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Drug Monograph

Rivastigmine (Exelon)

rivastigmine tartrate
Cholinesterase Inhibitor (AChE + BuChE) · Oral (Capsule, Solution) & Transdermal Patch
Pharmacokinetic Profile
Half-Life
~1.5 h (PK); 8–10 h (PD effect)
Metabolism
Cholinesterase hydrolysis (not CYP450)
Protein Binding
~40%
Bioavailability
~36% (oral, 3 mg dose)
Volume of Distribution
1.8–2.7 L/kg
Clinical Information
Drug Class
Cholinesterase inhibitor (dual AChE/BuChE)
Available Doses
Caps: 1.5, 3, 4.5, 6 mg; Patch: 4.6, 9.5, 13.3 mg/24 h
Route
Oral & Transdermal
Renal Adjustment
May tolerate lower doses only
Hepatic Adjustment
Mild–moderate: lower doses; Severe: not studied
Pregnancy
No adequate studies; use only if benefit outweighs risk
Lactation
Unknown if excreted in human milk; caution advised
Schedule
Rx only (not scheduled)
Generic Available
Yes
Rx

Rivastigmine Indications

IndicationApproved PopulationTherapy TypeStatus
Mild-to-moderate Alzheimer’s disease dementiaAdultsMonotherapyFDA Approved
Mild, moderate, and severe Alzheimer’s disease dementiaAdults (transdermal patch only)MonotherapyFDA Approved
Mild-to-moderate Parkinson’s disease dementiaAdultsMonotherapyFDA Approved

Rivastigmine is one of the cornerstone pharmacotherapies for dementia associated with both Alzheimer’s disease (AD) and Parkinson’s disease (PD). The oral formulation is approved for mild-to-moderate disease severity, while the transdermal patch received expanded approval in 2013 to cover all stages of AD including severe dementia. Its dual inhibition of both acetylcholinesterase and butyrylcholinesterase distinguishes it pharmacologically from donepezil and galantamine, which are selective for AChE. This broader mechanism may offer particular benefit in patients with prominent neuropsychiatric symptoms such as hallucinations and behavioural disturbance.

Off-Label Uses

Dementia with Lewy bodies (DLB): Rivastigmine has been studied in open-label trials for cognitive and behavioural symptoms of DLB, given the overlap between DLB and PDD neuropathology. Evidence quality: Moderate.

Postoperative delirium prevention: Small RCTs suggest the rivastigmine patch may reduce delirium incidence in older surgical patients with pre-existing cognitive impairment. Evidence quality: Low.

Gait instability in Parkinson’s disease (without dementia): The ReSPonD trial (Phase 2) demonstrated reductions in fall frequency with oral rivastigmine in PD patients without dementia. Evidence quality: Moderate.

Dose

Rivastigmine Dosing

Oral Dosing by Clinical Scenario

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
Alzheimer’s dementia — new diagnosis, oral1.5 mg BID3–6 mg BID6 mg BID (12 mg/day)Titrate by 1.5 mg/dose every 2 weeks as tolerated
Give with food; higher doses correlate with greater benefit (FDA PI)
Parkinson’s disease dementia — oral1.5 mg BID3–6 mg BID6 mg BID (12 mg/day)Slower titration: increase by 1.5 mg/dose every 4 weeks
Longer titration interval reduces GI side effects
Alzheimer’s dementia — transdermal patch initiation4.6 mg/24 h patch9.5 mg/24 h patch13.3 mg/24 h patchIncrease after minimum 4 weeks at each dose
9.5 mg/24 h is the minimum effective patch dose
Severe Alzheimer’s dementia — transdermal patch4.6 mg/24 h patch13.3 mg/24 h patch13.3 mg/24 h patchTarget the highest tolerated dose
ACTION trial supported 13.3 mg/24 h in severe AD
Parkinson’s disease dementia — transdermal patch4.6 mg/24 h patch9.5 mg/24 h patch13.3 mg/24 h patchIncrease after minimum 4 weeks per step
Patch associated with fewer GI effects than capsules in PDD
Switching from oral to transdermal<6 mg/day oral → 4.6 mg/24 h patch; 6–12 mg/day oral → 9.5 mg/24 h patch13.3 mg/24 h patchApply first patch the day after last oral dose
Do not use patch and oral simultaneously
Treatment interruption — restart1.5 mg BID (oral) or 4.6 mg/24 h (patch)Re-titrate to targetSame as original targetIf interrupted >3 days, restart at lowest dose and re-titrate
Abrupt re-initiation at prior dose risks severe vomiting

