Identification of a cyclohexylcarbonyl CoA biosynthetic gene cluster and application in the production of doramectin
The side chain of the antifungal antibiotic ansatrienin A from Streptomyces collinus contains a cyclohexanecarboxylic acid (CHC)-derived moiety. This moiety is also observed in trace amounts of ω-cyclohexyl fatty acids (typically less than 1% of total fatty acids) produced by S. collinus . Coenzyme...
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Veröffentlicht in: | Nature biotechnology 2000-09, Vol.18 (9), p.980-983 |
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Sprache: | eng |
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Zusammenfassung: | The side chain of the antifungal antibiotic ansatrienin A from
Streptomyces collinus
contains a cyclohexanecarboxylic acid (CHC)-derived moiety. This moiety is also observed in trace amounts of ω-cyclohexyl fatty acids (typically less than 1% of total fatty acids) produced by
S. collinus
. Coenzyme A-activated CHC (CHC-CoA) is derived from shikimic acid through a reductive pathway involving a minimum of nine catalytic steps. Five putative CHC-CoA biosynthetic genes in the ansatrienin biosynthetic gene cluster of
S. collinus
have been identified. Plasmid-based heterologous expression of these five genes in
Streptomyces avermitilis
or
Streptomyces lividans
allows for production of significant amounts of ω-cyclohexyl fatty acids (as high as 49% of total fatty acids). In the absence of the plasmid these organisms are dependent on exogenously supplied CHC for ω-cyclohexyl fatty acid production. Doramectin is a commercial antiparasitic avermectin analog produced by fermenting a
bkd
mutant of
S. avermitilis
in the presence of CHC. Introduction of the
S. collinus
CHC-CoA biosynthetic gene cassette into this organism resulted in an engineered strain able to produce doramectin without CHC supplementation. The CHC-CoA biosynthetic gene cluster represents an important genetic tool for precursor-directed biosynthesis of doramectin and has potential for directed biosynthesis in other important polyketide-producing organisms. |
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ISSN: | 1087-0156 1546-1696 |
DOI: | 10.1038/79479 |