Affiliation:
1. Department of Microbiology and Immunology1 and
2. Co-Operative Research Centre for Vaccine Technology,2 The University of Melbourne, Parkville, Victoria 3052, Australia
Abstract
ABSTRACT
This study describes the construction and analysis of three in vivo-inducible promoter expression plasmids, containing p
nirB
, p
pagC
, and p
katG
, for the delivery of foreign antigens in the Δ
aroAD
mutant of
Salmonella enterica
var. Typhimurium (hereafter referred to as
S. typhimurium
). The reporter genes encoding β-galactosidase and firefly luciferase were used to assess the comparative levels of promoter activity in
S. typhimurium
in vitro in response to different induction stimuli and in vivo in immunized mice. It was determined that the p
pagC
construct directed the expression of more β-galactosidase and luciferase in
S. typhimurium
than the p
nirB
and p
katG
constructs, both in vitro and in vivo. The gene encoding the C fragment of tetanus toxin was expressed in the
aroAD
mutant of
S. typhimurium
(BRD509) under the control of the three promoters. Mice orally immunized with attenuated
S. typhimurium
expressing C fragment under control of the
pagC
promoter [BRD509(pKK/p
pagC
/C frag)] mounted the highest tetanus toxoid-specific serum antibody response. Levels of luciferase expression in vivo and C-fragment expression in vitro from the
pagC
promoter appeared to be equivalent to if not lower than the levels of expression detected with the constitutive
trc
promoter. However, mice immunized with BRD509(pKK/p
pagC
/C frag) induced significantly higher levels of tetanus toxoid-specific antibody than BRD509(pKK/C frag)-immunized mice, suggesting that the specific location of foreign antigen expression may be important for immunogenicity. Mutagenesis of the ribosome binding sites (RBS) in the three promoter/C fragment expression plasmids was also performed. Despite optimization of the RBS in the three different promoter elements, the expression levels in vivo and overall immunogenicity of C fragment when delivered to mice by attenuated
S. typhimurium
were not affected. These studies suggest that in vivo-inducible promoters may give rise to enhanced immunogenicity and increase the efficacy of
S. typhimurium
as a vaccine vector.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Immunology,Microbiology,Parasitology
Cited by
50 articles.
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