Anti-platelet drugs and outcome in severe infection: Clinical impact and underlying mechanisms

Anti-platelet drugs and outcome in severe infection: Clinical impact and underlying mechanisms

Platelet activation contributes to microvascular thrombosis and organ failure in systemic inflammation. We tested the hypothesis whether anti-platelet drugs might favourably affect outcome in patients at risk for organ failure as well as in a mouse model of endotoxin shock. Two hundred twenty-four c...

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Veröffentlicht in:Platelets (Edinburgh) 2009-01, Vol.20 (1), p.50-57
Hauptverfasser: Winning, Johannes, Reichel, Julia, Eisenhut, Yvonne, Hamacher, Jürg, Kohl, Matthias, Deigner, Hans Peter, Claus, Ralf A., Bauer, Michael, Lösche, Wolfgang
Format: Artikel
Sprache:eng
Schlagworte:
Adult
Aged
Animals
anti-platelet drugs
Cell Line
Female
Fibrin - metabolism
Gene Expression Profiling
Hemodynamics - drug effects
Humans
Infection - drug therapy
Infection - pathology
Intensive Care Units - statistics & numerical data
Length of Stay - statistics & numerical data
Leukocytes - cytology
Leukocytes - drug effects
Leukocytes - metabolism
Lung - drug effects
Lung - metabolism
Lung - pathology
Male
Mice
Mice, Inbred BALB C
Middle Aged
Oligonucleotide Array Sequence Analysis
organ failure
Platelet Activation - drug effects
Platelet Aggregation Inhibitors - pharmacology
Platelet Aggregation Inhibitors - therapeutic use
pneumonia
Pneumonia - diagnosis
Pneumonia - drug therapy
Retrospective Studies
Shock, Septic - metabolism
Shock, Septic - prevention & control
systemic inflammation
Ticlopidine - analogs & derivatives
Ticlopidine - pharmacology
Ticlopidine - therapeutic use
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Zusammenfassung:Platelet activation contributes to microvascular thrombosis and organ failure in systemic inflammation. We tested the hypothesis whether anti-platelet drugs might favourably affect outcome in patients at risk for organ failure as well as in a mouse model of endotoxin shock. Two hundred twenty-four consecutive patients who were admitted for community acquired pneumonia over a time period of 5 years to a University Hospital were enrolled; about 20% of whom received anti-platelet drugs (acetylsalicylic acid, thienopyridines) for secondary prevention of cardiovascular disease. Patients with anti-platelet drugs were about 12 years old but did not differ in SOFA score and routine laboratory parameters at admission. Logistic regression and 2 × 2 table analysis in age-matched subgroups indicated that anti-platelet drugs may reduce the need of intensive care treatment (odds ratio (OR) 0.32 [95% confidential interval: 0.10-1.00] and 0.19 [0.04-0.87], respectively). In age-matched subgroups, the use of anti-platelet drugs was also associated with a shorter stay in hospital (13.9 ± 6.2 vs. 18.2 ± 10.2 days; p < 0.02). In the animal model Balb/c mice were pre-treated with clopidogrel (added to drinking water) for 4 days prior to intraperitoneal (i.p.) administration of endotoxin (lipopolsaccharide (LPS) from Escherichia coli 0111:B4). Within the first 48 hours after LPS there were no differences between clopidogrel and control animals (n = 26 each) in macro-haemodynamics. However, clopidogrel abolished the LPS-induced drop in platelet count and reduced fibrin deposition in lung tissue. Using DNA microarray technology, we could show that clopidogrel suppressed endotoxin-induced up-regulation of inflammation-relevant genes, including arachidonate-5-lipoxygenase activating protein and leukotriene B4 receptor 1. According to our data a possible benefit of anti-platelet drugs in patients on risk for systemic inflammation and organ failure should be tested in a prospective trial.
ISSN:0953-7104
1369-1635
DOI:10.1080/09537100802503368