.

SUBMITTER: Metsa-Ketela M 

PROVIDER: S-EPMC152523 | biostudies-literature | 2003 Apr

REPOSITORIES: biostudies-literature

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Engineering anthracycline biosynthesis toward angucyclines.

Metsä-Ketelä Mikko M   Palmu Kaisa K   Kunnari Tero T   Ylihonko Kristiina K   Mäntsälä Pekka P  

Antimicrobial agents and chemotherapy 20030401 4


The biosynthesis pathways of two anthracyclines, nogalamycin and aclacinomycin, were directed toward angucyclines by using an angucycline-specific cyclase, pgaF, isolated from a silent antibiotic biosynthesis gene cluster. Addition of pgaF to a gene cassette that harbored the early biosynthesis genes of nogalamycin resulted in the production of two known angucyclinone metabolites, rabelomycin and its precursor, UWM6. Substrate flexibility of pgaF was demonstrated by replacement of the nogalamyci  ...[more]

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