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Drug Monograph

Xarelto (Rivaroxaban)

rivaroxaban
Direct Factor Xa Inhibitor (DOAC) · Oral · 10 FDA-Approved Indications
Pharmacokinetic Profile
Half-Life
5–9 h (young adults); 11–13 h (elderly)
Metabolism
CYP3A4/5 (~18%) and CYP2J2 (~14%); substrate of P-gp and BCRP
Bioavailability
2.5/10 mg: 80–100% (food-independent); 20 mg: 66% fasted; AUC +39% with food
Tmax
2–4 hours after dose
Elimination
~36% renal as unchanged drug; ~7% faecal as unchanged drug; remainder as inactive metabolites
Clinical Information
Drug Class
Direct oral anticoagulant (factor Xa inhibitor)
Available Doses
2.5, 10, 15, 20 mg tablets; 1 mg/mL oral suspension
Reversal Agent
Andexanet alfa (Andexxa) approved for life-threatening bleeding
Renal Adjustment
Indication-specific; avoid if CrCl <15 mL/min for most uses
Hepatic Adjustment
Avoid in Child-Pugh B/C or any hepatic disease with coagulopathy
Pregnancy
Use with caution; risk of obstetric haemorrhage; crosses placenta
Lactation
Detected in human milk; weigh risks/benefits
Schedule / Legal Status
Rx only; not scheduled
Black Box Warning
Yes — (1) thrombotic events on premature discontinuation; (2) spinal/epidural haematoma
Generic Available
Yes for 2.5 mg only (FDA approved March 2025); 10/15/20 mg generics not yet approved at time of writing
Rx

Indications

Rivaroxaban is the most broadly indicated direct oral anticoagulant in the United States, with ten distinct FDA-approved uses spanning stroke prevention in atrial fibrillation, treatment and secondary prevention of venous thromboembolism, post-orthopaedic and medical-patient prophylaxis, secondary prevention in chronic atherosclerotic disease, and paediatric VTE and post-Fontan thromboprophylaxis. The dosing varies substantially across indications, and the FDA prescribing information explicitly cautions against off-label use in prosthetic heart valves and triple-positive antiphospholipid syndrome.

IndicationApproved PopulationTherapy TypeStatus
Stroke and systemic embolism prevention in nonvalvular atrial fibrillation (NVAF)Adults with NVAFMonotherapyFDA Approved
Treatment of deep vein thrombosis (DVT)Adults with acute DVTMonotherapy (no parenteral lead-in required)FDA Approved
Treatment of pulmonary embolism (PE)Adults with acute PE (haemodynamically stable)Monotherapy (no parenteral lead-in required)FDA Approved
Reduction in risk of recurrence of DVT and/or PEAdults at continued risk after ≥6 months of standard anticoagulationExtended secondary preventionFDA Approved
Prophylaxis of DVT after hip or knee replacement surgeryAdult orthopaedic surgery patientsPostoperative prophylaxisFDA Approved
Prophylaxis of VTE in acutely ill medical patientsHospitalised medical patients with restricted mobility, not at high bleeding riskIn-hospital and post-discharge prophylaxis (31–39 days)FDA Approved
Reduction of risk of major CV events in coronary artery disease (CAD)Adults with chronic CADCombination with low-dose aspirin (vascular dose 2.5 mg BID)FDA Approved
Reduction of risk of major thrombotic vascular events in PAD, including post-LERAdults with PAD, including patients post-lower extremity revascularisationCombination with low-dose aspirin (vascular dose 2.5 mg BID)FDA Approved
Treatment and reduction of recurrence of VTE in paediatric patientsBirth to <18 years; after ≥5 days of parenteral anticoagulationWeight-based oral suspension or tabletsFDA Approved
Thromboprophylaxis after Fontan procedurePaediatric patients ≥2 years with congenital heart disease post-FontanWeight-based oral suspension or tabletsFDA Approved
Cancer-associated thrombosis (CAT) treatmentAdults with active malignancy and acute VTEMonotherapy (no specific FDA CAT indication; CHEST and ASH guidelines endorse selected patients)Off-label
Cerebral or splanchnic vein thrombosisAdults with confirmed thrombosis at unusual sitesMonotherapy (off-label; growing observational data)Off-label

The pivotal evidence supporting these indications spans more than ten randomised trials. ROCKET-AF (Patel 2011) established non-inferiority to dose-adjusted warfarin for stroke prevention in 14,264 NVAF patients; EINSTEIN-DVT and EINSTEIN-PE (2010, 2012) established single-drug oral therapy for acute VTE without parenteral lead-in; EINSTEIN-CHOICE (Weitz 2017) supported the 10 mg extended-prevention dose; the RECORD program (1–3) established 10 mg once daily for orthopaedic prophylaxis; MAGELLAN (Cohen 2013) supported extended prophylaxis in acutely ill medical patients (with caveats around bleeding-risk subgroups now excluded from labelling); and COMPASS (Eikelboom 2017) and VOYAGER PAD (Bonaca 2020) established the vascular dose of 2.5 mg BID with aspirin for chronic CAD and PAD respectively.

Where rivaroxaban is NOT recommended (FDA PI)

Mechanical heart valves and TAVR: the GALILEO trial showed higher rates of death and bleeding with rivaroxaban after transcatheter aortic valve replacement; rivaroxaban is not recommended in patients with prosthetic heart valves.

Triple-positive antiphospholipid syndrome: direct-acting oral anticoagulants (DOACs), including rivaroxaban, are associated with increased recurrent thrombotic events compared with vitamin K antagonists in this population.

Haemodynamically unstable PE or patients requiring thrombolysis or pulmonary embolectomy: not recommended as initial therapy in place of unfractionated heparin.

Acutely ill medical patients at high bleeding risk: excluded from MAGELLAN labelling (history of bronchiectasis or pulmonary cavitation, active cancer with in-hospital treatment, dual antiplatelet therapy, recent gastroduodenal ulcer or recent bleeding).

