Affiliation:
1. School of Pharmacy1and
2. Global Supply/CFO/API, Pharmacia and Upjohn, 20014 Nerviano, Milan, Italy2
3. Department of Bacteriology,3University of Wisconsin, Madison, Wisconsin 53706, and
Abstract
ABSTRACT
Doxorubicin-overproducing strains of
Streptomyces peucetius
ATCC 29050 can be obtained through manipulation of the genes in the region of the doxorubicin (DXR) gene cluster that contains
dpsH
, the
dpsG
polyketide synthase gene, the putative
dnrU
ketoreductase gene,
dnrV
, and the
doxA
cytochrome P-450 gene. These five genes were characterized by sequence analysis, and the effects of replacing
dnrU
,
dnrV
,
doxA
, or
dpsH
with mutant alleles and of
doxA
overexpression on the production of the principal anthracycline metabolites of
S. peucetius
were studied. The exact roles of
dpsH
and
dnrV
could not be established, although
dnrV
is implicated in the enzymatic reactions catalyzed by DoxA, but
dnrU
appears to encode a ketoreductase specific for the C-13 carbonyl of daunorubicin (DNR) and DXR or their biosynthetic precursors. The highest DXR titers were obtained in a
dnrX dnrU
(N. Lomovskaya, Y. Doi-Katayama, S. Filippini, C. Nastro, L. Fonstein, M. Gallo, A. L. Colombo, and C. R. Hutchinson, J. Bacteriol. 180:2379–2386, 1998) double mutant and a
dnrX dnrU dnrH
(C. Scotti and C. R. Hutchinson, J. Bacteriol. 178:7316–7321, 1996) triple mutant. Overexpression of
doxA
in a
doxA::aphII
mutant resulted in the accumulation of DXR precursors instead of in a notable increase in DXR production. In contrast, overexpression of
dnrV
and
doxA
jointly in the
dnrX dnrU
double mutant or the
dnrX dnrU dnrH
triple mutant increased the DXR titer 36 to 86%.
Publisher
American Society for Microbiology
Subject
Molecular Biology,Microbiology
Reference64 articles.
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F.
Doxorubicin: anticancer antibiotics.
1981
Academic Press
New York N.Y
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