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

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.