| pathology | Demonstrated benefit and harm | k | | | |
|---|
| acute coronary syndrome | versus placebo or control No demonstrated result for efficacy rivaroxaban 2.5mg inferior to placebo in terms of major bleeding in ATLAS ACS 2 - TIMI 51 (2.5mg), 2011 rivaroxaban 2.5mg inferior to placebo in terms of ISTH major or clinically relevant nonmajor bleeding in ATLAS ACS 2 - TIMI 51 (2.5mg), 2011 rivaroxaban 2.5mg inferior to placebo in terms of any bleeding in ATLAS ACS 2 - TIMI 51 (2.5mg), 2011 rivaroxaban 2.5mg inferior to placebo in terms of major or minor bleeding in ATLAS ACS 2 - TIMI 51 (2.5mg), 2011 rivaroxaban 5mg inferior to placebo in terms of major bleeding in ATLAS ACS 2 - TIMI 51 (5mg), 2011 rivaroxaban 5mg inferior to placebo in terms of ISTH major or clinically relevant nonmajor bleeding in ATLAS ACS 2 - TIMI 51 (5mg), 2011 rivaroxaban 5mg inferior to placebo in terms of any bleeding in ATLAS ACS 2 - TIMI 51 (5mg), 2011 rivaroxaban 5mg inferior to placebo in terms of major bleeding in ATLAS ACS-TIMI 46 (5mg), 2009 rivaroxaban 5mg inferior to placebo in terms of ISTH major or clinically relevant nonmajor bleeding in ATLAS ACS-TIMI 46 (5mg), 2009 | 4 trials | meta-analysis | | | Trial | control | p<0.05 | harm | NS |
|---|
| ATLAS ACS 2 - TIMI 51 (2.5mg), 2011 | rivaroxaban 2.5mg vs placebo | death 0.67 [0.53; 0.86] cardiovascular death 0.66 [0.51; 0.85] Cardiovascular death, MI, or stroke
0.83 [0.72; 0.96] | major bleeding 3.43 [2.06; 5.71] ISTH major or clinically relevant nonmajor bleeding 1.75 [1.52; 2.01] any bleeding 1.75 [1.52; 2.01] major or minor bleeding 1.75 [1.52; 2.01] | fatal bleeding 0.67 [0.24; 1.88] MI 0.90 [0.74; 1.08] | | ATLAS ACS 2 - TIMI 51 (5mg), 2011 | rivaroxaban 5mg vs placebo | death 0.42 [0.33; 0.53] cardiovascular death 0.42 [0.33; 0.53] MI 0.53 [0.45; 0.63] Cardiovascular death, MI, or stroke
0.50 [0.44; 0.57] | major bleeding 4.33 [2.63; 7.12] ISTH major or clinically relevant nonmajor bleeding 2.27 [1.98; 2.59] any bleeding 2.27 [1.98; 2.59] | fatal bleeding 1.67 [0.73; 3.82] | | ATLAS ACS-TIMI 46 (5mg), 2009 | rivaroxaban 5mg vs placebo | | major bleeding 17.64 [2.34; 132.76] ISTH major or clinically relevant nonmajor bleeding 3.36 [2.21; 5.10] | Cardiovascular death, MI, or stroke
0.63 [0.39; 1.01] | | ATLAS ACS-TIMI 46 (2.5mg), 2009 | rivaroxaban 2.5mg vs placebo | | | major bleeding 3.76 [0.24; 59.88] Cardiovascular death, MI, or stroke
0.52 [0.23; 1.19] death, MI, stroke, recurrent ischaemia 0.60 [0.29; 1.25] ISTH major or clinically relevant nonmajor bleeding 1.71 [0.76; 3.85] |
| Trial | Treatments | Patients | Method |
|---|
| ATLAS ACS 2 - TIMI 51 (2.5mg), 2011 | rivaroxaban 2.5 mg twice daily in addition to standard care (n=5174) vs. placebo (n=5176) 3 arms: rivaroxaban (2.5 mg twice daily or 5 mg twice daily) in addition to standard care and placebo | patients with a recent ACS | double blind Parallel groups Sample size: 5174/5176 Primary endpoint: CV death, MI, stroke FU duration: 13 months | | ATLAS ACS 2 - TIMI 51 (5mg), 2011 | rivaroxaban 5 mg twice daily in addition to standard care
