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Infection and Immunity, November 1999, p. 6067-6075, Vol. 67, No. 11
0019-9567/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
Enterococcus faecalis Bearing Aggregation Substance Is
Resistant to Killing by Human Neutrophils despite Phagocytosis
and Neutrophil Activation
Robert M.
Rakita,1,2,*
Natalie N.
Vanek,1
Karen
Jacques-Palaz,1
Mee
Mee,1
M. Michele
Mariscalco,3
Gary M.
Dunny,4
Mark
Snuggs,5
W. Barry
Van
Winkle,5 and
Scott I.
Simon3
Division of Infectious Diseases, Department
of Internal Medicine,1 and Department of
Pathology and Laboratory Medicine,5 University
of Texas Medical School at Houston, and Speros P. Martel
Section of Leukocyte Biology, Department of Pediatrics, Baylor College
of Medicine,3 Houston, Texas 77030;
Virginia Mason Medical Center, Seattle, Washington
981112; and Department of
Microbiology, University of Minnesota Medical School, Minneapolis,
Minnesota 554554
Received 1 April 1999/Returned for modification 24 May
1999/Accepted 26 August 1999
Enterococcus faecalis aggregation substance (AS)
mediates efficient bacterium-bacterium contact to facilitate plasmid
exchange as part of a bacterial sex pheromone system. We have
previously determined that AS promotes direct, opsonin-independent
binding of E. faecalis to human neutrophils (PMNs) via
complement receptor type 3 and other receptors on the PMN surface. We
have now examined the functional consequences of this bacterium-host
cell interaction. AS-bearing E. faecalis was phagocytosed
and internalized by PMNs, as determined by deconvolution fluorescence
microscopy. However, these bacteria were not killed by PMNs, and
internalized bacteria excluded propidium iodide, indicating intact
bacterial membranes. Resistance to killing occurred despite activation
of PMNs, as indicated by an increase in both functional and total
surface Mac-1 expression, shedding of L-selectin, and an
increase in PMN extracellular superoxide and phagosomal oxidant
production. Deconvolution fluorescence microscopy also revealed that
phagosomes containing AS-bearing bacteria were markedly larger than
phagosomes containing opsonized E. faecalis, suggesting
that some modification of phagosomal maturation may be involved in
AS-induced resistance to killing. PMN phagosomal pH was significantly
higher after ingestion of nonopsonized AS-bearing E. faecalis than after that of opsonized bacteria. The novel ability
of AS to promote intracellular survival of E. faecalis
inside PMNs suggests that AS may be a virulence factor used by strains
of E. faecalis.
*
Corresponding author. Mailing address: Virginia Mason
Medical Center, 1100 Ninth Ave., P.O. Box 900 (Mail Stop: C7-PUL),
Seattle, WA 98111. Phone: (206) 341-0846. Fax: (206) 223-6814. E-mail: cidrmr{at}vmmc.org.
Infection and Immunity, November 1999, p. 6067-6075, Vol. 67, No. 11
0019-9567/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
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