Anticoagulants (Thrombin Inhibitors) and Aspirin Synergize With P2Y 12 Receptor Antagonism in Thrombosis

Author:

André Patrick1,LaRocca Thomas1,Delaney Suzanne M.1,Lin Pei Hua1,Vincent Diana1,Sinha Uma1,Conley Pamela B.1,Phillips David R.1

Affiliation:

1. From Millennium Pharmaceuticals, Inc, South San Francisco, Calif.

Abstract

Background— This study was designed to determine whether (1) P2Y 12 antagonism synergizes with other antithrombotics and (2) anticoagulants (thrombin inhibitors) affect the antithrombotic activity elicited by P2Y 12 antagonism. Methods and Results— Thrombosis was achieved by perfusion of human and murine blood through type III collagen–coated capillaries at arterial shear rate. CT50547, a direct-acting P2Y 12 antagonist, inhibited thrombosis in PPACK- but not heparin-anticoagulated human blood. In contrast, CT50547 inhibited thrombosis in aspirin-treated individuals independently of the anticoagulant. Thrombin and TXA 2 also synergized with P2Y 12 in the absence of anticoagulation, because combined treatment of aspirin or C921-78 (a factor Xa inhibitor) with CT50547 or 2-MeSAMP (a P2Y 12 antagonist) inhibited the thrombotic process, whereas all treatments failed to inhibit thrombosis when used individually. Synergism was also observed ex vivo when P2Y 12 -deficient (P2Y 12 −/− ) mice were administered aspirin or coagulation inhibitors (C921-78 and bivalirudin). Finally, using intravital microscopy, we found that both C921-78 and bivalirudin abrogated the thrombotic process in P2Y 12 +/ mice, whereas each showed only partial efficacy in P2Y 12 +/+ animals. Conclusions— Our study indicates that (1) thrombin inhibitors and aspirin have a demonstrable synergy of antithrombotic activity with P2Y 12 antagonism and (2) the in vitro analysis of the antithrombotic activity of P2Y 12 antagonists is affected by the anticoagulant used for blood collection. This suggests that the antithrombotic potential of P2Y 12 antagonists in vitro may be overestimated in anticoagulated samples of blood and best achieved in vivo by the inclusion of aspirin and/or a thrombin inhibitor.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Physiology (medical),Cardiology and Cardiovascular Medicine

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