Reversal of Heparin Anticoagulation by Recombinant Platelet Factor 4 in Humans

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Circulation. 1995;91:2188-2194

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(Circulation. 1995;91:2188-2194.)
© 1995 American Heart Association, Inc.

Articles

Reversal of Heparin Anticoagulation by Recombinant Platelet Factor 4 in Humans

Gregory J. Dehmer, MD; Melrose Fisher, RN, BSN; David A. Tate, MD; Steve Teo, PhD; Eric M. Bonnem, MD

From the C.V. Richardson Cardiac Catheterization Laboratory of the University of North Carolina Hospitals and the Cardiology Division of the University of North Carolina at Chapel Hill.

Correspondence to Gregory J. Dehmer, MD, Director, Cardiac Catheterization Laboratory, University of North Carolina Hospitals, 101 Manning Dr, Chapel Hill, NC 27514.

Background Protamine is used to reverse the anticoagulant effectsof heparin, but it can have important side effects. Platelet factor4 (PF4) is a protein found in platelet alpha granules that binds toand thereby neutralizes heparin. We evaluated the safety and effectivenessof intravenous recombinant PF4 to neutralize heparin anticoagulationafter cardiac catheterization in a phase 1, open-label trial.

Methods and Results The study group consisted of 18 patients havingdiagnostic cardiac catheterization. Heparin (5000 U) was given aftervascular access was obtained. In the first 12 patients, additionalheparin was given at the conclusion of the procedure so that allpatients had activated coagulation times >300 seconds beforerPF4 was given. Three patients each received 0.5, 1.0, 2.5,or 5.0 mg/kg rPF4 over a period of 3 minutes at the conclusionof the catheterization procedure. In 6 additional patients,extra heparin was not given at the conclusion of the procedure,and 1.0 mg/kg rPF4 was given. Hemodynamic measurements, cardiacoutput, and serial blood tests were performed 5, 10, 20, and30 minutes after rPF4 and then into the next 24 hours. Therewere no serious side effects in any patient, despite transientrPF4 levels as high as 14 870 ng/mL in the patients receiving5.0 mg/kg. One patient receiving 2.5 mg/kg had a slight transientrise in liver enzymes possibly related to the rPF4. There wereno important hemodynamic effects of rPF4 administration at any doseused. Doses of 2.5 and 5.0 mg/kg were uniformly effective in reversingthe anticoagulant effect of heparin. At lower doses, rPF4 neutralizedthe effects of heparin in most but not all patients. Pharmacokineticanalysis suggested a monophasic and one-compartment clearanceof the PF4-heparin complex. No neutralizing factors to rPF4 weredetected in the samples collected 7 days after dosing.

Conclusions rPF4, in doses ranging from 0.5 to 5.0 mg/kg over3 minutes, had no serious side effects. Given in sufficientamounts, rPF4 can completely and rapidly reverse the anticoagulanteffects of heparin.

Key Words: angiography • anticoagulants • heparin • cardiopulmonary bypass • platelet-derived factors

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