Recovery of fibrinogen concentrate after intraosseous application is equivalent to the intravenous route in a porcine model of hemodilution

Christoph J Schlimp; Cristina Solomon; Claudia Keibl; Johannes Zipperle; Sylvia Nürnberger; Wolfgang Ohlinger; Heinz Redl; Herbert Schöchl

doi:10.1097/TA.0000000000000174

Recovery of fibrinogen concentrate after intraosseous application is equivalent to the intravenous route in a porcine model of hemodilution

J Trauma Acute Care Surg. 2014 May;76(5):1235-42. doi: 10.1097/TA.0000000000000174.

Authors

Christoph J Schlimp¹, Cristina Solomon, Claudia Keibl, Johannes Zipperle, Sylvia Nürnberger, Wolfgang Ohlinger, Heinz Redl, Herbert Schöchl

Affiliation

¹ From the Ludwig Boltzmann Institute for Experimental and Clinical Traumatology (C.J.S., C.S., C.K., J.Z., W.O., H.R., H.S.), AUVA Research Centre, Vienna; and Bernhard Gottlieb University of Dentistry (S.N.), Vienna; and Department of Traumatology (S.N.), Medical University of Vienna; and AUVA Trauma Hospital of Salzburg (H.S.), Academic Teaching Hospital of the Paracelsus Medical University, Salzburg, Austria; and CSL Behring (C.S.), Marburg, Germany.

Abstract

Background: Fibrinogen concentrate is increasingly considered as a hemostatic agent for trauma patients experiencing bleeding. Placing a venous access is sometimes challenging during severe hemorrhage. Intraosseous access may be considered instead. Studies of intraosseous infusion of coagulation factor concentrates are limited. We investigated in vivo recovery following intraosseous administration of fibrinogen concentrate and compared the results with intravenous administration.

Methods: This study was performed on 12 pigs (mean [SD] body weight, 34.1 [2.8] kg). Following controlled blood loss (35 mL/kg) and fluid replacement with balanced crystalloid solution, intraosseous (n = 6) administration of fibrinogen concentrate (80 mg per kilogram of bodyweight) in the proximal tibia was compared with intravenous (n = 6) administration of the same dose (fibrinogen infusion time approximately 5 minutes in both groups). The following laboratory parameters were assessed: blood cell count, prothrombin time index, activated partial thromboplastin time, and plasma fibrinogen concentration (Clauss assay). Coagulation status was also assessed by thromboelastometry.

Results: All tested laboratory parameters were comparable between the intraosseous and intravenous groups at baseline, hemodilution, and 30 minutes after fibrinogen concentrate administration. In vivo recovery of fibrinogen was also similar in the two groups (89% [23%] and 91% [22%], respectively). There were no significant between-group differences in any of the thromboelastometric parameters. Histologic examination indicated no adverse effects on the tissue surrounding the intraosseous administration site.

Conclusion: This study suggests that intraosseous administration of fibrinogen concentrate results in a recovery of fibrinogen similar to that of intravenous administration. The intraosseous route of fibrinogen concentrate could be a valuable alternative in situations where intravenous access is not feasible or would be time consuming.

Level of evidence: Prospective, randomized, therapeutic feasibility study in an animal model, level V.

Publication types

Comparative Study
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Blood Coagulation / drug effects
Blood Loss, Surgical
Crystalloid Solutions
Disease Models, Animal
Fibrinogen / administration & dosage*
Fibrinogen / pharmacokinetics
Hemodilution / methods*
Hemorrhage / drug therapy*
Hemorrhage / mortality
Hemostatics / administration & dosage
Infusions, Intraosseous / methods*
Infusions, Intravenous
Isotonic Solutions / administration & dosage
Male
Prothrombin Time
Random Allocation
Sensitivity and Specificity
Thrombelastography

Substances

Crystalloid Solutions
Hemostatics
Isotonic Solutions
Fibrinogen