Bleeding Clinical Trial
Official title:
Cardiac Surgery : In Vivo Titration of Protamine
Safe use of cardiopulmonary bypass (CPB) requires massive doses of intravenous
unfractionated heparin. At end-CPB, residual heparin is neutralized with intravenous
injection of protamine sulfate. This prospective, randomized, controlled study will be
conducted in 82 voluntary subjects admitted for elective, first intention, cardiac surgery
requiring cardiopulmonary bypass. Each will be randomly assigned to one of two groups. The
control group will be submitted to a standard protamine infusion of 1.3mg :100U of the total
heparin dose given during bypass. The test group will receive an infusion of protamine (over
15 minutes) until activated clotting time (ACT) values (determined every 3 minutes) depict a
plateau, sign that the optimal protamine to heparin ratio has been attained. The
investigators hypothesize this new in vivo titration method to be as efficient as the
standard protocol (adequacy of heparin neutralization, % heparin rebound, bleeding, and
transfusion), and potentially safer by its ability to prevent protamine overdose and its
deleterious impact on platelet function.15
Principal Objective
Evaluate a new in vivo method of titration of protamine sulfate.
Secondary Objective
Evaluate the impact of this method on the adequacy of heparin neutralization by measuring:
1. platelet count
2. postoperative bleeding
3. transfusion exposure a
4. incidence of heparin rebound
Protamine sulfate is administered to reverse the anticoagulant effects of heparin upon completion of cardiopulmonary bypass (CPB). In most cases, protamine is given in amounts sufficient to neutralize the total dose of heparin.9 This dose is usually calculated with a ratio of 1.3mg protamine for every 100U heparin given.10 In the literature, reported doses of intraoperatively administered protamine range from 0 to 8mg per 100U of heparin. Given in excess, protamine can, in addition to complement activation and hemodynamic instability,11 induce platelet dysfunctions.12-16 The latter significantly increases both the cost and morbidity of cardiac interventions as it is one of the main causes of postoperative bleeding. The optimal protamine/heparin ratio is difficult to individualize for each patient because of the great interpatient variability in heparin's metabolism4-7 and of the absence of correlation between ACT and heparin's plasma concentration.8 Consumption of heparin may vary from 0.01 to 3.86U/Kg per minute during CPB.30 The exact concentration of remaining circulating heparin at the end of bypass is not easily obtained. ;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Investigator), Primary Purpose: Treatment
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