Affiliation:
1. Institute of Infections and Immunity,1
2. Department of Applied Biochemistry and Food Science,2 and
3. School of Pharmaceutical Sciences,3University of Nottingham, Nottingham NG7 2UH, United Kingdom
Abstract
ABSTRACT
From a mass-excised
Staphylococcus aureus
λZapII expression library, we cloned an operon encoding a novel ABC transporter with significant homology to bacterial siderophore transporter systems. The operon encodes four genes designated
sstA
, -
B
, -
C
, and -
D
encoding two putative cytoplasmic membrane proteins (
sstA
and
sstB
), an ATPase (
sstC
), and a membrane-bound 38-kDa lipoprotein (
sstD
). The
sst
operon is preceded by two putative Fur boxes, which indicated that expression of the
sst
operon was likely to be iron dependent. SstD was overexpressed in
Escherichia coli
, purified by Triton X-114 phase partitioning, and used to generate monospecific antisera in rats. Immunoblotting studies located SstD in the membrane fraction of
S. aureus
and showed that expression of the lipoprotein was reduced under iron-rich growth conditions. Triton X-114 partitioning studies on isolated membranes provided additional biochemical evidence that SstD in
S. aureus
is a lipoprotein. Immunoreactive polypeptides of approximately 38 kDa were detected in a wide range of staphylococcal species, but no antigenic homolog was detected in
Bacillus subtilis
. Expression of SstD in vivo was confirmed by immunoblotting studies with
S. aureus
recovered from a rat intraperitoneal chamber implant model. To further define the contribution of SstD in promoting growth of
S. aureus
in vitro and in vivo, we used antisense RNA technology to modulate expression of SstD. Expression of antisense
sstD
RNA in
S. aureus
resulted in a decrease in SstD expression under both iron-rich and iron-restricted growth conditions. However, this reduction in SstD levels did not affect the growth of
S. aureus
in vitro in an iron-limited growth medium or when grown in an intraperitoneal rat chamber implant model in vivo.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Immunology,Microbiology,Parasitology
Cited by
84 articles.
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