Affiliation:
1. Megan Health, Inc., St. Louis, Missouri 63110,1 and
2. Department of Biology, Washington University, St. Louis, Missouri 631302
Abstract
ABSTRACT
Salmonella enterica poxA
mutants exhibit a pleiotropic phenotype, including reduced pyruvate oxidase activity; reduced growth rate; and hypersensitivity to the herbicide sulfometuron methyl, α-ketobutyrate, and amino acid analogs. These mutants also failed to grow in the presence of the host antimicrobial peptide, protamine. In this study, PoxA
−
mutants of
S. enterica
serovar Typhimurium (
S. typhimurium
) were found to be 10,000-fold attenuated in orally inoculated BALB/c mice and 1,000-fold attenuated in intraperitoneally inoculated BALB/c mice, compared to wild-type
S. typhimurium
UK-1. In addition,
poxA
mutants were found to be capable of colonizing the spleen, mesenteric lymph nodes, and Peyer’s patches; to induce strong humoral immune responses; and to protect mice against a lethal wild-type
Salmonella
challenge. A 2-kb DNA fragment was isolated from wild-type
S. typhimurium
UK-1 based on its ability to complement an isogenic
poxA
mutant. The nucleotide sequence of this DNA fragment revealed an open reading frame of 325 amino acids capable of encoding a polypeptide of 36.8 kDa that was confirmed in the bacteriophage T7 expression system. Comparison of the translated sequence to the available databases indicated high homology to a family of lysyl-tRNA synthetases. Our results indicate that a mutation of
poxA
has an attenuating effect on
Salmonella
virulence. Further,
poxA
mutants are immunogenic and could be useful in designing live vaccines with a variety of bacterial species. To our knowledge, this is the first report on the effect of
poxA
mutation on bacterial virulence.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Immunology,Microbiology,Parasitology
Cited by
49 articles.
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