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Drug Monograph

Comtan (Entacapone)

entacapone
Peripheral COMT Inhibitor·Oral Tablet
Pharmacokinetic Profile
Half-Life
Biphasic: 0.4–0.7 h (β); 2.4 h (γ)
Metabolism
Isomerisation → glucuronidation (non-CYP)
Protein Binding
98% (serum albumin)
Bioavailability
35%
Volume of Distribution
20 L (limited tissue distribution)
Clinical Information
Drug Class
Peripheral COMT inhibitor
Available Dose
200 mg (single strength only)
Route
Oral
Renal Adjustment
Not required (no important PK effects)
Hepatic Adjustment
Caution: AUC/Cmax doubled in cirrhosis; EMA contraindicates
Pregnancy
Category C; always co-prescribed with LD/CD (teratogenic in animals)
Lactation
Excreted in rat milk; unknown in humans
Schedule
Prescription only (not scheduled)
Generic Available
Yes
Rx

Indications

IndicationApproved PopulationTherapy TypeStatus
Parkinson’s disease — adjunct to levodopa/carbidopa for end-of-dose “wearing-off”AdultsAlways adjunctive to LD/CD (or LD/benserazide)FDA Approved

Entacapone is a selective, reversible, peripherally acting COMT inhibitor indicated exclusively as an adjunct to levodopa/carbidopa (or levodopa/benserazide) therapy. By blocking peripheral COMT-mediated methylation of levodopa, entacapone increases the AUC of levodopa by approximately 35% and extends its elimination half-life from about 1.3 hours to 2.4 hours, leading to more sustained dopaminergic stimulation. It is specifically targeted at patients experiencing end-of-dose motor fluctuations (“wearing-off”). Entacapone has no anti-parkinsonian effect when used alone and must always be administered alongside levodopa.

Key Distinction from Tolcapone

Unlike tolcapone, entacapone acts only peripherally (does not cross the blood-brain barrier significantly) and does not require mandatory liver function monitoring. Tolcapone carries an FDA boxed warning for fatal hepatotoxicity; entacapone does not.

Dose

Dosing

Standard Dosing — Adults With Motor Fluctuations

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
End-of-dose wearing-off — adjunct to LD/CD200 mg with each LD/CD dose200 mg with each LD/CD dose200 mg × 8/day = 1,600 mg/day (FDA)No titration required; flat dose with every LD intake
EMA allows up to 200 mg × 10/day (2,000 mg/day)
Patients on LD ≥800 mg/day or with moderate-severe dyskinesia200 mg with each LD/CD dose200 mg with each LD/CD dose + LD reduction1,600 mg/dayReduce LD dose by ~25% on average; >58% of patients on LD >800 mg/day required LD reduction in trials
Extending dosing interval may also be needed

Special Populations

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
Renal impairment (any severity)200 mg (standard)Standard1,600 mg/dayNo important PK effects of renal impairment (FDA PI)
EMA suggests dialysis patients may need increased dosing interval
Hepatic impairmentUse with caution; AUC and Cmax approximately doubled in cirrhosis patients. EMA contraindicates use in hepatic impairment.
Elderly (≥65 years)200 mg (standard)Standard1,600 mg/dayPK independent of age; no dose adjustment required
Clinical Pearl: No Titration Needed

Unlike dopamine agonists, entacapone requires no dose titration. The fixed 200 mg dose is taken with each levodopa dose from day one. The key dosing decision is whether to proactively reduce the levodopa dose by approximately 25% at initiation — strongly recommended when the patient is already on levodopa ≥800 mg/day or has significant dyskinesia.

Do Not Stop Abruptly

Although no cases of NMS following abrupt entacapone withdrawal were reported in clinical trials, postmarketing cases of a symptom complex resembling NMS have been reported in association with rapid dose reduction or withdrawal of dopaminergic drugs. Withdraw gradually and monitor closely, adjusting other dopaminergic therapies as needed.

