A lethal role for lipid A in Salmonella infections.

Khan, SA; Everest, P; Servos, S; Foxwell, N; Zähringer, U; Brade, H; Rietschel, ET; Dougan, G; Charles, IG; Maskell, DJ

A lethal role for lipid A in Salmonella infections.

Khan, SA Everest, P Servos, S Foxwell, N Zähringer, U Brade, H Rietschel, ET Dougan, G Charles, IG Maskell, DJ

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Publication Type:: Journal Article
Citation:: Mol Microbiol, 1998, 29 (2), pp. 571 - 579
Issue Date:: 1998-07

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Field	Value	Language
dc.contributor.author	Khan, SA	en_US
dc.contributor.author	Everest, P	en_US
dc.contributor.author	Servos, S	en_US
dc.contributor.author	Foxwell, N	en_US
dc.contributor.author	Zähringer, U	en_US
dc.contributor.author	Brade, H	en_US
dc.contributor.author	Rietschel, ET	en_US
dc.contributor.author	Dougan, G	en_US
dc.contributor.author	Charles, IG	en_US
dc.contributor.author	Maskell, DJ	en_US
dc.date.issued	1998-07	en_US
dc.identifier.citation	Mol Microbiol, 1998, 29 (2), pp. 571 - 579	en_US
dc.identifier.issn	0950-382X	en_US
dc.identifier.uri	http://hdl.handle.net/10453/13279
dc.description.abstract	Salmonella infections in naturally susceptible mice grow rapidly, with death occurring only after bacterial numbers in vivo have reached a high threshold level, commonly called the lethal load. Despite much speculation, no direct evidence has been available to substantiate a role for any candidate bacterial components in causing death. One of the most likely candidates for the lethal toxin in salmonellosis is endotoxin, specifically the lipid A domain of the lipopolysaccharide (LPS) molecule. Consequently, we have constructed a Salmonella mutant with a deletion-insertion in its waaN gene, which encodes the enzyme that catalyses one of the two secondary acylation reactions that complete lipid A biosynthesis. The mutant biosynthesizes a lipid A molecule lacking a single fatty acyl chain and is consequently less able to induce cytokine and inducible nitric oxide synthase (iNOS) responses both in vivo and in vitro. The mutant bacteria appear healthy, are not sensitive to increased growth temperature and synthesize a full-length O-antigen-containing LPS molecule lacking only the expected secondary acyl chain. On intravenous inoculation into susceptible BALB/c mice, wild-type salmonellae grew at the expected rate of approximately 10-fold per day in livers and spleens and caused the death of the infected mice when lethal loads of approximately 10(8) were attained in these organs. Somewhat unexpectedly, waaN mutant bacteria grew at exactly the same rate as wild-type bacteria in BALB/c mice but, when counts reached 10(8) per organ, mice infected with mutant bacteria survived. Bacterial growth continued until unprecedentedly high counts of 10(9) per organ were attained, when approximately 10% of the mice died. Most of the animals carrying these high bacterial loads survived, and the bacteria were slowly cleared from the organs. These experiments provide the first direct evidence that death in a mouse typhoid infection is directly dependent on the toxicity of lipid A and suggest that this may be mediated via pro-inflammatory cytokine and/or iNOS responses.	en_US
dc.language	eng	en_US
dc.relation.ispartof	Mol Microbiol	en_US
dc.relation.isbasedon	10.1046/j.1365-2958.1998.00952.x	en_US
dc.subject.classification	Microbiology	en_US
dc.subject.mesh	Animals	en_US
dc.subject.mesh	Mice, Inbred BALB C	en_US
dc.subject.mesh	Mice	en_US
dc.subject.mesh	Salmonella typhimurium	en_US
dc.subject.mesh	Salmonella Infections, Animal	en_US
dc.subject.mesh	Acyltransferases	en_US
dc.subject.mesh	Lipid A	en_US
dc.subject.mesh	Tumor Necrosis Factor-alpha	en_US
dc.subject.mesh	Escherichia coli Proteins	en_US
dc.subject.mesh	Interleukin-1	en_US
dc.subject.mesh	Virulence	en_US
dc.subject.mesh	Phenotype	en_US
dc.subject.mesh	Mutation	en_US
dc.subject.mesh	Nitric Oxide Synthase	en_US
dc.subject.mesh	Nitric Oxide Synthase Type II	en_US
dc.title	A lethal role for lipid A in Salmonella infections.	en_US
dc.type	Journal Article
utslib.citation.volume	2	en_US
utslib.citation.volume	29	en_US
utslib.location.activity	England	en_US
utslib.for	0605 Microbiology	en_US
utslib.for	06 Biological Sciences	en_US
utslib.for	07 Agricultural and Veterinary Sciences	en_US
utslib.for	11 Medical and Health Sciences	en_US
dc.location.activity	ISI:000075560500015	en_US
pubs.embargo.period	Not known	en_US
pubs.organisational-group	/University of Technology Sydney
pubs.organisational-group	/University of Technology Sydney/Faculty of Science
pubs.organisational-group	/University of Technology Sydney/Strength - ithree - Institute of Infection, Immunity and Innovation
utslib.copyright.status	closed_access
pubs.issue	2	en_US
pubs.publication-status	Published	en_US
pubs.volume	29	en_US

Abstract:

Salmonella infections in naturally susceptible mice grow rapidly, with death occurring only after bacterial numbers in vivo have reached a high threshold level, commonly called the lethal load. Despite much speculation, no direct evidence has been available to substantiate a role for any candidate bacterial components in causing death. One of the most likely candidates for the lethal toxin in salmonellosis is endotoxin, specifically the lipid A domain of the lipopolysaccharide (LPS) molecule. Consequently, we have constructed a Salmonella mutant with a deletion-insertion in its waaN gene, which encodes the enzyme that catalyses one of the two secondary acylation reactions that complete lipid A biosynthesis. The mutant biosynthesizes a lipid A molecule lacking a single fatty acyl chain and is consequently less able to induce cytokine and inducible nitric oxide synthase (iNOS) responses both in vivo and in vitro. The mutant bacteria appear healthy, are not sensitive to increased growth temperature and synthesize a full-length O-antigen-containing LPS molecule lacking only the expected secondary acyl chain. On intravenous inoculation into susceptible BALB/c mice, wild-type salmonellae grew at the expected rate of approximately 10-fold per day in livers and spleens and caused the death of the infected mice when lethal loads of approximately 10(8) were attained in these organs. Somewhat unexpectedly, waaN mutant bacteria grew at exactly the same rate as wild-type bacteria in BALB/c mice but, when counts reached 10(8) per organ, mice infected with mutant bacteria survived. Bacterial growth continued until unprecedentedly high counts of 10(9) per organ were attained, when approximately 10% of the mice died. Most of the animals carrying these high bacterial loads survived, and the bacteria were slowly cleared from the organs. These experiments provide the first direct evidence that death in a mouse typhoid infection is directly dependent on the toxicity of lipid A and suggest that this may be mediated via pro-inflammatory cytokine and/or iNOS responses.

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http://hdl.handle.net/10453/13279