(n=5176) vs. placebo
(n=5176) 3 arms: rivaroxaban (2.5 mg twice daily or 5 mg twice daily) in addition to standard care and placebo
| patients with a recent ACS
| double blind Sample size: 5176/5176 Primary endpoint: CV death, MI, stroke FU duration: 13 months
| | ATLAS ACS-TIMI 46 (5mg), 2009 | rivaroxaban 5 mg twice daily
(n=519) vs. placebo
(n=1160) dose finding study: rivaroxaban 5 mg, 10 mg, or 20 mg once daily, 2.5 mg, 5 mg, or 10 mg twice daily and placebo
| recent ACS patients treated with aspirin alone (n=761) or aspirin plus clopidogrel (n=2730)
| double blind Parallel groups Sample size: 519/1160 Primary endpoint: clinically significant bleeding FU duration: 6 months dose-finding study
| | ATLAS ACS-TIMI 46 (2.5mg), 2009 | rivaroxaban 2.5 mg twice daily
(n=152) vs. placebo
(n=1160) dose finding study: rivaroxaban 5 mg, 10 mg, or 20 mg once daily, 2.5 mg, 5 mg, or 10 mg twice daily and placebo
| recent ACS patients treated with aspirin alone (n=761) or aspirin plus clopidogrel (n=2730)
| double blind Sample size: 152/1160 Primary endpoint: clinically significant bleeding FU duration: 6 months dose-finding study
|
|
| atrial fibrillation | versus anticoagulant No demonstrated result for efficacy rivaroxaban inferior to warfarin standard dose in terms of Gastrointestinal major bleeding in ROCKET-AF, 2010 | 2 trials | meta-analysis | | | Trial | control | p<0.05 | harm | NS |
|---|
| ROCKET-AF, 2010 | rivaroxaban vs warfarin standard dose | haemorragic stroke(or intracerebral hemorrhage) 0.58 [0.38; 0.89] fatal bleeding 0.50 [0.31; 0.80] Life threatening major bleeding 0.69 [0.53; 0.89] | Gastrointestinal major bleeding 1.46 [1.19; 1.78] | vascular death,TIA,nonfatal stroke or systemic embolism 0.94 [0.84; 1.05] all death 0.92 [0.82; 1.03] coronary events 0.80 [0.62; 1.04] vascular death 0.94 [0.81; 1.09] major bleeding 1.04 [0.90; 1.20] fatal stroke(ischemic+hemorrhagic) 0.70 [0.49; 1.02] thrombo-embolic event (cerebral or systemic) 0.88 [0.75; 1.04] ischemic stroke 0.99 [0.82; 1.20] All stroke(ischemic+hemorrhagic/fatal+non fatal) 0.84 [0.69; 1.01] major and clinically relevant non-major bleeding 1.03 [0.96; 1.11] systemic thrombo-embolic complication 0.74 [0.42; 1.31] | | ROCKET (2nd prevention subgroup) , 2011 | rivaroxaban vs warfarin | | | thromboembolic event(cerebral or systemic) 0.98 [0.80; 1.19] thromboembolic event*(TE event or ischemic stroke or systemic thromboembolic event) 0.98 [0.80; 1.19] |
| Trial | Treatments | Patients | Method |
|---|
| ROCKET-AF, 2010 | Rivaroxaban 20mg p.o. once daily (n=7131) vs. Warfarin p.o. once daily titrated to a target INR of 2.5 (range 2.0 to 3.0, inclusive) (n=7133) | Subjects With Non-Valvular Atrial Fibrillation | double blind Parallel groups Sample size: 7131/7133 Primary endpoint: stroke or non-CNS systemic embolism FU duration: median 1.94 y | | ROCKET (2nd prevention subgroup) , 2011 | rivaroxaban (n=3892) vs. warfarin INR 2-3 (n=3875) | patients with a prior stroke or transient ischemic attack | double-blind Parallel groups Sample size: 3892/3875 Primary endpoint: FU duration: |