Dose

Dosing

Rivaroxaban dosing varies by indication, renal function, and food-coadministration requirements. The 15 mg and 20 mg doses must be taken with food; the 2.5 mg and 10 mg doses can be taken with or without food. The FDA-approved labelling avoids use in CrCl <15 mL/min for VTE-related indications; for NVAF, 15 mg once daily is used in CrCl 15–50 mL/min.

IndicationLoading / InitiationMaintenance DoseDurationNotes
NVAF, CrCl >50 mL/minNone20 mg PO once dailyLong-termTake with the evening meal
Food increases AUC of 20 mg dose by ~39% and Cmax by ~76%
NVAF, CrCl 15–50 mL/minNone15 mg PO once dailyLong-termTake with the evening meal
For ESRD on dialysis, 15 mg daily expected to give similar exposure to ROCKET-AF (clinical outcomes not established)
Treatment of acute DVT or PE, CrCl ≥15 mL/minNone — oral monotherapy15 mg PO BID for 21 days20 mg PO once dailyTypically ≥3–6 monthsTake all doses with food
Avoid in CrCl <15 mL/min
Reduction of recurrent DVT/PE riskAfter ≥6 months of standard anticoagulation10 mg PO once dailyContinued indefinitely while risk persistsWith or without food; avoid in CrCl <15 mL/min
EINSTEIN-CHOICE: 10 mg dose preferred over 20 mg for extended prevention (lower bleeding)
Hip replacement prophylaxis, CrCl ≥15 mL/min6–10 h after surgery, once haemostasis established10 mg PO once daily35 daysWith or without food
Knee replacement prophylaxis, CrCl ≥15 mL/min6–10 h after surgery, once haemostasis established10 mg PO once daily12 daysWith or without food
VTE prophylaxis in acutely ill medical patientsNone10 mg PO once daily31–39 days total (in-hospital plus post-discharge)Exclude high-bleeding-risk subgroups (see Indications callout)
Chronic CAD or PAD — vascular doseNone2.5 mg PO BID + ASA 75–100 mg dailyLong-term while net benefit favourableWith or without food
No CrCl-based dose adjustment for CAD/PAD; limited data in CrCl 15–30 mL/min
Post-LER for symptomatic PADInitiate after haemostasis established post-procedure2.5 mg PO BID + ASA 75–100 mg dailyLong-term per VOYAGER PADWith or without food
Paediatric VTE (birth to <18 yr)After ≥5 days of parenteral anticoagulationWeight-based; see PI Table 2 (oral suspension 1 mg/mL or tablet)≥3 months (1 month minimum if <2 yr with catheter-related VTE)Take all doses with feeding/food
Avoid in eGFR <50 mL/min/1.73 m² or hepatic impairment
Paediatric Fontan thromboprophylaxis (≥2 yr)NoneWeight-based; see PI Table 3Long-termCan be taken with or without food

Special populations

PopulationAdjustmentRationale
CrCl <15 mL/min (non-dialysis)Avoid use for VTE-related and orthopaedic indicationsNo clinical data; rivaroxaban exposure increased; bleeding risk likely higher
End-stage renal disease on haemodialysis (NVAF only)15 mg once daily is expected to give exposure similar to ROCKET-AFPK modelling only; clinical efficacy and safety in dialysis patients not established
Moderate hepatic impairment (Child-Pugh B)Avoid useRivaroxaban exposure and bleeding risk increased; safety not established
Severe hepatic impairment (Child-Pugh C) or hepatic disease with coagulopathyAvoid useNo clinical data; coagulopathy already present
Geriatric (≥65 years)No specific adjustment beyond renal dosingHalf-life prolonged to 11–13 h vs 5–9 h in younger adults; bleeding rates higher in absolute terms
Body weight extremesNo formal dose adjustmentLimited efficacy and bleeding data at body weight >120 kg or BMI >40 kg/m²; ISTH 2021 guidance describes DOAC use as acceptable in obesity for some indications but with cautions
Pregnancy and lactationAvoid use unless benefit clearly outweighs riskCrosses placenta in animal studies; detected in human breast milk; LMWH preferred during pregnancy
Switching from warfarin to rivaroxabanStart when INR <3.0 (adults) or <2.5 (paediatric)Avoid periods of inadequate anticoagulation
Switching from rivaroxaban to warfarin (adults)Discontinue rivaroxaban and bridge with parenteral anticoagulant + warfarinINR is unreliable during rivaroxaban co-administration
Switching to/from non-warfarin anticoagulantsGive first dose of new agent at time of next scheduled rivaroxaban doseMaintains continuous anticoagulation given the rapid onset/offset of DOACs
Clinical pearls — dosing and administration

Food matters for 15 and 20 mg doses. Fasted bioavailability of the 20 mg dose is only ~66%; food increases AUC by ~39% and Cmax by ~76%. Counsel patients to take the dose with the largest meal of the day to minimise variability.

Discontinue at least 24 hours before invasive procedures with bleeding risk. Some bleeding-risk procedures may need a longer interval (48 h or more) particularly in CrCl 15–50 mL/min.

Premature discontinuation increases thrombotic events (boxed warning). If stopping for any reason other than bleeding or end of therapy, bridge with another anticoagulant.

Tablets can be crushed and mixed with applesauce or suspended in water for feeding-tube administration. The 15 and 20 mg crushed doses must be followed by enteral feeding to ensure absorption.

Avoid administration distal to the stomach (e.g. jejunostomy tubes) — absorption is significantly reduced.

Routine coagulation monitoring is not needed. Anti-factor Xa activity (rivaroxaban-calibrated) is the most useful test if quantification is needed in bleeding, urgent surgery, or suspected non-adherence.