PK

Pharmacology

Mechanism of Action

Entacapone is a selective and reversible inhibitor of catechol-O-methyltransferase (COMT), a ubiquitous enzyme that catalyses the O-methylation of catechol substrates including levodopa, dopamine, and catecholamine neurotransmitters. In the presence of an aromatic amino acid decarboxylase inhibitor such as carbidopa, COMT becomes the major peripheral metabolising pathway for levodopa. By blocking this pathway, entacapone prevents the conversion of levodopa to 3-O-methyldopa (3-OMD) in peripheral tissues, increasing the proportion of each levodopa dose reaching the brain. This manifests clinically as an approximately 35% increase in levodopa AUC and prolongation of levodopa half-life from about 1.3 to 2.4 hours, reducing motor fluctuations.

ADME Profile

ParameterValueClinical Implication
AbsorptionRapidly absorbed; Tmax ~1 h; bioavailability 35%; Cmax ~1.2 mcg/mL after 200 mg; food has no effect on PKCan be taken with or without food; taking with food may help if nausea occurs
DistributionVd 20 L (IV); 98% bound to serum albumin; does not cross BBB significantly; low lipophilicitySmall Vd and high protein binding confine entacapone to the peripheral compartment, explaining its peripheral-only COMT inhibition
MetabolismAlmost completely metabolised; isomerisation to cis-isomer → direct glucuronidation; glucuronide conjugate is inactive; 0.2% excreted unchanged in urine; non-CYP mediatedNo CYP-based drug interactions; hepatic impairment doubles AUC (biliary excretion is major route)
EliminationBiphasic: t½β 0.4–0.7 h; t½γ 2.4 h (γ-phase ~10% of AUC); total clearance 850 mL/min (IV); 10% urine / 90% faecesShort half-life necessitates dosing with each levodopa dose; renal impairment does not significantly affect PK
SE

Side Effects

Most adverse effects of entacapone result from enhanced dopaminergic activity (due to increased levodopa exposure) and can be managed by reducing the levodopa dose. Diarrhea and urine discolouration are unique to entacapone itself. Data below are from FDA PI double-blind, placebo-controlled trials (N=1,003 total; 603 entacapone, 400 placebo).

≥10%Very Common
Adverse EffectIncidenceClinical Note
Dyskinesia25% (vs 15% placebo)Most common adverse effect; due to increased LD exposure; reduce LD dose by ~25%; DC for dyskinesia 1.5% vs 0.8% placebo
Urine discolouration (brownish-orange)10% (vs 0% placebo)Benign; due to entacapone metabolites; reassure patient that it is harmless
Diarrhea10%May have delayed onset (4–12 weeks after initiation); can be severe/watery; may indicate colitis; most common reason for serious discontinuation
1–10%Common (≥3% Greater Than Placebo per FDA PI)
Adverse EffectIncidenceClinical Note
Nausea≥3% > placeboDopaminergic effect; usually manageable with LD dose reduction; take with food
Hyperkinesia≥3% > placeboRelated to enhanced LD exposure; reduce LD dose
Abdominal pain≥3% > placeboEvaluate for diarrhea-related causes or colitis if persistent
Vomiting≥3% > placeboDopaminergic; monitor hydration and electrolytes
Dry mouth≥3% > placeboMay overlap with anticholinergic medications in PD regimen
SeriousSerious (Regardless of Frequency)
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Diarrhea with colitisUncommon (subset of 10% diarrhea)4–12 weeks after initiation; can be delayed monthsDiscontinue entacapone; consider colonoscopy/biopsy if diarrhea persists after stopping; monitor hydration, potassium, weight
RhabdomyolysisRare (postmarketing)Variable; may relate to severe prolonged dyskinesiaCheck CPK; discontinue if confirmed; may be linked to NMS-like syndrome
NMS-like syndrome (hyperpyrexia, rigidity, altered consciousness)Rare (postmarketing)During rapid withdrawal or dose reduction of dopaminergic therapyWithdraw gradually; supportive care; monitor CPK, temperature
Hallucinations / psychosisUncommon; led to DC and hospitalisation in trialsVariableReduce LD dose or discontinue entacapone; evaluate for pimavanserin or low-dose quetiapine
Impulse control disordersUncommon (class effect of dopaminergic therapy)Weeks to monthsScreen at every visit; dose reduction of dopaminergic therapy; involve caregivers
DiscontinuationDiscontinuation Rates
Entacapone (N=603)
14% vs 9% placebo (N=400)
Top reasons: Psychiatric disorders, diarrhea, dyskinesia/hyperkinesia, nausea, abdominal pain
Diarrhea-Related DC
2% vs 0% placebo
Most common reason for severe discontinuation; may recur on rechallenge
Reason for DiscontinuationEntacaponePlacebo
Psychiatric disorders2%1%
Diarrhea2%0%
Dyskinesia / hyperkinesia2%1%
Nausea2%1%
Abdominal pain1%0%
Aggravation of PD symptoms1%1%
Managing Diarrhea