|
| cardiovascular prevention | versus No demonstrated result for efficacy rivaroxaban + aspirin inferior to aspirin in terms of major bleeding in COMPASS (rivaroxaban + aspirin), 2017 (secondary prevention patients) rivaroxaban + aspirin inferior to aspirin in terms of CV events in COMPASS (rivaroxaban + aspirin), 2017 (secondary prevention patients) rivaroxaban + aspirin inferior to aspirin in terms of all causes deaths in COMPASS (rivaroxaban + aspirin), 2017 (secondary prevention patients) rivaroxaban + aspirin inferior to aspirin in terms of CV death (IHD+stroke) in COMPASS (rivaroxaban + aspirin), 2017 (secondary prevention patients) rivaroxaban + aspirin inferior to aspirin in terms of fatal stroke in COMPASS (rivaroxaban + aspirin), 2017 (secondary prevention patients) rivaroxaban + aspirin inferior to aspirin in terms of ischemic stroke in COMPASS (rivaroxaban + aspirin), 2017 (secondary prevention patients) rivaroxaban + aspirin inferior to aspirin in terms of all stroke in COMPASS (rivaroxaban + aspirin), 2017 (secondary prevention patients) | 2 trials | meta-analysis | | | Trial | control | p<0.05 | harm | NS |
|---|
| COMPASS (rivaroxaban alone), 2017 | rivaroxaban vs aspirin | | | | | COMPASS (rivaroxaban + aspirin), 2017 | rivaroxaban + aspirin vs aspirin | | major bleeding 17.00 [6.50; 44.44] CV events 76.00 [66.58; 86.75] all causes deaths 82.00 [70.52; 95.35] CV death (IHD+stroke) 78.00 [63.69; 95.53] fatal stroke 78.00 [63.69; 95.53] ischemic stroke 51.00 [38.12; 68.22] all stroke 58.00 [44.13; 76.23] | |
| Trial | Treatments | Patients | Method |
|---|
| COMPASS (rivaroxaban alone), 2017 | Rivaroxaban 2.5 mg twice daily alone (n=27400) vs. aspirin 100 mg once daily (n=0) 3 arms rivaroxaban and aspirin, rivaroxaban alone, aspirin alone | Patients With Coronary or Peripheral Artery Disease | Sample size: 27400/0 Primary endpoint: FU duration: | | COMPASS (rivaroxaban + aspirin), 2017 | rivaroxaban (2.5 mg twice daily) plus aspirin (100 mg once daily) (n=9152) vs. aspirin 100 mg once daily
(n=9126) 3 arms rivaroxaban and aspirin, rivaroxaban alone, aspirin alone
| Patients With Coronary or Peripheral Artery Disease
| double-blind Parallel groups Sample size: 9152/9126 Primary endpoint: cardiovascular death, stroke, MI FU duration: 23 months
|
|
| heart failure | versus No demonstrated result for efficacy | 1 trial | meta-analysis | | | Trial | control | p<0.05 | harm | NS |
|---|
| COMMANDER HF, 2018 | rivaroxaban vs placebo | | | death 0.98 [0.87; 1.10] |
| Trial | Treatments | Patients | Method |
|---|
| COMMANDER HF, 2018 | rivaroxaban at a dose of 2.5 mg twice daily (n=2507) vs. placebo (n=2515) | patients who had chronic heart failure, a left ventricular ejection fraction of 40% or less, coronary artery disease, and elevated plasma concentrations of natriuretic peptides and who did not have atrial fibrillation | Sample size: 2507/2515 Primary endpoint: death all cause, MI, stroke FU duration: 21.1 months |
|
