Affiliation:
1. Department of Chemistry, The Johns Hopkins University, Baltimore, Maryland 21218
Abstract
ABSTRACT
Clavulanic acid is a potent inhibitor of β-lactamase enzymes and is of demonstrated value in the treatment of infections by β-lactam-resistant bacteria. Previously, it was thought that eight contiguous genes within the genome of the producing strain
Streptomyces clavuligerus
were sufficient for clavulanic acid biosynthesis, because they allowed production of the antibiotic in a heterologous host (K. A. Aidoo, A. S. Paradkar, D. C. Alexander, and S. E. Jensen, p. 219–236,
In
V. P. Gullo et al., ed.,
Development in industrial microbiology series
, 1993). In contrast, we report the identification of three new genes,
orf10
(
cyp
),
orf11
(
fd
), and
orf12
, that are required for clavulanic acid biosynthesis as indicated by gene replacement and
trans
-complementation analysis in
S. clavuligerus
. These genes are contained within a 3.4-kb DNA fragment located directly downstream of
orf9
(
cad
) in the clavulanic acid cluster. While the
orf10
(
cyp
) and
orf11
(
fd
) proteins show homologies to other known
CYP-150
cytochrome P-450 and [3Fe-4S] ferredoxin enzymes and may be responsible for an oxidative reaction late in the pathway, the protein encoded by
orf12
shows no significant similarity to any known protein. The results of this study extend the biosynthetic gene cluster for clavulanic acid and attest to the importance of analyzing biosynthetic genes in the context of their natural host. Potential functional roles for these proteins are proposed.
Publisher
American Society for Microbiology
Subject
Molecular Biology,Microbiology
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V. P.
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R. K.
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