Anti-inflammatory actions of aprotinin provide dose-dependent cardioprotection from reperfusion injury

6533b7d7fe1ef96bd12678a7

RESEARCH PRODUCT

Anti-inflammatory actions of aprotinin provide dose-dependent cardioprotection from reperfusion injury

Axel Schlitt E Rössner Sebastian Schubert Diethard Pruefer Henning Ebelt Ute Buerke Michael Buerke Martin Russ Justin M. Carter Karl Werdan Hendrik Schmidt

subject

Pharmacology Cardioprotection Proteases Necrosis Antifibrinolytic medicine.drug_class business.industry Ischemia Pharmacology medicine.disease Apoptosis Immunology medicine Aprotinin medicine.symptom business Reperfusion injury hormones hormone substitutes and hormone antagonists medicine.drug

description

Background and purpose: Myocardial injury following ischaemia and reperfusion has been attributed to activation and transmigration of polymorphonuclear leukocytes (PMNs) with release of mediators including oxygen-derived radicals and proteases causing damage. Experimental approach: We studied the serine protease inhibitor aprotinin in an in vivo rabbit model of 1 h of myocardial ischaemia followed by 3 h of reperfusion (MI+R). Aprotinin (10 000 Ukg−1) or its vehicle were injected 5 min prior to the start of reperfusion. Key results: Myocardial injury was significantly reduced with aprotinin treatment as indicated by a reduced necrotic area (11±2.7% necrosis as percentage of area at risk after aprotinin; 24±3.1% after vehicle; P<0.05) and plasma creatine kinase activity (12.2±1.5 and 17.3±2.3 IU g−1 protein in aprotinin and vehicle groups, respectively, P<0.05). PMN infiltration (assessed by myeloperoxidase activity) was significantly decreased in aprotinin-treated animals compared to vehicle (P<0.01). Histological analysis also revealed a substantial increase in PMN infiltration following MI+R and this was significantly reduced by aprotinin therapy (44±15 vs 102±2 PMN mm2 in aprotinin vs vehicle-treated animals, P<0.05). In parallel in vitro experiments, aprotinin inhibited neutrophil-endothelium interaction by reducing PMN adhesion on isolated, activated aortic endothelium. Finally, immunohistochemical analysis illustrated aprotinin significantly reduced myocardial apoptosis following MI+R. Conclusions and implications: Inhibition of serine proteases by aprotinin inhibits an inflammatory cascade initiated by MI+R. The cardioprotective effect appears to be at least partly due to reduced PMN adhesion and infiltration with subsequently reduced myocardial necrosis and apoptosis. British Journal of Pharmacology (2008) 155, 93–102; doi:10.1038/bjp.2008.223; published online 9 June 2008

year	journal	country	edition	language
2008-09-01	British Journal of Pharmacology

https://doi.org/10.1038/bjp.2008.223