| post stroke | versus No demonstrated result for efficacy | 1 trial | meta-analysis | | | Trial | control | p<0.05 | harm | NS |
|---|
| NAVIGATE ESUS, 2018 | rivaroxaban vs aspirin | | | |
| Trial | Treatments | Patients | Method |
|---|
| NAVIGATE ESUS, 2018 | rivaroxaban (at a daily dose of 15 mg) (n=3609) vs. aspirin (at a daily dose of 100 mg) (n=3604) | patients with recent ischemic stroke that was presumed to be from cerebral embolism but without arterial stenosis, lacune, or an identified cardioembolic source | Sample size: 3609/3604 Primary endpoint: first recurrence of ischemic or hemorrhagic stroke or systemic embolism FU duration: |
|
| pulmonary embolism | versus heparin/VKA No demonstrated result for efficacy | 1 trial | meta-analysis | | | Trial | control | p<0.05 | harm | NS |
|---|
| Einstein-PE Evaluation, 2012 | rivaroxaban (without LMWH) vs LMWH/VKA | | | |
| Trial | Treatments | Patients | Method |
|---|
| Einstein-PE Evaluation, 2012 | rivaroxaban (15 mg twice daily for 3 weeks, followed by 20 mg once daily) for 3, 6, or 12 months (n=2419) vs. standard therapy with enoxaparin followed by an adjusted-dose vitamin
K antagonist (n=2413) | patients
who had acute symptomatic pulmonary embolism with or without deep-vein thrombosis | open Parallel groups Sample size: 2419/2413 Primary endpoint: symptomatic recurrent venous thromboembolism FU duration: 9.8 months |
|
| thrombosis prevention | versus No demonstrated result for efficacy rivaroxaban inferior to placebo in terms of Clinically relevant bleeding in MARINER, 2018 (medical patients patients) | 1 trial | meta-analysis | | | Trial | control | p<0.05 | harm | NS |
|---|
| MARINER, 2018 | rivaroxaban vs placebo | Symptomatic deep vein thrombosis during follow-up 0.44 [0.22; 0.88] Venous thromboembolism or death 0.73 [0.54; 0.98] | Clinically relevant bleeding 1.66 [1.17; 2.35] | All-cause death during follow-up 0.80 [0.58; 1.10] Major bleeding during follow-up 1.88 [0.84; 4.22] VTE 0.76 [0.52; 1.10] |
| Trial | Treatments | Patients | Method |
|---|
| MARINER, 2018 | once-daily rivaroxaban at a dose of 10 mg (with the dose adjusted for renal insufficiency) , begun at hospital discharge and continued for 45 days (n=6007) vs. placebo (n=6012) | high-risk medical patients : medically ill patients who were at increasedrisk for venous thromboembolism on the basis of a modified International Medical Prevention Registry on Venous Thromboembolism (IMPROVE) score of 4 or higher (scores range from 0 to 10, with higher scores indicating a higher risk of venous thromboembolism) or a score of 2 or 3 plus a plasma d-dimer level of more than twice the upper limit of the normal range (defined according to local laboratory criteria) | double blind Sample size: 6007/6012 Primary endpoint: symptomatic venous thromboembolism or death due to venous thromboembolism FU duration: |
|
| thrombosis prevention | versus Low molecular weight heparin No demonstrated result for efficacy | 6 trials | meta-analysis | | | Trial | control | p<0.05 | harm | NS |
|---|