Special Population Adjustments

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
Low body weight (<50 kg)1.5 mg BIDIndividually titratedTolerated doseDrug exposure approximately doubles at 35 kg vs 65 kg; monitor closely for GI toxicity
Hepatic impairment (Child-Pugh A/B)1.5 mg BID or 4.6 mg/24 h patchLower doses only4.6 mg/24 h patch (per StatPearls)Oral clearance 60–65% lower in hepatic impairment; severe (Child-Pugh C) not studied
Renal impairment (moderate–severe)1.5 mg BID or 4.6 mg/24 h patchIndividually titratedTolerated doseMay tolerate lower doses only; titrate based on tolerability
Clinical Pearl: Transdermal Patch Advantages

The 9.5 mg/24 h patch delivers comparable systemic exposure to the maximum oral dose (12 mg/day capsules) but with a smoother pharmacokinetic profile. In the IDEAL trial, the patch produced approximately two-thirds fewer reports of nausea and vomiting compared with oral capsules at equivalent efficacy, making it the preferred formulation for patients with poor GI tolerability.

PK

Pharmacology

Mechanism of Action

Rivastigmine is a carbamate-type, pseudo-irreversible inhibitor of both acetylcholinesterase (AChE) and butyrylcholinesterase (BuChE). It forms a covalent carbamylated complex with the enzyme’s active-site serine residue, producing sustained inhibition that outlasts the drug’s short plasma half-life. The pharmacodynamic duration of effect is approximately 8 to 10 hours, even though plasma levels decline within 1–2 hours. This “slow-off” binding characteristic drives a disconnect between the brief pharmacokinetic half-life and the longer duration of clinical activity. Rivastigmine demonstrates regional selectivity in the CNS, preferentially inhibiting the G1 isoform of AChE concentrated in the hippocampus and cortex — areas critically involved in memory and executive function. Its additional inhibition of BuChE, which is up-regulated in AD brain tissue as AChE declines, may provide a pharmacological advantage in patients with more advanced or rapidly progressing disease, particularly those with prominent neuropsychiatric features such as hallucinations.

ADME Profile

ParameterValueClinical Implication
AbsorptionRapid and nearly complete (>96%); Tmax ~1 h oral; bioavailability ~36% at 3 mg (extensive first-pass metabolism); food delays Tmax by 90 min, reduces Cmax ~30%, but increases AUC ~30%Administer with food to improve tolerability and enhance overall exposure, though peak levels are lower
DistributionVd 1.8–2.7 L/kg; ~40% plasma protein binding; crosses BBB readily; CSF Tmax 1.4–2.6 h; CSF/plasma AUC ratio ~40%Extensive CNS penetration supports central pharmacological effect; low protein binding minimises displacement interactions
MetabolismPrimarily hydrolysed by target cholinesterases to decarbamylated metabolite (NAP226-90); minimal CYP450 involvement; nonlinear PK at doses >3 mg BID (3-fold AUC increase when doubling from 3 to 6 mg BID)CYP-independent metabolism makes rivastigmine one of the lowest interaction-risk cholinesterase inhibitors; saturable first-pass explains nonlinear kinetics at higher doses
Eliminationt½ ~1.5 h; >90% renally excreted as metabolites within 24 h; <1% in faecesShort half-life limits accumulation and allows rapid washout; dialysis is not effective for overdose due to rapid endogenous clearance
SE

Side Effects

Adverse effects are driven by peripheral and central cholinergic stimulation and are strongly dose-related. Gastrointestinal effects predominate during titration and often attenuate at stable doses. Incidence data below are from controlled clinical trials of oral rivastigmine 6–12 mg/day in Alzheimer’s disease (FDA PI, n = 1,189 rivastigmine vs n = 868 placebo) unless noted otherwise.

