From Steve Idell and colleagues: Dose dependency of outcomes of intrapleural fibrinolytic therapy in new rabbit empyema models

Am J Physiol Lung Cell Mol Physiol. 2016 Jun 24:ajplung.00171.2016. doi: 10.1152/ajplung.00171.2016. [Epub ahead of print]

Dose dependency of outcomes of intrapleural fibrinolytic therapy in new rabbit empyema models.

Komissarov AA1, Florova G2, Azghani AO3, Buchanan A2, Boren J4, Allen TC5, Rahman NM6, Koenig K7, Chamiso M7, Karandashova S2, Henry J7, Idell S8.

Author information

• 1The Texas Lung Injury Institute. University of Texas Health Science Center at Tyler andrey.komissarov@uthct.edu.
• 2University of Texas Health Science Center, Tyler, TX.
• 3The University of Texas at Tyler.
• 4University of Texas Health Science Center at Tyler.
• 5The University of Texas Medical Branch.
• 6Oxford University Hospitals.
• 7The Texas Lung Injury Institute of The University of Texas Health Science Center at Tyler.
• 8The University of Texas Health Center at Tyler.

Abstract

The incidence of empyema (EMP) is increasing worldwide, generally occurs with pleural loculation and impaired drainage is often treated with intrapleural fibrinolytic therapy (IPFT) or surgery. A number of IPFT options are used clinically with empiric dosing and variable outcomes in adults. To evaluate the mechanisms governing intrapleural fibrinolysis and disease outcomes, rabbit models of Pasteurella multocida and Streptococcus pneumoniae-induced EMP were generated. The animals were treated with either human tissue (tPA) plasminogen activator or prourokinase (scuPA). Rabbit EMP was characterized by the development of pleural adhesions detectable by chest ultrasonography and fibrinous coating of the pleura. Similar to human EMP, rabbits with EMP accumulated sizable; 20-40 ml fibrinopurulent pleural effusions associated with extensive intrapleural organization, significantly increased pleural thickness, suppression of fibrinolytic and plasminogen activating activities and accumulation of high levels of plasminogen activator inhibitor 1, plasminogen and extracellular DNA. IPFT with tPA (0.145 mg/kg) or scuPA (0.5 mg/kg) was ineffective in rabbit EMP (n=9 and 3 for P. multocida and S. pneumoniae, respectively). 2 mg/kg tPA or scuPA IPFT (n=5) effectively cleared S. pneumoniae-induced EMP collections in 24h with no bleeding observed. While intrapleural fibrinolytic activity for up to 40 min after IPFT was similar for effective and ineffective doses of fibrinolysin, it was lower for tPA compared to scuPA treatments. These results demonstrate the similarities between rabbit and human EMP, the importance of pleural fluid PAI-1 activity and levels of plasminogen in the regulation of intrapleural fibrinolysis and illustrate the dose dependency of IPFT outcomes in EMP.