| ODIXa-HIP 10mg, 2006 | rivaroxaban vs enoxaparin (short duration) | DVT (asymptomatic or symptomatic) 0.42 [0.22; 0.79] distal DVT 0.36 [0.17; 0.73] total VTE and all-cause mortality 0.42 [0.22; 0.79] | | proximal DVT 0.95 [0.20; 4.59] non-fatal PE NaN [NaN; NaN] | | ODIXa-KNEE, 2005 | rivaroxaban vs enoxaparin (US regimen) | | | major bleeding 0.00 [0.00; NaN] | | RECORD 1, 2008 | rivaroxaban vs enoxaparin | DVT (asymptomatic or symptomatic) 0.23 [0.12; 0.43] proximal DVT 0.03 [0.00; 0.23] total VTE and all-cause mortality 0.30 [0.18; 0.51] major VTE (fatal and non fatal DVT,PE) 0.12 [0.04; 0.34] | | death 0.98 [0.24; 3.90] coronary events 0.49 [0.12; 1.95] major bleeding 3.02 [0.61; 14.95] distal DVT 0.49 [0.24; 1.00] non-fatal PE 3.91 [0.44; 34.92] Symptomatic venous thromboembolism 0.55 [0.20; 1.48] | | RECORD 2, 2008 | rivaroxaban (long duration) vs enoxaparin (short duration) | DVT (asymptomatic or symptomatic) 0.20 [0.11; 0.35] proximal DVT 0.11 [0.05; 0.29] distal DVT 0.34 [0.16; 0.71] total VTE and all-cause mortality 0.21 [0.13; 0.35] Symptomatic venous thromboembolism 0.20 [0.06; 0.69] major VTE (fatal and non fatal DVT,PE) 0.12 [0.05; 0.28] | | death 0.34 [0.07; 1.66] coronary events 1.33 [0.30; 5.95] major bleeding 1.00 [0.06; 15.98] non-fatal PE 0.25 [0.03; 2.25] major or clinically relevant non-major bleeding 1.20 [0.93; 1.54] | | RECORD 3, 2008 | rivaroxaban vs enoxaparin (europe regimen) | DVT (asymptomatic or symptomatic) 0.53 [0.41; 0.68] distal DVT 0.53 [0.41; 0.70] total VTE and all-cause mortality 0.51 [0.39; 0.65] Symptomatic venous thromboembolism 0.34 [0.15; 0.75] major VTE (fatal and non fatal DVT,PE) 0.38 [0.18; 0.82] | | death 0.00 [0.00; NaN] coronary events 0.51 [0.05; 5.59] major bleeding 1.19 [0.40; 3.53] myocardial infarction 0.51 [0.05; 5.61] proximal DVT 0.48 [0.22; 1.05] non-fatal PE 0.00 [0.00; NaN] | | RECORD 4, 2009 | rivaroxaban vs enoxaparin (US regimen) | proximal DVT 0.23 [0.07; 0.80] total VTE and all-cause mortality 0.69 [0.51; 0.92] | | death 0.66 [0.11; 3.94] coronary events 0.33 [0.03; 3.16] major bleeding 2.47 [0.78; 7.86] myocardial infarction 0.20 [0.02; 1.69] distal DVT 0.82 [0.57; 1.17] non-fatal PE 0.49 [0.15; 1.64] asymptomatic DVT 0.72 [0.51; 1.01] Symptomatic venous thromboembolism 0.60 [0.29; 1.27] major VTE (fatal and non fatal DVT,PE) 0.59 [0.30; 1.16] symptomatic DVT 0.60 [0.22; 1.63] major or clinically relevant non-major bleeding 1.34 [0.86; 2.07] |
| Trial | Treatments | Patients | Method |
|---|
| ODIXa-HIP 10mg, 2006 | rivaroxaban 10mg daily for 5–9 days (n=142) vs. once-daily subcutaneous enoxaparin dose of 40 mg for 5–9 days (n=157) dose finding study (doses of 5, 10, 20, 30, or 40 mg) | patients undergoing elective total hip replacement | double blind Parallel groups Sample size: 142/157 Primary endpoint: any DVT, PE, all cause death FU duration: 5-9 days | | ODIXa-KNEE, 2005 | BAY 59-7939 5mg b.i.d. for 5–9 days (n=102) vs. enoxaparin 30 mg b.i.d. for 5–9 days (n=105) dose ranging study with doses 2.5, 5, 10, 20, and 30 mg | patients undergoing elective total knee replacement | double blind