≥10% Very Common
Adverse EffectIncidenceClinical Note
Nausea47% (vs 12% placebo)Most common reason for discontinuation; higher during titration (43%) than maintenance (17%); take with food
Vomiting31% (vs 6% placebo)Higher during titration (24%) vs maintenance (14%); severe in 2% of patients; more frequent in women
Dizziness21% (vs 11% placebo)Central and cholinergic origin; advise caution with driving and machinery
Diarrhea19% (vs 11% placebo)Cholinergic-mediated increase in GI motility; usually self-limiting
Anorexia17% (vs 3% placebo)Monitor weight regularly; 26% of women on high doses experienced ≥7% weight loss
Headache17% (vs 12% placebo)Usually mild and transient; no specific management required
Abdominal pain13% (vs 6% placebo)Related to increased gastric acid secretion; consider antacids if persistent
1–10% Common
Adverse EffectIncidenceClinical Note
Fatigue9% (vs 5% placebo)May compound cognitive slowing in dementia patients; assess functional impact
Insomnia9% (vs 7% placebo)Consider timing of evening dose; avoid late-night administration
Dyspepsia9% (vs 4% placebo)Consistent with increased gastric acid; PPI or H2-blocker if needed
Confusion8% (vs 7% placebo)Difficult to distinguish from disease progression; evaluate if new-onset
Urinary tract infection7% (vs 6% placebo)Likely related to underlying population risk rather than drug mechanism
Asthenia6% (vs 2% placebo)Dose-related; may improve with dose adjustment
Depression6% (vs 4% placebo)Screen for mood changes at follow-up visits; may overlap with dementia-associated apathy
Malaise5% (vs 2% placebo)Non-specific; may be related to GI intolerance or anorexia
Somnolence5% (vs 3% placebo)Warn regarding driving impairment; particularly relevant in PDD population
Anxiety5% (vs 3% placebo)Cholinergic arousal may contribute; usually mild
Tremor4% (vs 1% placebo)Especially relevant in PDD (10.2% in EXPRESS trial); not reflected in UPDRS motor worsening
Increased sweating4% (vs 1% placebo)Cholinergic stimulation of sweat glands; typically mild
Weight loss3% (vs <1% placebo)18–26% of patients on high dose experienced ≥7% loss of baseline weight
Syncope3% (vs 2% placebo)Vagotonic effect on heart rate; assess in patients with cardiac conduction disease
Serious Serious Adverse Effects (Regardless of Frequency)
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Severe vomiting with dehydrationUncommonTitration phase or after dose re-initiationHold drug, IV fluid replacement, restart at lowest dose; esophageal rupture reported post-marketing after inappropriate re-initiation
Bradycardia / vagotonic cardiac effectsRareAny time during therapyECG monitoring in patients with sick sinus syndrome or conduction disorders; discontinue if symptomatic bradycardia
Gastrointestinal haemorrhage / peptic ulcerRareAny time; increased risk with NSAIDsMonitor for occult bleeding; discontinue if active bleed; avoid concurrent NSAIDs when possible
SeizuresRareAny timeDifferentiate from disease-related seizure activity; hold rivastigmine and evaluate
Disseminated allergic dermatitisVery rare (post-marketing)Days to weeks after patch initiationDiscontinue all rivastigmine formulations immediately; switch to oral form only after negative allergy testing
Cholinergic crisis (overdose)Very rareWithin hours of ingestionAtropine sulphate as antidote; supportive care; no role for dialysis given short half-life
Medication errors (patch dosing)Uncommon (post-marketing)Any time; especially with caregiver-applied patchesEnsure old patch is removed before applying new one; multiple patch application has caused hospitalisation and death
Discontinuation Discontinuation Rates
Alzheimer’s Disease (Oral)
15% vs 5% placebo (titration)
Maintenance phase: 6% vs 4% placebo. Top reasons: nausea (8%), vomiting (5%), anorexia (3%), dizziness (2%)
Parkinson’s Disease Dementia (Oral)
18% vs 11% placebo
Top reasons: nausea (3.6%), vomiting (1.9%), tremor (1.7%)
Reason for DiscontinuationIncidence (Rivastigmine)Context
Nausea8%vs <1% placebo; predominantly during titration phase
Vomiting5%vs <1% placebo; more common in women
Anorexia3%vs 0% placebo; often accompanied by clinically significant weight loss
Dizziness2%vs <1% placebo; central cholinergic effect
Managing GI Side Effects

