Complete reversal of acid-induced acute lung injury by blocking of platelet-neutrophil aggregation
Alexander Zarbock, … , Kai Singbartl, Klaus Ley
Alexander Zarbock, … , Kai Singbartl, Klaus Ley
Published December 1, 2006
Citation Information: J Clin Invest. 2006;116(12):3211-3219. https://doi.org/10.1172/JCI29499.
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Research Article Pulmonology

Complete reversal of acid-induced acute lung injury by blocking of platelet-neutrophil aggregation

Abstract

Acute lung injury (ALI) causes high mortality, but its molecular mechanisms are poorly understood. Acid aspiration is a frequent cause of ALI, leading to neutrophil sequestration, increased permeability, and deterioration of gas exchange. We investigated the role of platelet-neutrophil interactions in a murine model of acid-induced ALI. Acid aspiration induced P-selectin–dependent platelet-neutrophil interactions in blood and in lung capillaries. Reducing circulating platelets or blocking P-selectin halted the development of ALI. Bone marrow chimeras showed that platelet, not endothelial, P-selectin was responsible for the injury. The interaction of platelets with neutrophils and endothelia was associated with TXA2 formation, with detrimental effects on permeability and tissue function. Activated platelets induced endothelial expression of ICAM-1 and increased neutrophil adhesion. Inhibition of platelet-neutrophil aggregation improved gas exchange, reduced neutrophil recruitment and permeability, and prolonged survival. The key findings were confirmed in a sepsis-induced model of ALI. These findings may translate into improved clinical treatments for ALI.

Authors

Alexander Zarbock, Kai Singbartl, Klaus Ley

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Figure 6

Endothelial cell response to TP activation as reflected by F-actin localization and content.

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Endothelial cell response to TP activation as reflected by F-actin local...
(A) Human pulmonary endothelial cells were treated with 75 or 150 nM of TXA2 analogue (SQ 29548), and F-actin was localized by phalloidin staining. Images are representative of 3 experiments with similar results. Original magnification, ×175. (B) Activated platelets and activated PMNs induced a significant increase of F-actin formation in endothelial cells (n = 3 per group). The combination of stimulated platelets and PMNs caused a further increase of F-actin polymerization. ΧP < 0.05; #P < 0.05 versus control. (C) Platelet depletion with busulfan or TP antagonist SQ 29548 prior to induction of ALI led to significant prolongation of survival compared with that of HCl-treated mice (n = 4 per group). All mice treated with a P-selectin Ab survived until termination of the experiment (300 min), as did control mice (data not shown). The HCl group was significantly different from the other groups. P = 0.0002 by log rank test.