Because anticoagulation is a balancing act between the prevention of clots and the risk of major bleeds, tremendous efforts have been made to find the safest, most effective drugs possible. The foundations of anticoagulant therapy – warfarin (taken orally) and heparin (taken intravenously) – are being shaken by an onslaught of the newer oral factor Xa inhibitors and a direct thrombin inhibitor.
Two of these inhibitors are currently approved by the Food and Drug Administration, with others poised for approval.
Warfarin, the current standard for outpatient oral anticoagulant therapy, leaves a lot to be desired. The need for International Normalized Ratio (INR) monitoring has made patient compliance a significant problem, as some patients must travel routinely to their doctor’s office or warfarin clinics for blood monitoring (although there has been some movement toward putting the INR-monitoring process into patient hands). Even for compliant patients, reaching and maintaining an appropriate INR can be difficult, and warfarin carries the risk of a major bleed, especially among fragile elderly patients.
But is a move from warfarin to the new drugs premature? Many concerns remain, including potential difficulties with surgery in patients taking these agents.
The two FDA-approved drugs are rivaroxaban (Xarelto, marketed by Janssen Pharmaceuticals), which is a direct factor Xa inhibitor, and dabigatran (Pradaxa, marketed by Boehringer Ingelheim), a direct thrombin inhibitor.*
Rivaroxaban (a member of the "xaban" family) was approved for two separate indications: the prevention of deep vein thrombosis in knee or hip replacement surgery (July 2011) and stroke prophylaxis in patients with nonvalvular atrial fibrillation (November 2011). Taken as a once-daily dose, the drug does not require routine blood monitoring – a key advantage over warfarin. According to the ROCKET-AF trial on which the approval was based, rivaroxaban had a major bleeding rate similar to that of warfarin; however, while it caused less bleeding into the brain, it caused more bleeding into the stomach and intestines.
During the approval process for rivaroxaban, FDA panelists questioned whether the drug was properly compared with the highest contemporary standards for warfarin and noted that it did not provide a "robust noninferiority" to dabigatran. These concerns led the panel to suggest that rivaroxaban be used only as a third-line therapy when warfarin and dabigatran are not options. Panelists also wondered what happens when patients stop using the drug. Rivaroxaban is now marketed with a boxed warning that sudden discontinuation increases the risk of stroke.
The FDA approved dabigatran in October 2010 for long-term anticoagulation in patients with atrial fibrillation, and by late August 2011, U.S. physicians had written 250,000 prescriptions for the drug.
But questions about the drug’s safety have been raised recently. In December 2011, the FDA announced that it was looking into reports of serious bleeding events associated with dabigatran, while reaffirming its belief that "the benefit of Pradaxa continues to exceed the potential risks when the drug is used appropriately."
The FDA’s concerns were prompted in part by a European Medicines Agency (EMA) safety update in November noting "a worldwide total of 256 spontaneous case reports of serious bleeding resulting in death."
In October, the EMA’s Committee for Medicinal Products for Human Use had recommended that dabigatran be labeled to advise testing for renal function in all patients before starting treatment and, for those taking the drug, renal function assessment at least once a year in patients older than 75 years and in patients of any age with a suspected decline in renal function.
A meta-analysis of seven randomized clinical trials published online in the January 2012 Archives of Internal Medicine (Arch. Intern. Med. 2012 Jan. 9 [doi:10.1001/archinternmed.2011.1666]) showed that dabigatran appeared to increase the risk of myocardial infarction and acute coronary syndrome, compared with warfarin, enoxaparin, and placebo. The incidence of these events was 1.19% in those taking dabigatran vs. 0.79% in the controls.
Another new anticoagulant, apixaban, has been approved as Eliquis in the European Union and fast-tracked for approval in the United States. Apixaban outperformed warfarin in the ARISTOTLE trial in preventing stroke, reducing bleeding, and increasing survival, regardless of how well controlled patients were on warfarin, dabigatran, and rivaroxaban. Results achieved with apixaban were better than those seen in the trials of dabigatran and rivaroxaban against warfarin (N. Engl. J. Med 2011;365:981-92).
Of particular interest is apixaban’s good bleeding profile, compared with those of the other drugs (N. Engl. J. Med. 2011;364:806-17). "We have two trials in a large program showing this safety. In AVERROES, the bleeding risk with apixaban was the same as with low-dose aspirin," Dr. Lars Wallentin said in an interview. Dr. Wallentin is professor and head of cardiology research at Uppsala (Sweden) University and a coinvestigator in the ARISTOTLE trial.