Affiliation:
1. The Biodesign Institute, Arizona State University, Tempe, Arizona, USA
2. School of Life Sciences, Arizona State University, Tempe, Arizona, USA
Abstract
ABSTRACT
Salmonella enterica
serovar Typhimurium genome encodes 13 fimbrial operons. Most of the fimbriae encoded by these operons are not produced under laboratory conditions but are likely to be synthesized
in vivo
. We used an
in vivo
expression technology (IVET) strategy to identify four fimbrial operons,
agf
,
saf
,
sti
, and
stc
that are expressed in the spleen. When any three of these operons were deleted, the strain retained wild-type virulence. However, when all four operons were deleted, the resulting strain was completely attenuated, indicating that these four fimbriae play functionally redundant roles critical for virulence. In mice, oral doses of as low as 1 × 10
5
CFU of the strain with four fimbrial operons deleted provided 100% protection against challenge with 1 × 10
9
CFU of wild-type
S
. Typhimurium. We also examined the possible effect of these fimbriae on the ability of a
Salmonella
vaccine strain to deliver a guest antigen. We modified one of our established attenuated vaccine strains, χ9088, to delete three fimbrial operons while the fourth operon was constitutively expressed. Each derivative was modified to express the
Streptococcus pneumoniae
antigen PspA. Strains that constitutively expressed
saf
or
stc
elicited a strong Th1 response with significantly greater levels of anti-PspA serum IgG and greater protective efficacy than strains carrying
saf
or
stc
deletions. The isogenic strain in which all four operons were deleted generated the lowest anti-PspA levels and did not protect against challenge with virulent
S. pneumoniae
. Our results indicate that these fimbriae play important roles, as yet not understood, in
Salmonella
virulence and immunogenicity.
IMPORTANCE
Salmonella enterica
is the leading cause of bacterial food-borne infection in the United States. S. Typhimurium is capable of producing up to 13 distinct surface structures called fimbriae that presumably mediate its adherence to surfaces. The roles of most of these fimbriae in disease are unknown. Identifying fimbriae produced during infection will provide important insights into how these bacterial structures contribute to disease and potentially induce protective immunity to
Salmonella
infection. We identified four fimbriae that are produced during infection. Deletion of all four of these fimbriae results in a significant reduction in virulence. We explored ways in which the expression of these fimbriae may be exploited for use in recombinant
Salmonella
vaccine strains and found that production of Saf and Stc fimbriae are important for generating a strong immune response against a vectored antigen. This work provides new insight into the role of fimbriae in disease and their potential for improving the efficacy of
Salmonella
-based vaccines.
Funder
HHS | National Institutes of Health
Publisher
American Society for Microbiology
Cited by
14 articles.
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