PK

Pharmacology

Mechanism of Action

Rivaroxaban is a selective, reversible, direct inhibitor of activated factor X (factor Xa). It binds free factor Xa as well as factor Xa within the prothrombinase complex without requiring antithrombin as a cofactor — a key difference from heparins and fondaparinux. By blocking factor Xa, rivaroxaban inhibits thrombin generation and downstream fibrin formation, producing a predictable, dose-dependent anticoagulant effect. It has no direct effect on platelet aggregation, but indirectly reduces thrombin-mediated platelet activation. Onset is rapid: peak plasma concentrations occur within 2–4 hours and peak anti-factor Xa activity tracks closely with plasma drug levels. The PT, INR, and aPTT are dose-dependently prolonged but are not reliable for therapeutic monitoring.

ADME profile

ParameterValueClinical Implication
Absorption2.5/10 mg: 80–100% bioavailable, food-independent. 20 mg: 66% fasted; with food AUC increases by ~39% and Cmax by ~76%; Tmax 2–4 h15 and 20 mg tablets must be taken with food; absorption decreases markedly if drug is released distal to stomach
Distribution~92–95% bound to plasma protein (mainly albumin); steady-state Vd ~50 LNot effectively dialysable due to high protein binding; modest tissue distribution
MetabolismHepatic CYP3A4/5 (~18%) and CYP2J2 (~14%); plus ~14% via CYP-independent hydrolysis of amide bonds. Substrate of P-gp and BCRP transportersCombined P-gp + strong CYP3A inhibitors (ketoconazole, ritonavir) raise exposure significantly — avoid use; combined inducers (rifampin, carbamazepine) reduce exposure — avoid use
EliminationTerminal t½ 5–9 h in young adults, 11–13 h in elderly. ~36% excreted unchanged in urine (via glomerular filtration plus active tubular secretion); ~7% unchanged in faeces; remainder as inactive metabolitesRenal impairment increases exposure ~44–64%; significant dose adjustments required for VTE indications; use caution in elderly
Why the vascular dose is unique

The 2.5 mg twice-daily “vascular dose” tested in COMPASS and VOYAGER PAD is roughly one-quarter of the standard NVAF dose. At this exposure, rivaroxaban achieves partial factor Xa inhibition that — combined with low-dose aspirin — produces additive antithrombotic benefit on the arterial side without the bleeding penalty of full-dose anticoagulation. COMPASS reported a 24% relative reduction in CV death/MI/stroke (4.1% vs 5.4% with aspirin alone) at the cost of a hazard ratio of 1.8 for modified ISTH major bleeding (1.6%/yr vs 0.9%/yr). The 2.5 mg dose is not effective for stroke prevention in AF or for VTE treatment.

SE

Side Effects

Bleeding is by far the most common adverse reaction across all rivaroxaban indications and is the most frequent cause of treatment discontinuation. Frequencies vary substantially by trial and clinical setting; rates below are drawn from the FDA prescribing information and the original pivotal trials. The principal non-haemorrhagic adverse reactions are mild (back pain, dizziness, pruritus, abdominal pain, fatigue) and generally do not require discontinuation.

