Journalartikel

ENDOTOXIN PRIMING POTENTIATES LUNG VASCULAR ABNORMALITIES IN RESPONSE TO ESCHERICHIA-COLI HEMOLYSIN - AN EXAMPLE OF SYNERGISM BETWEEN ENDOTOXIN AND EXOTOXIN


AutorenlisteWALMRATH, D; Ghofrani, Hossein-Ardeschir; ROSSEAU, S; SCHUTTE, H; CRAMER, A; KADDUS, W; Grimminger, Friedrich; BHAKDI, S; Seeger, Werner

Jahr der Veröffentlichung1994

Seiten1437-1443

ZeitschriftJournal of Experimental Medicine

Bandnummer180

Heftnummer4

ISSN0022-1007

Open Access StatusGreen

DOI Linkhttps://doi.org/10.1084/jem.180.4.1437

VerlagRockefeller University Press


Abstract
The pore-forming hemolysin of Escherichia coli (HlyA), an important virulence factor in extraintestinal E. coli infections, causes thromboxane generation and related vasoconstriction in perfused rabbit lungs (Seeger, W., H. Waiter, N. Suttorp, M. Muhly, and S. Bhakdi. 1989. J. Clin. Invest, 84:220). We investigated the influence of pulmonary vascular ''priming'' with endotoxin on the responsiveness of the lung to a low-dose HlyA challenge. Rabbit lungs were perfused with Krebs Henseleit buffer containing 0.1-100 ng/ml Salmonella abortus equii lipopolysaccharide (LPS) for 60-180 min. This treatment caused protracted release of tumor necrosis factor into the recirculating medium, but did not induce significant alterations of pulmonary hemodynamics and fluid balance. At a dose of 1 ng/ml, HlyA elicited only moderate thromboxane release (<200 pg/ml) and pulmonary artery pressure increase (less than or equal to 6 mmHg) in control lungs. Acceleration and potentiation of both the metabolic and vasoconstrictor response occurred in lungs primed with LPS. This priming effect displayed dose (threshold similar to 0.1-1 ng/ml LPS) and time dependencies (threshold similar to 60-90 min LPS incubation). Maximum thromboxane release and pulmonary artery pressure increase surpassed the responses to HlyA in nonprimed lungs by more than 15-fold. Cyclooxygenase inhibition and thromboxane-receptor antagonism blocked these effects. These data demonstrate that LPS priming synergizes with HlyA challenge to provoke vascular abnormalities that are possibly relevant to the pathogenesis of organ failure in severe local and systemic infections.



Zitierstile

Harvard-ZitierstilWALMRATH, D., Ghofrani, H., ROSSEAU, S., SCHUTTE, H., CRAMER, A., KADDUS, W., et al. (1994) ENDOTOXIN PRIMING POTENTIATES LUNG VASCULAR ABNORMALITIES IN RESPONSE TO ESCHERICHIA-COLI HEMOLYSIN - AN EXAMPLE OF SYNERGISM BETWEEN ENDOTOXIN AND EXOTOXIN, Journal of Experimental Medicine, 180(4), pp. 1437-1443. https://doi.org/10.1084/jem.180.4.1437

APA-ZitierstilWALMRATH, D., Ghofrani, H., ROSSEAU, S., SCHUTTE, H., CRAMER, A., KADDUS, W., Grimminger, F., BHAKDI, S., & Seeger, W. (1994). ENDOTOXIN PRIMING POTENTIATES LUNG VASCULAR ABNORMALITIES IN RESPONSE TO ESCHERICHIA-COLI HEMOLYSIN - AN EXAMPLE OF SYNERGISM BETWEEN ENDOTOXIN AND EXOTOXIN. Journal of Experimental Medicine. 180(4), 1437-1443. https://doi.org/10.1084/jem.180.4.1437



Schlagwörter

ARACHIDONIC-ACIDBACTERIAL LIPOPOLYSACCHARIDESCELL-MEMBRANESENHANCED PRODUCTIONHUMAN-MONOCYTESHUMAN-NEUTROPHILSPROTEIN KINASE-CRABBIT LUNGS


Nachhaltigkeitsbezüge

Zuletzt aktualisiert 2025-30-09 um 09:05