Diarrhea affects approximately 10% of patients and may have a uniquely delayed onset (4–12 weeks). In some patients, biopsy-confirmed colitis has been identified. If prolonged diarrhea is suspected to be drug-related, entacapone should be discontinued. Diarrhea has recurred upon rechallenge in some patients with confirmed colitis. Monitor hydration, weight, and potassium levels in affected patients.

Int

Drug Interactions

Entacapone does not undergo CYP-mediated metabolism and has a distinct interaction profile from dopamine agonists. Its primary interactions stem from COMT inhibition affecting catechol-structured drugs and its effects on levodopa pharmacokinetics.

MajorNon-Selective MAO Inhibitors (phenelzine, tranylcypromine)
MechanismCombined COMT + MAO inhibition prevents two major catecholamine degradation pathways
EffectPotential for hypertensive crisis from accumulated catecholamines
ManagementAvoid concomitant use of non-selective MAOIs; selective MAO-B inhibitors (selegiline, rasagiline) are acceptable
FDA PI
ModerateCOMT-Metabolised Catecholamines (epinephrine, norepinephrine, dobutamine, isoproterenol)
MechanismCOMT inhibition reduces metabolism of exogenous catecholamines
EffectPotentiated haemodynamic effects (tachycardia, arrhythmia, excessive BP changes)
ManagementUse with caution; monitor cardiovascular response closely if catecholamines required
FDA PI
ModerateMethyldopa / Bitolterol
MechanismBoth contain catechol structures metabolised by COMT
EffectIncreased plasma levels and prolonged effects of these drugs
ManagementMonitor closely; dose adjustments of interacting drug may be necessary
FDA PI
ModerateIron Supplements / Cholestyramine
MechanismChelation (iron) or bile acid binding (cholestyramine) may reduce entacapone absorption
EffectReduced entacapone bioavailability
ManagementSeparate administration by at least 2 hours
FDA PI
MinorSelegiline (MAO-B Inhibitor)
MechanismNo pharmacokinetic interaction demonstrated
EffectNo significant interaction in >600 patients studied
ManagementSafe to combine; no dose adjustment needed
FDA PI
MinorLevodopa / Carbidopa
MechanismEntacapone increases LD AUC by ~35% and extends LD t½ from 1.3 to 2.4 h (by design)
EffectEnhanced dopaminergic effects — including dyskinesia (25% vs 15% placebo)
ManagementReduce LD dose by ~25% if LD ≥800 mg/day or dyskinesia present; expected therapeutic interaction
FDA PI
Mon

Monitoring

  • DyskinesiaEach visit; closely at initiation
    Routine    Most common adverse effect (25%); typically requires LD dose reduction. Evaluate within days to weeks of starting entacapone.
  • Diarrhea / GIEach visit for first 3 months; then ongoing
    Routine    Delayed onset (4–12 weeks); monitor hydration, weight, potassium. If prolonged, consider colonoscopy; discontinue entacapone.
  • Blood PressureBaseline, each visit
    Routine    Orthostatic hypotension may occur, especially during initial therapy. Lying and standing measurements.
  • NeuropsychiatricEach visit
    Routine    Hallucinations, psychosis, confusion; enhanced dopaminergic tone is the mechanism. Screen for ICDs (gambling, hypersexuality).
  • Hepatic FunctionBaseline (if clinical suspicion)
    Trigger-Based    Unlike tolcapone, mandatory LFT monitoring is NOT required. However, check baseline LFTs if hepatic disease suspected, as AUC doubles in cirrhosis.
  • Skin ExaminationAnnually
    Routine    PD patients have an elevated melanoma risk (disease-related, not drug-specific).
  • CPKIf symptoms arise
    Trigger-Based    Check if fever, rigidity, myalgia, or altered consciousness develop (rhabdomyolysis/NMS concern).
CI

