ENOXAPARIN SUPPRESSES THROMBIN FORMATION AND ACTIVITY DURING CARDIOPULMONARY BYPASS IN BABOONS

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ENOXAPARIN SUPPRESSES THROMBIN FORMATION AND ACTIVITY DURING CARDIOPULMONARY BYPASS IN BABOONS

Nicolas Gikakis, BSE^a, A. Koneti Rao, MD^b, Shinji Miyamoto, MD^a, Joseph H. Gorman III, MD^a, Mohammed M. H. Khan, MD^b, Harry L. Anderson, MD^a, C. Eric Hack, PhD^c, Ling Sun, MD^b, Stefan Niewiarowski, MD, PhD^b, Robert W. Colman, MD^b, L. Henry Edmunds, Jr, MD^a

Supported by HL47186 from the National Heart Lung Blood Institute, National Institutes of Health, Bethesda, Md.

Received for publication Feb 12, 1998. Revisions requested April 15, 1998; revisions received July 14, 1998. Accepted for publication July 21, 1998. Address for reprints: L. Henry Edmunds, Jr, MD, Department of Surgery, Hospital of the University of Pennsylvania, Six Silverstein, 3400 Spruce St, Philadelphia, PA 19104.

Objective:This study tests the hypotheses that enoxaparin, alow molecular weight heparin and potent inhibitor of factorXa, alone or in combination with standard heparin, inhibitsthrombin formation and activity and modulates complement activationand neutrophil elastase release during cardiopulmonary bypassin baboons.
Methods: After preliminary studies to determinedoses and possible species differences to anticoagulants andprotamine, 27 anesthesized baboons had normothermic cardiopulmonarybypass with standard, unfractionated, porcine intestinal heparin,enoxaparin, or a combination of heparin and enoxaparin. Protaminein appropriate doses was used to reverse anticoagulation. Bloodsamples were obtained at 6 time points. Activated clotting timeswere monitored; template bleeding times were measured beforeand up to 24 hours after cardiopulmonary bypass.
Results: Hemodynamicmeasurements were not affected by the anticoagulant. Activatedclotting times remained above 400 seconds throughout bypass,and no clots were observed. The anticoagulant did not alterplatelet count, aggregation to adenosine diphosphate, releaseof ß-thromboglobulin, release of neutrophil elastase,or complement C3b/c and C4b/c. Enoxaparin alone, but not incombination, significantly reduced plasma levels of prothrombinfragment F1.2, fibrinopeptide A, and thrombin-antithrombin complexesbut prolonged template bleeding times for more than 24 hours.
Conclusion: Enoxaparin significantly reduces thrombin formationand activity during cardiopulmonary bypass but does not suppresscomplement activation and neutrophil elastase release and isnot adequately reversed by protamine after bypass.

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CARDIOPULMONARY SUPPORT AND PHYSIOLOGY

ENOXAPARIN SUPPRESSES THROMBIN FORMATION AND ACTIVITY DURING CARDIOPULMONARY BYPASS IN BABOONS