Abstract

Rivaroxaban (BAY 59-7939) is a novel, oral, direct Factor Xa (FXa) inhibitor in advanced clinical development for the prevention and treatment of thromboembolic disorders. The antithrombotic activity of rivaroxaban has been demonstrated in several venous and arterial thrombosis models in rats, at doses that did not increase bleeding times. However, as with all anticoagulants, high doses of rivaroxaban cause prolongation of bleeding time. The aim of this study was to assess the ability of recombinant Factor VIIa (rFVIIa, NovoSeven®) to neutralize the anticoagulant effects of high-dose rivaroxaban. Animals were divided into four study groups receiving the following treatment and the appropriate placebo: rivaroxaban 2 mg/kg, rivaroxaban 2 mg/kg plus rFVIIa 100 or 400 μg/kg i.v, and rFVIIa 400 μg/kg i.v. Anesthetized rats were pretreated with rivaroxaban (or placebo); rFVIIa (or placebo) was then injected intravenously 1 minute after induction of bleeding. Mesenteric bleeding times were measured after cutting small branched arteries using microsurgery scissors, while the intestinal surface was superfused with 0.9% NaCl solution. Bleeding times were obtained from three control vessel incisions before treatment, and one after intravenous administration of rivaroxaban and/or rFVIIa (n=10). Prothrombin time (PT), thrombin generation (TG), and inhibition of FXa activity (activated by Russell's viper venom) were measured in blood from animals that had received study medication (rivaroxaban 2 mg/kg and/or rFVIIa 400 μg/kg) or placebo, but had not been used for bleeding time determination (n=6). Administration of rFVIIa (400 μg/kg) reduced mesenteric bleeding time to 0.7-times baseline (Table). High-dose rivaroxaban increased bleeding time to 3.3-times baseline. The administration of rFVIIa to animals which had received rivaroxaban significantly reduced the bleeding times to 2.4- and 1.7-times baseline at doses of 100 μg/kg and 400 μg/kg, respectively. Administration of rFVIIa (400 μg/kg) reduced PT and the lag time of TG, but had no effect on endogenous thrombin potential (ETP: total amount of thrombin activity) in control animals. Rivaroxaban-induced prolongation of PT and lag time of TG were partially reversed by rFVIIa, as was the reduction in ETP. Rivaroxaban-induced inhibition of FXa activity was not affected by rFVIIa. These results demonstrate that rFVIIa partially reverses the anticoagulation effect (bleeding time, prolongation of PT, ETP, and lag time of TG) of rivaroxaban without affecting inhibition of FXa activity. Thus, these data indicate that rFVIIa has the potential to be used as an antidote to the oral, direct FXa inhibitor, rivaroxaban, if this was necessary.GroupChange in bleeding time (x-fold)PT (sec)Thrombin generation (ETP) (nM x min)Thrombin generation lag time (min)Inhibition of FXa activity (%)Placebo1 (baseline)15±0.4516±161.2 ±0.040±3rFVIIa 400 μg/kg0.7±0.17±0.2507±190.7±0.011±4Rivaroxaban 2 mg/kg3.3±0.597±5.6363±142.4±0.277±4Rivaroxaban 2 mg/kg + rFVIIa 400 μg/kg1.7±0.254±3.5428±131.9±0.181±2ETP: endogenous thrombin potential

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