Contraindications & Cautions

Absolute Contraindications

  • Hypersensitivity to entacapone or any excipient (FDA PI).
  • Hepatic impairment (EMA SmPC; FDA PI advises caution rather than absolute contraindication).
  • Pheochromocytoma (EMA SmPC; risk of hypertensive crisis via COMT inhibition of catecholamines).

Relative Contraindications (Specialist Input Recommended)

  • Concomitant non-selective MAO inhibitors: Risk of hypertensive crisis. Selective MAO-B inhibitors (selegiline, rasagiline) are safe.
  • History of rhabdomyolysis or NMS: Postmarketing cases reported; exercise caution.

Use with Caution

  • Biliary obstruction: Major excretion route is biliary; impaired biliary flow may increase exposure.
  • Patients with history of diarrhea-related colitis: Entacapone-associated diarrhea/colitis has recurred on rechallenge.
  • Pregnancy/Lactation: Always co-administered with LD/CD (known teratogen in animals); excreted in rat milk.
FDA Class-Wide Regulatory Warning Falling Asleep During Activities of Daily Living

Patients treated with dopaminergic medications, including entacapone in combination with levodopa, have reported suddenly falling asleep without warning during daily activities. Patients should be advised not to drive or engage in hazardous activities until they have gained sufficient experience with the medication.

Pt

Patient Counselling

Purpose of Therapy

Entacapone is an “add-on” medication that makes your levodopa work longer. It does not replace levodopa and has no effect on its own. By taking entacapone with each levodopa dose, the levodopa stays active in your body for a longer period, which helps reduce the return of symptoms (“wearing off”) between doses.

How to Take

Take one 200 mg tablet at the same time as each levodopa/carbidopa dose, up to 8 times per day. The tablet can be taken with or without food. Do not break or crush the tablet. Do not take extra doses — the dose is always 200 mg.

Urine Colour Change
Tell patientYour urine may turn brownish-orange. This is completely harmless and caused by the medication’s breakdown products. It may also slightly discolour sweat.
Call prescriberNot required for colour change alone; however, report dark brown or cola-coloured urine (may indicate rhabdomyolysis).
Involuntary Movements (Dyskinesia)
Tell patientThis medication boosts the effect of levodopa, which may increase involuntary movements. Your prescriber may reduce your levodopa dose to manage this.
Call prescriberIf involuntary movements are bothersome or worsening.
Diarrhea
Tell patientDiarrhea can occur and may start weeks after you begin the medication. Drink plenty of fluids and monitor your weight. It usually resolves after stopping the medication.
Call prescriberIf diarrhea is severe, watery, persistent (more than a few days), or accompanied by abdominal pain, weight loss, or dehydration.
Do Not Stop Suddenly
Tell patientStopping suddenly can cause a dangerous condition with high fever, muscle stiffness, and confusion. Always follow your prescriber’s instructions when stopping this medication.
Call prescriberIf you develop fever, severe stiffness, or confusion, especially if any of your Parkinson’s medications have been changed.
Unusual Urges & Compulsive Behaviours
Tell patientMedications that increase dopamine activity, including this one taken with levodopa, can cause unusual urges such as gambling, increased sexual behaviour, or compulsive shopping.
Call prescriberIf you or your family notice new or increased gambling, spending, sexual urges, or compulsive eating.
Ref