Parallel groups Sample size: 102/105 Primary endpoint: FU duration: 5-9 days | | RECORD 1, 2008 | rivaroxaban 10mg once daily for 35 days (n=2266) vs. enoxaparin 40mg subcutaneous once daily for 31-39 days (n=2275) | patients undergoing total hip arthroplasty | double blind Parallel groups Sample size: 2266/2275 Primary endpoint: DVT, PE, death FU duration: 36 days (range 30-42) | | RECORD 2, 2008 | extended thromboprophylaxis with rivaroxaban 10mg once daily for 31-39 days (n=1252) vs. enoxaparin 40mg subcutaneous once daily for 10-14 days (n=1257) | patients undergoing elective total hip replacement | double blind Parallel groups Sample size: 1252/1257 Primary endpoint: DVT, PE , all cause death FU duration: 30-42 days | | RECORD 3, 2008 | rivaroxaban 10 mg once daily for 10- 14 days (n=1254) vs. enoxaparin 40 mg subcutaneous once daily for 10-14 days (n=1277) | patients undergoing total knee arthroplasty | double blind Parallel groups Sample size: 1254/1277 Primary endpoint: DVT, PE all cause mortality FU duration: 13-17 days | | RECORD 4, 2009 | rivaroxaban 10mg once daily for 10 to 14 days (n=1584) vs. enoxaparin 30 mg twice daily by subcutaneous injection for 10-14 days (n=1564) | patients who had undergone total-knee-replacement surgery | double blind Parallel groups Sample size: 1584/1564 Primary endpoint: total VTE events FU duration: 40 days |
|
| venous thrombosis | versus No demonstrated result for efficacy rivaroxaban inferior to dalteparin in terms of all bleeding in SELECT D, 2018 (patients with cancer patients) | 2 trials | meta-analysis | | | Trial | control | p<0.05 | harm | NS |
|---|
| SELECT D, 2018 | rivaroxaban vs dalteparin | recurrent VTE 0.43 [0.19; 0.98] | all bleeding 3.76 [1.63; 8.68] | Major hemorrhage 1.83 [0.68; 4.94] | | EINSTEIN (subgroup), 2014 | rivaroxaban vs enoxaparin | recurrent
venous thromboembolism or major bleeding 0.54 [0.33; 0.89] Major hemorrhage 0.42 [0.18; 0.98] | | All-cause mortality 0.93 [0.64; 1.35] all bleeding 0.80 [0.54; 1.19] recurrent VTE 0.67 [0.35; 1.29] |
| Trial | Treatments | Patients | Method |
|---|
| SELECT D, 2018 | rivaroxaban (15 mg twice daily for 3 weeks, then 20 mg once daily for a total of 6 months) (n=203) vs. dalteparin (200 IU/kg daily during month 1, then 150 IU/kg daily for months 2-6) (n=203) | patients with active cancer who had symptomatic pulmonary embolism (PE), incidental PE, or symptomatic lowerextremity proximal deep vein thrombosis (DVT) | open-design Sample size: 203/203 Primary endpoint: FU duration: pilot trial | | EINSTEIN (subgroup), 2014 | rivaroxaban (15 mg twice daily for 21 days, followed by 20 mg once daily (n=354) vs. (enoxaparin1·0 mg/kg twice daily and warfarin or acenocoumarol; international normalised ratio 2·0–3·0 (n=301) | subgroup analysis of patients with active cancer (either at baseline or diagnosed during the study) who were enrolled in the EINSTEIN-DVT and EINSTEIN-PE trials | Sample size: 354/301 Primary endpoint: FU duration: sub group analysis |
|
