The direct, oral, factor Xa inhibitor rivaroxaban has been used in clinics for many
years. The knowledge garnered from this non-vitamin K antagonist (VKA) oral anticoagulant
(NOAC) has continued to grow since its first approval in 2008 for the prevention of
venous thromboembolism (VTE) in patients undergoing elective hip or knee replacement
surgery and subsequent approvals for prevention of stroke and systemic embolism in
adult patients with nonvalvular atrial fibrillation (NVAF), treatment and prevention
of recurrent VTE and the prevention of atherothrombotic events in adult patients following
an acute coronary syndrome (ACS). Through an extensive research program, Bayer AG
and Janssen Research & Development, LLC strive to identify—and subsequently answer—important
clinical questions that arise in thrombosis research, and the potential benefits of
rivaroxaban in wider patient populations.
It is through landmark randomized controlled trials (RCTs) such as the Phase III Cardiovascular
OutcoMes for People using Anticoagulation StrategieS (COMPASS) trial that we have
learned important lessons around the benefits of a ‘vascular’ dose of rivaroxaban
(2.5 mg twice daily [bid]) in combination with acetylsalicylic acid (ASA)—supporting
the concept of combined antithrombotic therapy with an anticoagulant and an antiplatelet
agent, to provide long-lasting vascular protection. In the setting of secondary stroke
prevention, the Phase III oPen-label, randomized, controlled, multicentre study explorIng
twO treatmeNt stratEgiEs of Rivaroxaban and a dose-adjusted oral vitamin K antagonist
treatment strategy in patients with Atrial Fibrillation who undergo Percutaneous Coronary
Intervention (PIONEER AF-PCI) trial is the first to show benefits of a NOAC (rivaroxaban
15 mg once daily [od]) + a P2Y12 inhibitor, by presenting a lower rate of clinically significant bleeding versus a
VKA + dual antiplatelet therapy, in patients with NVAF who underwent PCI with stent
placement. Moreover, this regimen has recently been approved by the European Medicines
Agency (EMA) for use in the aforementioned population for a maximum of 12 months'
duration. We have seen further novel data from the Phase III EINSTEIN CHOICE trial,
which concluded that rivaroxaban 10 mg od, when used for extended VTE treatment, reduced
the risk of recurrent VTE without significantly increasing the risk of bleeding compared
with ASA (following 6–12 months of anticoagulation). These data have subsequently
led to label updates by both the EMA and the Food and Drug Administration to include
extended prevention of recurrent VTE with rivaroxaban 10 mg od following ≥6 months
of standard anticoagulation therapy. EINSTEIN CHOICE data suggest this alternative
lower rivaroxaban dose may be a potentially valuable option for those whose benefit–risk
profile requires less intense treatment, without a compromise on clinical benefit.
These and other RCTs are summarized in the following series of articles.
Real-world data are also in abundance and allow further characterization of unmet
medical needs in the management of thrombosis. Such evaluations offer important opportunities
to generate robust data complementary to those from RCTs. Considerations around generation
of high-quality real-world data will be covered in this series, along with updates
from several real-world analyses focusing on rivaroxaban for stroke prevention in
AF. These include a pooled analysis that was performed for three prospective, observational
studies in the XArelto on preveNtion of sTroke and non-central nervoUS system systemic
embolism in patients with non-valvular atrial fibrillation (XANTUS) program, which
assessed the global safety profile of rivaroxaban in routine practice, collecting
information on AF patients in 47 countries from Western and Eastern Europe, Canada
and Israel; Asia-Pacific and Eastern Europe; and the Middle East, Africa and Latin
America. In addition, we appraise findings from a selection of country-specific datasets,
including the Danish cohort study, the REAFFIRM study (US) and the U.S. Department
of Defense Military Health Service Post-Marketing Safety Surveillance study. Even
while evaluating global patient populations using a wide variety of study designs,
we continue to see consistent benefits for rivaroxaban in AF patients in routine clinical
practice.
I anticipate that these articles will provide an interesting perspective on the comprehensive
rivaroxaban research program, which is continuously identifying novel rivaroxaban
treatment strategies in stroke prevention, vascular protection and venous protection.