≥10% Very Common
Adverse EffectIncidenceClinical Note
Any bleeding (EINSTEIN DVT/PE pooled)28.3% vs 28.0% enoxaparin/VKAIncludes nuisance bleeding (epistaxis, gum bleeding, easy bruising)
Any bleeding (EINSTEIN-CHOICE 10 mg)13.4% vs 12.2% aspirinReflects long-term low-intensity exposure
Menorrhagia (paediatric ≥12 yr who reached menarche, EINSTEIN Junior)27% vs 10% comparatorCounsel adolescent female patients; tranexamic acid or hormonal options may help
Cough (paediatric Fontan, UNIVERSE)15.6% vs 8.8% aspirinGenerally mild; assess for other causes if persistent
Vomiting (paediatric VTE, EINSTEIN Junior)10.6% vs 8.0% comparatorRe-administer dose if vomiting occurs within 30 min
Gastroenteritis (paediatric Fontan)12.5% vs 2.9% aspirinCombined viral and non-viral; generally self-limiting
1–10% Common
Adverse EffectIncidenceClinical Note
Clinically relevant non-major bleeding (EINSTEIN DVT/PE)8.6% vs 8.7%Most common cause of dose interruption in VTE treatment
Any bleeding (RECORD 1-3 hip/knee)5.8% vs 5.6% enoxaparinMost occur in the first postoperative week
NVAF major bleeding (ROCKET-AF)3.6%/yr vs 3.5%/yr warfarinNumerically similar to warfarin overall but with different anatomical pattern
Pediatric “trivial bleeding” (EINSTEIN Junior)34.3% vs 27.2% comparatorIncludes minor mucocutaneous bleeding not requiring intervention
CRNM bleeding (MAGELLAN)2.9% vs 1.1% enoxaparin/placeboHigher with rivaroxaban in extended prophylaxis setting
Wound secretion (RECORD post-orthopaedic)2.8% vs 2.0% enoxaparinSurgical site oozing or discharge; usually self-limiting
Back pain (EINSTEIN DVT)2.9% vs 1.8% enoxaparin/VKAInvestigate to rule out retroperitoneal bleed if severe
Abdominal pain (EINSTEIN DVT)2.7% vs 1.5%Consider GI bleeding work-up if persistent
Pruritus (EINSTEIN PE; RECORD)2.2% vs 1.1%; 2.1% vs 1.8%Usually mild; rule out drug rash if persistent
Dizziness (EINSTEIN DVT)2.2% vs 1.3%Consider orthostatic vitals; rule out occult bleeding
GI bleeding (ROCKET-AF NVAF)2.0%/yr vs 1.2%/yr warfarinHigher than warfarin; PPI may be considered in high-risk patients
Major CV-disease bleeding (COMPASS, modified ISTH)1.6%/yr vs 0.9%/yr placebo (HR 1.8)Vascular dose plus aspirin vs aspirin alone
TIMI major bleeding (VOYAGER PAD)1.9% vs 1.4% placebo (HR 1.4)Principally GI bleeding
Major bleeding (EINSTEIN DVT/PE pooled)1.0% vs 1.7% enoxaparin/VKALower than VKA in acute VTE treatment
Pain in extremity, muscle spasm, syncope (RECORD)1.7%, 1.2%, 1.2%Higher than enoxaparin in postoperative orthopaedic setting
Serious Regardless of frequency
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Major bleeding (any indication)0.3% (post-op) to 3.6%/yr (NVAF)Throughout therapyHold rivaroxaban; assess severity; consider andexanet alfa or 4F-PCC if life-threatening
Intracranial haemorrhage0.5%/yr (ROCKET-AF) — lower than warfarin (HR 0.67)Any timePermanent discontinuation; emergency neuroimaging; reverse with andexanet alfa; neurosurgery consult
Fatal bleeding (NVAF)0.2%/yr vs 0.5%/yr warfarin (ROCKET-AF; HR 0.50)Any timeResuscitation; reversal; root-cause review
Spinal or epidural haematoma (boxed warning)Rare; risk increases with neuraxial proceduresHours to days after neuraxial interventionEmergency MRI; urgent surgical decompression; can result in permanent paralysis
GI bleeding0.7%/yr (CAD/PAD) to 2.0%/yr (NVAF)Any timeHold drug; endoscopy; treat source; consider PPI prophylaxis on resumption
Anticoagulant-related nephropathy (postmarketing)Rare; underrecognisedDays to weeks; often subacuteHold drug; investigate haematuria and rising creatinine; nephrology referral if persists
Hepatotoxicity (postmarketing: hepatitis, cholestasis, jaundice)Rare; idiosyncraticDays to months after initiationDiscontinue; check LFTs and bilirubin; switch to non-DOAC if confirmed
Anaphylaxis / angioedema (postmarketing)Very rareMinutes to hoursPermanent discontinuation; epinephrine and supportive care; switch to apixaban or VKA
Stevens-Johnson syndrome / DRESS (postmarketing)Very rareDays to weeksPermanent discontinuation; dermatology referral; admit if severe
Eosinophilic pneumonia (postmarketing)Very rareDays to weeksDiscontinue; pulmonology consult; corticosteroids may be required
Agranulocytosis, thrombocytopenia (postmarketing)RareVariableDiscontinue; haematology referral; supportive care
Recurrent thrombosis after premature discontinuation (boxed warning)Increased rate observed during transitionsHours to weeks after stoppingBridge with parenteral or oral anticoagulant if discontinuation is for non-bleeding reason
Discontinuation Withdrawal rates by trial
ROCKET-AF (NVAF) — bleeding-related
4.3% vs 3.1% warfarin
Bleeding was the most frequent cause of permanent discontinuation; non-bleeding AE rates similar between arms.
COMPASS (CAD/PAD vascular dose) — bleeding-related
2.7% vs 1.2% placebo (both on ASA)
More than double the discontinuation rate vs aspirin alone — weigh ischaemic benefit against bleeding burden.
VOYAGER PAD — bleeding-related
4.1% vs 1.6% placebo (both on ASA)
Highest discontinuation rate among adult indications; reflects post-revascularisation bleeding risk plus aspirin.
EINSTEIN DVT/PE — bleeding-related
1.7% vs 1.5% enoxaparin/VKA
Comparable to standard-of-care; long-term acute VTE treatment safety profile.
The ROCKET-AF bleeding pattern

In NVAF, rivaroxaban does not produce more major bleeding overall than well-controlled warfarin (3.6% vs 3.5% per year), but the anatomical pattern is different: fewer intracranial bleeds (HR 0.67) and fewer fatal bleeds (HR 0.50) but more GI bleeds (HR 1.61). This trade-off — less catastrophic but more nuisance bleeding — is a recurring DOAC theme and should shape patient selection. In patients with a history of GI bleeding, apixaban may be a reasonable alternative; in patients with ICH risk factors, rivaroxaban or another DOAC is generally preferred over warfarin.

Int

Drug Interactions

Rivaroxaban is a substrate of both CYP3A4/5 and the P-glycoprotein efflux transporter. Drugs that simultaneously inhibit both pathways significantly increase exposure and bleeding risk; combined inducers reduce exposure and increase thrombotic risk. Coadministration with other antithrombotics (anticoagulants, antiplatelets, NSAIDs, fibrinolytics) is the dominant pharmacodynamic concern. Unlike warfarin, rivaroxaban has no clinically significant interactions with vitamin K–rich foods, gastric pH modulators (PPIs, H2 blockers, antacids), or atorvastatin.

