L- and P-selectin and CD11/CD18 in intracapillary neutrophil sequestration in rabbit lungs

Infusion of complement fragments induces rapid sequestration of neutrophils within pulmonary capillaries. This study examined the mechanisms through which this sequestration occurs, as well as the effect of complement fragments on the expression of L-selectin and CD11/CD18 using ultrastructural immu...

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Veröffentlicht in:American journal of respiratory and critical care medicine 1999, Vol.159 (1), p.267-274
Hauptverfasser: KUBO, H, DOYLE, N. A, GRAHAM, L, BHAGWAN, S. D, QUINLAN, W. M, DOERSCHUK, C. M
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container_issue 1
container_start_page 267
container_title American journal of respiratory and critical care medicine
container_volume 159
creator KUBO, H
DOYLE, N. A
GRAHAM, L
BHAGWAN, S. D
QUINLAN, W. M
DOERSCHUK, C. M
description Infusion of complement fragments induces rapid sequestration of neutrophils within pulmonary capillaries. This study examined the mechanisms through which this sequestration occurs, as well as the effect of complement fragments on the expression of L-selectin and CD11/CD18 using ultrastructural immunohistochemistry. Studies using anti-P-selectin antibodies, fucoidin, L-selectin-depleted neutrophils, and anti-CD18 antibodies showed that selectins and CD18 were not required for neutrophil sequestration. However, maintaining the sequestered neutrophils within the pulmonary capillaries required both L-selectin and CD11/CD18. Neutrophils in the pulmonary capillaries of rabbits given complement fragments expressed 72% less L-selectin and 98% more CD11/CD18 than did those in rabbits given saline. Shedding of L-selectin occurred preferentially from the microvillar processes of the plasma membrane rather than from the flat intervening regions. About 28% of L-selectin still remained on intracapillary neutrophil membranes after 15 min and was likely available for binding. Shedding of L-selectin appeared slower in vivo than in vitro. These studies indicate that neutrophil sequestration induced by complement fragments requires at least two sequential steps, one that does not require recognized adhesion molecules followed by a second that requires L-selectin and CD11/ CD18.
doi_str_mv 10.1164/ajrccm.159.1.9709011
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ispartof American journal of respiratory and critical care medicine, 1999, Vol.159 (1), p.267-274
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source MEDLINE; Elektronische Zeitschriftenbibliothek - Frei zugängliche E-Journals; Journals@Ovid Complete; American Thoracic Society (ATS) Journals Online
subjects Air breathing
Animals
Antibodies - pharmacology
Biological and medical sciences
Capillaries - physiology
CD11 Antigens - metabolism
CD11 Antigens - physiology
CD18 Antigens - immunology
CD18 Antigens - metabolism
CD18 Antigens - physiology
Chymotrypsin - pharmacology
Fundamental and applied biological sciences. Psychology
Immunohistochemistry
L-Selectin - metabolism
L-Selectin - physiology
Neutrophils - drug effects
Neutrophils - metabolism
Neutrophils - physiology
Neutrophils - ultrastructure
P-Selectin - immunology
P-Selectin - physiology
Polysaccharides - pharmacology
Pulmonary Circulation - physiology
Rabbits
Respiratory system: anatomy, metabolism, gas exchange, ventilatory mechanics, respiratory hemodynamics
Tissue Distribution
Vertebrates: respiratory system
title L- and P-selectin and CD11/CD18 in intracapillary neutrophil sequestration in rabbit lungs
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