Sources

Regulatory (PI / SmPC)
  1. COMTAN (entacapone) Tablets — FDA Prescribing Information. Revised 2014. accessdata.fda.govPrimary regulatory source for dosing, PK data, adverse reaction tables, drug interactions, and discontinuation rates.
  2. COMTAN (entacapone) Tablets — FDA Prescribing Information. Revised 2010. accessdata.fda.govEarlier label version with identical PK parameters and clinical trial results; confirms consistency of regulatory data.
  3. Comtan (entacapone) — EMA Summary of Product Characteristics. ema.europa.euEuropean regulatory source; contraindicates hepatic impairment and pheochromocytoma; allows max 10 doses/day (2000 mg).
Key Clinical Trials
  1. Rinne UK, Larsen JP, Siden A, Worm-Petersen J. Entacapone enhances the response to levodopa in parkinsonian patients with motor fluctuations. Neurology. 1998;51(5):1309–1314. doi:10.1212/WNL.51.5.1309Nordic pivotal trial (N=171) demonstrating +1.5 h “on” time and −87 mg/day LD dose reduction with entacapone.
  2. Parkinson Study Group. Entacapone improves motor fluctuations in levodopa-treated Parkinson’s disease patients. Ann Neurol. 1997;42(5):747–755. doi:10.1002/ana.410420511North American pivotal trial (N=205) supporting FDA approval; primary endpoint was proportion of awake time “on.”
  3. Stocchi F, Rascol O, Kieburtz K, et al. Initiating levodopa/carbidopa therapy with and without entacapone in early Parkinson disease: the STRIDE-PD study. Ann Neurol. 2010;68(1):18–27. doi:10.1002/ana.22060Large RCT (N=747) that found earlier onset of dyskinesia with initial LD/CD/entacapone vs LD/CD alone; shaped current use for fluctuators only.
Guidelines
  1. Fox SH, Katzenschlager R, Lim SY, et al. International Parkinson and Movement Disorder Society Evidence-Based Medicine Review: Update on Treatments for the Motor Symptoms of Parkinson’s Disease. Mov Disord. 2018;33(8):1248–1266. doi:10.1002/mds.27372MDS evidence review classifying COMT inhibitors as “efficacious” for reducing off-time in motor fluctuations.
  2. National Institute for Health and Care Excellence (NICE). Parkinson’s disease in adults. NICE guideline [NG71]. Updated 2024. nice.org.ukUK guideline recommending COMT inhibitors as adjunctive therapy for motor fluctuations in PD.
Mechanistic / Basic Science
  1. Kaakkola S. Clinical pharmacology, therapeutic use and potential of COMT inhibitors in Parkinson’s disease. Drugs. 2000;59(6):1233–1250. doi:10.2165/00003495-200059060-00004Comprehensive review of COMT pharmacology; source for mechanism details and peripheral vs central COMT inhibition.
  2. Nissinen E, Lindén IB, Schultz E, Pohto P. Biochemical and pharmacological properties of a peripherally acting catechol-O-methyltransferase inhibitor entacapone. Naunyn Schmiedebergs Arch Pharmacol. 1992;346(3):262–266. doi:10.1007/BF00173538Original preclinical characterisation of entacapone as a peripheral COMT inhibitor.
Pharmacokinetics / Special Populations
  1. Entacapone. In: DailyMed [Internet]. Bethesda (MD): U.S. National Library of Medicine. dailymed.nlm.nih.govGeneric label confirming PK parameters (t½, Vd, bioavailability, clearance) and adverse reaction data.
  2. Entacapone. In: Drugs.com Professional Drug Information. drugs.com/proConsolidated prescribing information with detailed pharmacokinetic tables and drug interaction data.
  3. Brooks DJ, Sagar H, and the UK-Irish Entacapone Study Group. Entacapone is beneficial in both fluctuating and non-fluctuating patients with Parkinson’s disease: a randomised, placebo controlled, double blind, six month study. J Neurol Neurosurg Psychiatry. 2003;74(8):1071–1079. doi:10.1136/jnnp.74.8.1071UK-Irish trial demonstrating benefit of entacapone in both fluctuating and non-fluctuating PD patients; an additional phase III study beyond the three pivotal trials.