Major Combined P-gp + strong CYP3A inhibitors (ketoconazole, itraconazole, ritonavir, indinavir, conivaptan, cobicistat)
MechanismDual inhibition increases rivaroxaban absorption and decreases clearance
EffectKetoconazole 400 mg/day increased rivaroxaban AUC by 158% (95% CI 136–182%) and Cmax by 72%; ritonavir increased AUC by 153%
ManagementAvoid coadministration. Use alternative anticoagulant or alternative antifungal/antiretroviral
FDA PI · Mueck 2013
Major Combined P-gp + strong CYP3A inducers (rifampin, carbamazepine, phenytoin, phenobarbital, St. John’s wort)
MechanismDual induction accelerates rivaroxaban metabolism and efflux
EffectRifampicin reduced rivaroxaban AUC by ~50%; loss of anticoagulant effect with increased thrombotic risk
ManagementAvoid coadministration. Use VKA or alternative anticoagulant; avoid St. John’s wort
FDA PI
Major Other anticoagulants (warfarin, heparin, LMWH, apixaban, dabigatran, edoxaban, fondaparinux)
MechanismAdditive anticoagulation through different targets
EffectSharply increased bleeding risk; clinically significant especially during transitions
ManagementAvoid concurrent use except during planned transition (see Dosing)
FDA PI
Major Fibrinolytic therapy (alteplase, tenecteplase, reteplase, streptokinase)
MechanismProfound additive bleeding risk in the acute lytic window
EffectSubstantially increased major and intracranial haemorrhage
ManagementAvoid concurrent administration; rivaroxaban not recommended in haemodynamically unstable PE requiring thrombolysis
FDA PI
Moderate Aspirin and dual antiplatelet therapy (clopidogrel, prasugrel, ticagrelor)
MechanismAdditive bleeding through complementary pathways
Effect2.5 mg BID + ASA 75–100 mg is the labelled vascular regimen; triple therapy substantially raises bleeding
ManagementUse 2.5 mg BID + ASA only when indicated (CAD/PAD); minimise duration of triple therapy in AF + PCI scenarios
FDA PI · 2023 ESC ACS
Moderate Chronic NSAIDs (ibuprofen, naproxen, COX-2 inhibitors)
MechanismNSAID gastric mucosal injury plus mild antiplatelet effect
EffectIncreased GI bleeding risk; particularly relevant given baseline GI bleeding signal with rivaroxaban
ManagementAvoid chronic NSAIDs. If unavoidable, add PPI; favour paracetamol/topical alternatives
FDA PI
Moderate Combined P-gp + moderate CYP3A inhibitors (erythromycin, diltiazem, verapamil, dronedarone, fluconazole)
MechanismModerate increases in rivaroxaban exposure
EffectErythromycin 500 mg QID raised AUC by 34% (95% CI 23–46%); fluconazole raised AUC by 42%; effects amplified in renal impairment
ManagementAvoid in patients with CrCl 15–80 mL/min unless benefit clearly outweighs risk; preserved renal function generally tolerable
FDA PI · Mueck 2013
Moderate SSRIs and SNRIs (sertraline, citalopram, venlafaxine, duloxetine)
MechanismSSRI-induced platelet serotonin depletion adds to anticoagulation
EffectModest increase in upper GI bleeding (class effect with anticoagulants)
ManagementAdd PPI in patients with GI bleeding risk factors
Lexicomp
Minor Clarithromycin
MechanismCombined P-gp and strong CYP3A inhibitor
EffectRaised AUC by 54% and Cmax by 40%; FDA PI states no precautions are necessary as the change is unlikely to affect bleeding risk
ManagementNo precautions required per FDA PI; use clinical judgement in renal impairment
FDA PI · Mueck 2013
Minor Gastric acid suppression (PPIs, H2 blockers, antacids)
MechanismNo effect on rivaroxaban PK
EffectCoadministration with omeprazole, ranitidine, or aluminium/magnesium hydroxide did not alter exposure
ManagementNo interaction; PPIs may even be helpful for GI bleed prophylaxis
FDA PI
The two-pathway rule

Rivaroxaban requires both CYP3A4 and P-gp for elimination. A drug that inhibits or induces just one pathway typically produces only a modest pharmacokinetic effect. The clinically dangerous interactions are with agents that affect both simultaneously — the “azoles, ritonavir, rifampin, carbamazepine, phenytoin, St. John’s wort” list. This pattern is the same for apixaban; for dabigatran (P-gp only), the risk profile differs.

Mon

Monitoring

Routine therapeutic drug monitoring is not required and is not recommended by the FDA prescribing information. Standard coagulation tests (PT, INR, aPTT) are influenced by rivaroxaban but are unreliable for dose titration. The principal monitoring tasks are renal function, bleeding surveillance, and adherence assessment.

  • Bleeding signs & symptoms Every visit; daily during inpatient
    Routine     Ask about bruising, epistaxis, gum bleeding, melena, haematuria, menorrhagia. Inspect mucous membranes. Suspect occult bleeding in any post-procedure or anticoagulated patient who becomes hypotensive or develops unexplained anaemia.
  • Renal function (eGFR or CrCl) Baseline; every 6–12 months; sooner if ≥75 years, frail, or unstable
    Routine     Use Cockcroft-Gault with actual body weight (not eGFR by MDRD or CKD-EPI) for FDA-aligned dose decisions in adults. Cross-check at any acute illness or contrast-imaging event — AKI is a common reason for inadvertent rivaroxaban over-exposure.
  • Haemoglobin / haematocrit Baseline; periodically; with new symptoms
    Trigger-based     Investigate unexplained anaemia (occult GI loss is the commonest cause). Consider faecal immunochemical testing or endoscopy in patients with progressive iron-deficiency anaemia.
  • Liver function (AST, ALT, bilirubin) Baseline; with new symptoms or jaundice
    Trigger-based     Postmarketing reports of hepatitis, cholestasis, and jaundice. Avoid initiation in Child-Pugh B or C. Discontinue and switch agents if hepatocellular injury appears drug-related.
  • Adherence assessment Every visit
    Routine     DOAC adherence is consistently lower than warfarin in real-world data. Use refill records, pill counts, or single-time anti-Xa levels in suspected non-adherence. Once-daily dosing aids compliance for NVAF and extended VTE prevention.
  • Bleeding-risk reassessment (HAS-BLED, ORBIT, ATRIA) Annually; with new comorbidity or medication
    Routine     Identify modifiable factors (uncontrolled BP, concomitant antiplatelets, alcohol, NSAIDs). Useful for shared decision-making rather than for stopping anticoagulation.
  • Anti-factor Xa activity (rivaroxaban-calibrated) Selected scenarios only
    Trigger-based     Use cases: active major bleeding, urgent surgery, suspected non-adherence, extreme body weight, dialysis, or breakthrough thrombosis. Not for routine dose adjustment. Plain anti-Xa (heparin-calibrated) underestimates rivaroxaban activity.
  • Pregnancy testing Baseline in females of reproductive potential; with menstrual changes
    Routine     Discuss contraception and pregnancy planning. Switch to LMWH if pregnancy occurs or is planned. Counsel about menorrhagia risk on rivaroxaban.
  • Periodic indication review At least annually
    Routine     Confirm ongoing indication, balance benefit/bleeding-risk, and reassess against alternative DOACs (apixaban often preferred in high GI bleeding risk; LMWH preferred in active malignancy with luminal GI tumour).
Perioperative management

Discontinue rivaroxaban at least 24 hours before procedures with low-to-moderate bleeding risk. For high bleeding-risk surgery, hold for 48 hours (CrCl ≥30 mL/min) or 72 hours (CrCl <30). For neuraxial procedures, an indwelling epidural catheter should not be removed until at least 2 elimination half-lives have elapsed (~18 h young adults, ~26 h elderly), and the next rivaroxaban dose should not be given until at least 6 hours after catheter removal. Resume rivaroxaban 24 hours postoperatively if haemostasis is established — sooner exposes the patient to surgical-site bleeding, later exposes them to thrombosis.

