Abstract
Haemostatic balance shifts towards pro-coagulation during infection. Plasminogen, a key molecule of fibrinolysis, may play an important role in the pathogenesis of staphylococcal infections. In the present study, we assessed the impact of inhibition of plasminogen activation by tranexamic acid on the course of staphylococcal sepsis and septic arthritis in mice. We found significantly down-regulated plasmin activity and increased D-dimer levels in the blood from the mice with staphylococcal sepsis. Treatment with tranexamic acid significantly increased the severity and mortality of staphylococcal infection. In addition, tranexamic acid reduced the survival rate in a murine model for staphylococcal enterotoxin A-induced death. The aggravation of diseases by tranexamic acid was due neither to the pro-inflammatory cytokine network, nor to impairment of bacterial clearance. Modulation of fibrinolysis, either by supplement of fibrinolytic molecules (tissue plasminogen activator or plasmin) or by fibrinogen depletion, did not reduce the mortality of staphylococcal sepsis. In conclusion, we report that treatment with tranexamic acid led to distinct aggravation of staphylococcal septic arthritis and sepsis in mice, suggesting the clinical importance of fibrinolytic balance in staphylococcal infection.
Acknowledgements
This study was approved by the Ethics Committee of Sahlgrenska Hospital. The work was supported by the Göteborg Medical Society, Swedish Association against Rheumatism, King Gustaf V Foundation, Swedish Medical Research Council, Nanna Svartz Foundation, Swedish National Inflammation Network, Stiftelsen Familjen Thöléns och Kristlers Donationsfond, Reumatikerföreningen i Göteborg, and the University of Göteborg.
Declaration of interest: We do not have any commercial associations that might pose a conflict of interest.