| venous thrombosis | versus discontinuation No demonstrated result for efficacy rivaroxaban inferior to discontinuation in terms of major or clinically
relevant nonmajor bleeding in EINSTEIN-extension, 2009 | 1 trial | meta-analysis | | | Trial | control | p<0.05 | harm | NS |
|---|
| EINSTEIN-extension, 2009 | rivaroxaban vs discontinuation | recurrent DVT only 0.16 [0.06; 0.41] non fatal PE 0.15 [0.03; 0.67] recurrent VTE 0.19 [0.09; 0.40] | major or clinically
relevant nonmajor bleeding 5.07 [2.28; 11.31] | death 0.49 [0.04; 5.43] All deaths 0.49 [0.04; 5.43] Major bleeding ∞ [NaN; ∞] fatal PE 0.00 [0.00; NaN] Death related to venous thromboembolism 0.99 [0.06; 15.74] |
| Trial | Treatments | Patients | Method |
|---|
| EINSTEIN-extension, 2009 | rivaroxaban 20 mg once-daily for an additional 6 or 12 months (n=602) vs. placebo (n=595) | patients who had completed six to 12 months of anticoagulant treatment for an acute episode of VTE | double blind Parallel groups Sample size: 602/595 Primary endpoint: symptomatic recurrent VTE FU duration: |
|
| venous thrombosis | versus heparin/VKA No demonstrated result for efficacy | 3 trials | meta-analysis | | | Trial | control | p<0.05 | harm | NS |
|---|
| Einstein-DVT Dose-Ranging Study, 2008 | rivaroxaban (without LMWH) vs LMWH/VKA | | | | | Einstein-DVT Evaluation, 2010 | rivaroxaban (without LMWH) vs LMWH/VKA | recurrent DVT only 0.50 [0.26; 0.94] | | All deaths 0.77 [0.51; 1.17] Major bleeding 0.70 [0.35; 1.38] non fatal PE 1.10 [0.59; 2.08] fatal PE ∞ [NaN; ∞] Symptomatic nonfatal pulmonary embolism 1.10 [0.59; 2.08] recurrent VTE during treatment 0.70 [0.46; 1.07] Death related to venous thromboembolism 0.66 [0.19; 2.35] recurrent VTE 0.70 [0.46; 1.07] | | Einstein-PE Evaluation, 2012 | rivaroxaban (without LMWH) vs LMWH/VKA | | | |
| Trial | Treatments | Patients | Method |
|---|
| Einstein-DVT Dose-Ranging Study, 2008 | rivaroxaban 20, 30, or 40 mg once daily (n=-9) vs. low-molecular-weight heparin followed by vitamin K antagonists (n=-9) | patients with deep vein thrombosis | open Sample size: -9/-9 Primary endpoint: FU duration: | | Einstein-DVT Evaluation, 2010 | rivaroxaban 15 mg twice daily for 3 weeks, then 20 mg daily (n=1731) vs. enoxaparin 1 mg/kg twice daily >=5 days, then warfarin with target INR between 2-3 (n=1718) treatment duration (3, 6, or 12 months) decided by physicians. treatment duration of 6 months in 63%, 3 mo in 12% and 12 mo in 25% | Patients with Confirmed Acute Symptomatic Deep-Vein Thrombosis without Pulmonary Embolism | open (assessor-blind) Parallel groups Sample size: 1731/1718 Primary endpoint: Symptomatic recurrent VTE FU duration: | | Einstein-PE Evaluation, 2012 | rivaroxaban (15 mg twice daily for 3 weeks, followed by 20 mg once daily) for 3, 6, or 12 months (n=2419) vs. standard therapy with enoxaparin followed by an adjusted-dose vitamin
K antagonist (n=2413) | patients
who had acute symptomatic pulmonary embolism with or without deep-vein thrombosis | open Parallel groups Sample size: 2419/2413 Primary endpoint: symptomatic recurrent venous thromboembolism FU duration: 9.8 months |
|