Reversal of anticoagulant effect

For life-threatening bleeding, andexanet alfa (Andexxa) is the FDA-approved reversal agent. It is a recombinant modified factor Xa decoy protein that binds rivaroxaban and other factor Xa inhibitors with high affinity, restoring endogenous factor Xa activity. If andexanet alfa is unavailable, 4-factor prothrombin complex concentrate (4F-PCC, e.g. Kcentra) at 25–50 IU/kg has been used off-label. Activated charcoal can be considered within 2 hours of ingestion. Rivaroxaban is highly protein-bound (~92–95%) and is not effectively dialysable. Vitamin K and protamine sulfate are ineffective.

CI

Contraindications & Cautions

FDA Boxed Warning A Premature discontinuation increases the risk of thrombotic events

Premature discontinuation of any oral anticoagulant, including XARELTO, in the absence of adequate alternative anticoagulation increases the risk of thrombotic events. An increased rate of stroke was observed during the transition from XARELTO to warfarin in clinical trials in atrial fibrillation patients. If XARELTO is discontinued for a reason other than pathological bleeding or completion of a course of therapy, consider coverage with another anticoagulant.

FDA Boxed Warning B Spinal/epidural haematoma

Epidural or spinal haematomas have occurred in patients treated with XARELTO who are receiving neuraxial anaesthesia or undergoing spinal puncture. These haematomas may result in long-term or permanent paralysis. Risk factors include indwelling epidural catheters, concomitant use of drugs that affect haemostasis (NSAIDs, platelet inhibitors, other anticoagulants), traumatic or repeated epidural or spinal punctures, and a history of spinal deformity or surgery. Monitor for neurological impairment and treat urgently if observed.

Absolute contraindications (FDA prescribing information, Section 4)

  • Active pathological bleeding (e.g., active peptic ulcer haemorrhage, active intracranial haemorrhage, retinal bleeding)
  • Severe hypersensitivity reaction to rivaroxaban (e.g., anaphylactic reactions)

Use NOT recommended (per FDA Warnings and Precautions)

  • Prosthetic heart valves — including post-TAVR: the GALILEO trial showed higher rates of death and bleeding with rivaroxaban after transcatheter aortic valve replacement. Safety and efficacy have not been studied in patients with other prosthetic heart valves or other valve procedures. Use a vitamin K antagonist for mechanical valves.
  • Triple-positive antiphospholipid syndrome (positive lupus anticoagulant, anticardiolipin, and anti-β2-glycoprotein I antibodies): higher rates of recurrent thrombotic events with DOACs vs warfarin. Use a vitamin K antagonist.
  • Haemodynamically unstable PE or PE patients who may receive thrombolysis or pulmonary embolectomy: not recommended as initial therapy in place of unfractionated heparin.
  • Acutely ill medical patients at high bleeding risk: bronchiectasis or pulmonary cavitation history, active cancer with in-hospital treatment, dual antiplatelet therapy, recent gastroduodenal ulcer or recent bleeding (excluded from the MAGELLAN labelled population).
  • CrCl <15 mL/min (other than NVAF in dialysis based on PK modelling) — avoid use in VTE-related and orthopaedic indications.
  • Moderate to severe hepatic impairment (Child-Pugh B or C) or any hepatic disease associated with coagulopathy.

Use with caution — specialist input recommended

  • Concomitant antiplatelet or NSAID therapy: assess net benefit; minimise duration of triple therapy in AF + PCI
  • Body weight >120 kg or BMI >40 kg/m²: limited PK data; ISTH 2021 guidance permits DOAC use for some indications in obesity but with cautions, particularly for treatment-dose VTE
  • Active malignancy with luminal GI tumours: some studies (e.g., SELECT-D) suggested higher GI bleeding with DOACs vs LMWH in this subgroup
  • Pregnancy: avoid; use LMWH instead
  • Lactation: rivaroxaban detected in human milk; weigh benefits against potential infant exposure
  • Older adults (≥75 years): bleeding rates are higher in absolute terms; assess fall risk and renal trajectory
  • Recent or planned spinal/epidural anaesthesia or lumbar puncture: see boxed warning B; carefully time around half-life
  • Frequent falls or significant cognitive impairment: bleeding risk may outweigh thrombotic benefit
  • Dual P-gp + moderate CYP3A inhibitors (erythromycin, dronedarone, fluconazole) in CrCl 15–80 mL/min: avoid unless clearly justified
Pt

Patient Counselling

Purpose of therapy

Explain that rivaroxaban is a blood-thinning medicine (an anticoagulant) that prevents the blood from forming dangerous clots. Depending on the indication, it is used to prevent strokes in atrial fibrillation, to treat or prevent blood clots in the legs (DVT) or lungs (PE), to prevent clots after major joint surgery, or — at a low dose — to reduce heart attacks, strokes, and limb events in long-standing artery disease. Stopping rivaroxaban without speaking to the prescriber can lead to a stroke or recurrent clot; this is among the most common preventable causes of treatment failure. Patients should never stop on their own.

