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Infect Immun, July 1998, p. 3242-3249, Vol. 66, No. 7
0019-9567/98/$04.00+0
Copyright © 1998, American Society for Microbiology. All rights reserved.
In Vitro Cellular Toxicity Predicts
Pseudomonas aeruginosa Virulence in Lung
Infections
Teiji
Sawa,1
Maria
Ohara,1
Kiyoyasu
Kurahashi,1
Sally S.
Twining,2
Dara W.
Frank,3
David B.
Doroques,1
Taicy
Long,1
Michael A.
Gropper,1 and
Jeanine
P.
Wiener-Kronish1,*
Departments of Anesthesia and Medicine,
Cardiovascular Research Institute, The University of California,
San Francisco, California 94143,1 and
Department of Biochemistry2 and
Department of Microbiology,3 Medical
College of Wisconsin, Milwaukee, Wisconsin 53226
Received 21 January 1998/Returned for modification 30 March
1998/Accepted 29 April 1998
The role of quorum sensing by Pseudomonas aeruginosa in
producing cytotoxicity has not been fully investigated. Strains of P. aeruginosa have been characterized as having an invasive
or a cytotoxic phenotype (S. M. J. Fleiszig et al., Infect.
Immun. 65:579-586, 1997). We noted that the application of a large
inoculum of the invasive strain 6294 caused cytotoxicity of cultured
epithelial cells. To investigate this dose-related cytotoxicity, we
compared the behavior of 6294 to that of another invasive strain, PAO1, and determined whether the cytotoxicity could be related to quorum sensing. Both invasive strains, 6294 and PAO1, appear to have quorum-sensing systems that were operative when large doses of bacteria
were applied to cultured lung epithelial cells or instilled into the
lungs of animals. Nonetheless, only 6294 was cytotoxic. Cytotoxicity
induced by 6294 correlated with increased elastase production. These
experiments suggest that there are multiple mechanisms for the
induction of cytotoxicity, pathology, and mortality in vivo. However,
in vivo cytotoxicity and mortality, but not pathology, could be
predicted by quantitative in vitro cellular damage experiments
utilizing a range of bacteria-to-cell ratios. It appears that quorum
sensing may inversely correlate with virulence in that strains that
produced PAI [N-(3-oxododecanoyl) homoserine lactone]
also appeared to attract more polymorphonuclear leukocytes in vivo and
were possibly eliminated more quickly. In addition, exoproduct
production in bacteriological medium in vitro may differ significantly
from exoproduct expression from infections in vivo or during
cocultivation of bacteria with tissue culture cells.
*
Corresponding author. Mailing address: Department of
Anesthesia and Critical Care Medicine, The University of California, San Francisco, CA 94143. Phone: (415) 476-8968. Fax: (415) 476-5434. E-mail: jwk{at}jemo.ucsf.edu.
Infect Immun, July 1998, p. 3242-3249, Vol. 66, No. 7
0019-9567/98/$04.00+0
Copyright © 1998, American Society for Microbiology. All rights reserved.
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