How to take

The 15 mg and 20 mg tablets must be taken with food (ideally the largest meal of the day) at the same time each day. The 2.5 mg and 10 mg tablets can be taken with or without food. Tablets can be swallowed whole or, if needed, crushed and mixed with applesauce immediately before use. If a once-daily dose is missed, take it as soon as remembered the same day; do not double up. For twice-daily dosing (15 mg BID for acute VTE, or 2.5 mg BID for vascular disease), take a missed dose as soon as possible — for the 15 mg BID, it is acceptable to take both 15 mg tablets together to make up the daily dose, then resume the regular schedule the next day. Bring a current medication list to every appointment. Patients should carry an anticoagulation alert card or wear a medical bracelet.

Bleeding and bruising
Tell patient You will bruise more easily, bleed longer from cuts, and may have more frequent nosebleeds. Use a soft toothbrush and an electric razor where possible. Tell every doctor, dentist, surgeon, and pharmacist that you take a blood thinner.
Call prescriber Black or tarry stools, red or pink urine, vomiting blood or material that looks like coffee grounds, sudden severe headache, sudden weakness or speech change, vision changes, coughing up blood, bleeding that does not stop within 10–15 minutes, or any large unexplained bruise — seek emergency care immediately.
Never stop without checking first
Tell patient Stopping rivaroxaban suddenly raises the risk of a stroke or new clot. Even if you feel well, do not stop because you have run out, are on holiday, or have a minor side effect. Order refills at least one week before running out.
Call prescriber If you have missed several doses, before any planned surgery or dental work, before pregnancy, or if any new doctor wants you to stop the medicine.
Surgery, dental work, and procedures
Tell patient Most surgical and many dental procedures require holding rivaroxaban for at least 24 hours before, and longer for major surgery or if your kidney function is reduced. Carry a wallet card with the medicine name, dose, and your prescriber’s contact.
Call prescriber Before any planned surgery, dental work involving extraction or deep cleaning, colonoscopy, or epidural/spinal anaesthesia — ideally at least 1 week in advance. Never stop without confirming the plan.
Other medicines, supplements, and food
Tell patient Avoid ibuprofen, naproxen, and other anti-inflammatories for routine pain — use paracetamol/acetaminophen instead. Tell your pharmacist about every new prescription. Avoid St. John’s wort. Limit alcohol. Unlike warfarin, you do not need to follow a special diet for vitamin K.
Call prescriber Before starting any new prescription, particularly antibiotics (rifampin, clarithromycin), antifungals (ketoconazole, itraconazole, fluconazole), seizure medicines, HIV/HCV treatments, or other blood thinners.
Pregnancy, breastfeeding, and menstrual periods
Tell patient Rivaroxaban can cross the placenta and may not be safe in pregnancy — use reliable contraception. Some patients have heavier menstrual periods on rivaroxaban; this is common and usually manageable. Rivaroxaban is detected in breast milk; the decision to breastfeed should be made with your prescriber.
Call prescriber If you become pregnant or plan to. Heavy or prolonged menstrual bleeding causing tiredness, dizziness, or anaemia — treatment options exist.
Falls, head injury, and emergency situations
Tell patient Even minor head injuries or falls deserve evaluation while you are on a blood thinner. Tell emergency clinicians immediately that you take rivaroxaban, the dose, and the time of your last dose. A specific reversal medicine (andexanet alfa) is available for life-threatening bleeding.
Call prescriber After any fall (especially head injury), motor vehicle accident, or significant trauma. Bring your medication list to the emergency department.
Adherence and refills
Tell patient Take rivaroxaban at the same time each day. Use a pill organiser, alarm, or app reminder. Order refills at least 1 week before running out. The medicine works for less than a day — missing doses opens a window for clot formation.
Call prescriber If you have missed several days, are travelling and need an extra supply, or are having difficulty affording the medicine. Patient assistance and savings programs may be available.
Ref

Sources

Regulatory (PI / SmPC)
  1. U.S. Food and Drug Administration. XARELTO (rivaroxaban) tablets and oral suspension — Prescribing Information (revised 06/2025). accessdata.fda.gov/drugsatfda_docs/label/2025/022406s044,215859s005lbl.pdf Primary regulatory source for indications, dosing, boxed warnings, contraindications, adverse-reaction frequencies, and interaction studies.
  2. European Medicines Agency. Xarelto (rivaroxaban) Summary of Product Characteristics. ema.europa.eu/en/medicines/human/EPAR/xarelto European prescribing reference; useful for additional warnings and pharmacovigilance updates.
  3. FDA Roundup. First generic rivaroxaban (2.5 mg) approval. March 4, 2025. fda.gov/news-events/press-announcements/fda-roundup-march-4-2025 Documents first generic ANDA approvals (Lupin, Taro) for the 2.5 mg vascular dose only; higher doses still under patent at time of writing.
Key Clinical Trials
  1. Patel MR, Mahaffey KW, Garg J, et al. Rivaroxaban versus warfarin in nonvalvular atrial fibrillation (ROCKET AF). N Engl J Med. 2011;365(10):883-891. doi.org/10.1056/NEJMoa1009638 Pivotal trial for stroke prevention in NVAF; basis for the 20 mg / 15 mg dose by renal function.
  2. EINSTEIN Investigators, Bauersachs R, Berkowitz SD, et al. Oral rivaroxaban for symptomatic venous thromboembolism (EINSTEIN-DVT). N Engl J Med. 2010;363(26):2499-2510. doi.org/10.1056/NEJMoa1007903 Established single-drug oral therapy for acute DVT without parenteral lead-in.
  3. EINSTEIN-PE Investigators, Büller HR, et al. Oral rivaroxaban for the treatment of symptomatic pulmonary embolism. N Engl J Med. 2012;366(14):1287-1297. doi.org/10.1056/NEJMoa1113572 Sister trial to EINSTEIN-DVT covering symptomatic PE; same dosing schema.
  4. Weitz JI, Lensing AWA, Prins MH, et al. Rivaroxaban or aspirin for extended treatment of venous thromboembolism (EINSTEIN-CHOICE). N Engl J Med. 2017;376(13):1211-1222. doi.org/10.1056/NEJMoa1700518 Established the 10 mg once-daily dose for extended VTE prevention with similar bleeding to aspirin.
  5. Eikelboom JW, Connolly SJ, Bosch J, et al. Rivaroxaban with or without aspirin in stable cardiovascular disease (COMPASS). N Engl J Med. 2017;377(14):1319-1330. doi.org/10.1056/NEJMoa1709118 Established the 2.5 mg BID + ASA vascular dose for chronic CAD/PAD; 24% relative reduction in CV events (4.1% vs 5.4%) at the cost of more major bleeding (HR 1.8).
  6. Bonaca MP, Bauersachs RM, Anand SS, et al. Rivaroxaban in peripheral artery disease after revascularization (VOYAGER PAD). N Engl J Med. 2020;382(21):1994-2004. doi.org/10.1056/NEJMoa2000052 Established benefit of vascular dose plus aspirin after lower-extremity revascularisation for symptomatic PAD.
  7. Cohen AT, Spiro TE, Büller HR, et al. Rivaroxaban for thromboprophylaxis in acutely ill medical patients (MAGELLAN). N Engl J Med. 2013;368(6):513-523. doi.org/10.1056/NEJMoa1111096 Basis for extended VTE prophylaxis indication in medically ill patients (with high-bleeding-risk subgroups now excluded from labelling).
  8. Eriksson BI, Borris LC, Friedman RJ, et al. Rivaroxaban versus enoxaparin for thromboprophylaxis after hip arthroplasty (RECORD1). N Engl J Med. 2008;358(26):2765-2775. doi.org/10.1056/NEJMoa0800374 First of three RECORD trials supporting orthopaedic VTE prophylaxis at 10 mg daily.
  9. Male C, Lensing AWA, Palumbo JS, et al. Rivaroxaban compared with standard anticoagulants for the treatment of acute venous thromboembolism in children (EINSTEIN Junior). Lancet Haematol. 2020;7(1):e18-e27. doi.org/10.1016/S2352-3026(19)30219-4 Paediatric pivotal trial supporting weight-based dosing in children with acute VTE.
  10. McCrindle BW, Michelson AD, Van Bergen AH, et al. Thromboprophylaxis for children post-Fontan procedure (UNIVERSE). J Am Heart Assoc. 2021;10(22):e021765. doi.org/10.1161/JAHA.120.021765 Paediatric trial supporting rivaroxaban for thromboprophylaxis after Fontan surgery.
  11. Dangas GD, Tijssen JGP, Wohrle J, et al. A controlled trial of rivaroxaban after transcatheter aortic-valve replacement (GALILEO). N Engl J Med. 2020;382(2):120-129. doi.org/10.1056/NEJMoa1911425 Negative trial — basis for the recommendation against rivaroxaban after TAVR.
Guidelines
  1. Joglar JA, Chung MK, Armbruster AL, et al. 2023 ACC/AHA/ACCP/HRS Guideline for the Diagnosis and Management of Atrial Fibrillation. J Am Coll Cardiol. 2024;83(1):109-279. doi.org/10.1016/j.jacc.2023.08.017 Current US recommendations on stroke prevention in NVAF, including DOAC selection.
  2. Stevens SM, Woller SC, Kreuziger LB, et al. Antithrombotic Therapy for VTE Disease: Second Update of the CHEST Guideline and Expert Panel Report. Chest. 2021;160(6):e545-e608. doi.org/10.1016/j.chest.2021.07.055 CHEST guideline endorsing DOACs as first-line for most VTE; weight-based and renal considerations.
  3. Konstantinides SV, Meyer G, Becattini C, et al. 2019 ESC Guidelines for the diagnosis and management of acute pulmonary embolism. Eur Heart J. 2020;41(4):543-603. doi.org/10.1093/eurheartj/ehz405 European recommendations for acute and extended PE management with rivaroxaban and other DOACs.
  4. Lyman GH, Carrier M, Ay C, et al. American Society of Hematology 2021 guidelines for management of venous thromboembolism: prevention and treatment in patients with cancer. Blood Adv. 2021;5(4):927-974. doi.org/10.1182/bloodadvances.2020003442 ASH guidance on cancer-associated thrombosis — supports DOACs (including rivaroxaban) in selected cancer patients.
Pharmacokinetics / Special Populations
  1. Mueck W, Stampfuss J, Kubitza D, Becka M. Clinical pharmacokinetic and pharmacodynamic profile of rivaroxaban. Clin Pharmacokinet. 2014;53(1):1-16. doi.org/10.1007/s40262-013-0100-7 Comprehensive PK/PD review including renal-impairment data, food effect, and elderly pharmacokinetics; source for CYP3A4 18%, CYP2J2 14%, hydrolysis 14%.
  2. Mueck W, Kubitza D, Becka M. Co-administration of rivaroxaban with drugs that share its elimination pathways: pharmacokinetic effects in healthy subjects. Br J Clin Pharmacol. 2013;76(3):455-466. doi.org/10.1111/bcp.12075 Source for verified interaction magnitudes: ketoconazole AUC +158%, ritonavir +153%, clarithromycin +54%, erythromycin +34%.
  3. Connolly SJ, Crowther M, Eikelboom JW, et al. Full study report of andexanet alfa for bleeding associated with factor Xa inhibitors (ANNEXA-4). N Engl J Med. 2019;380(14):1326-1335. doi.org/10.1056/NEJMoa1814051 Pivotal data supporting andexanet alfa as the FDA-approved reversal agent for rivaroxaban-associated major bleeding.
  4. Martin K, Beyer-Westendorf J, Davidson BL, et al. Use of direct oral anticoagulants in patients with obesity for treatment and prevention of venous thromboembolism: updated communication from the ISTH SSC. J Thromb Haemost. 2021;19(8):1874-1882. doi.org/10.1111/jth.15358 ISTH guidance on DOAC use in obesity; informs body-weight cautions for rivaroxaban.