Always administer rivastigmine with food. Use the slowest tolerated titration schedule. If nausea or vomiting becomes intolerable, hold for several doses and restart at the same or next lower dose. If treatment is interrupted for more than 3 days, restart from the lowest dose (1.5 mg BID oral or 4.6 mg/24 h patch) to prevent severe vomiting. Consider switching to the transdermal patch, which produces significantly fewer GI adverse effects at equivalent therapeutic exposure.

Int

Drug Interactions

Rivastigmine has an unusually favourable interaction profile because it is metabolised by its own target enzymes (cholinesterases) rather than hepatic cytochrome P450 isoenzymes. Population pharmacokinetic analysis of 625 patients confirmed no clinically significant interactions with commonly prescribed medications including antihypertensives, beta-blockers, calcium channel blockers, NSAIDs, estrogens, and antihistamines. No pharmacokinetic interaction was observed with digoxin, warfarin, diazepam, or fluoxetine in dedicated healthy-volunteer studies. However, pharmacodynamic interactions at the cholinergic synapse remain clinically important.

Major Succinylcholine & depolarising neuromuscular blockers
MechanismCholinesterase inhibition prolongs succinylcholine neuromuscular block
EffectExaggerated and prolonged muscle relaxation during anaesthesia
ManagementInform anaesthetist; consider non-depolarising agents; may need dose reduction of succinylcholine
FDA PI
Major Anticholinergic drugs
MechanismDirect pharmacodynamic antagonism of cholinesterase inhibition
EffectReduced efficacy of rivastigmine; may negate cognitive benefits
ManagementAvoid concurrent use; review anticholinergic burden at each visit (e.g., oxybutynin, diphenhydramine, amitriptyline)
FDA PI
Moderate Beta-blockers
MechanismAdditive vagotonic effects on cardiac conduction
EffectIncreased risk of bradycardia and syncope; cardioselective beta-blockers (e.g., atenolol) may pose particular risk
ManagementConcomitant use not recommended per FDA PI; if unavoidable, monitor heart rate and blood pressure closely; assess for syncope at each visit
FDA PI
Moderate Metoclopramide
MechanismAdditive cholinergic stimulation of GI motility
EffectIncreased risk of extrapyramidal symptoms and GI adverse effects
ManagementAvoid concomitant use; if antiemetic needed, prefer ondansetron or domperidone
FDA PI
Moderate Other cholinomimetic agents (bethanechol, pilocarpine)
MechanismAdditive cholinergic stimulation at muscarinic receptors
EffectExcessive cholinergic effects: bradycardia, salivation, bronchoconstriction, GI distress
ManagementAvoid concurrent use; if necessary, monitor closely for signs of cholinergic toxicity
FDA PI
Moderate NSAIDs
MechanismRivastigmine increases gastric acid; NSAIDs reduce mucosal protection
EffectTheoretically increased risk of peptic ulcer and GI bleeding
ManagementMonitor for GI bleeding; consider gastroprotection with PPI if chronic NSAID use required
FDA PI / Lexicomp
Minor Digoxin
MechanismNo pharmacokinetic interaction demonstrated; theoretical additive vagotonic effect
EffectMinimal clinical significance in dedicated studies
ManagementNo dosage adjustment needed; monitor heart rate in high-risk patients
FDA PI (Healthy volunteer study)
Minor Warfarin
MechanismNo pharmacokinetic interaction; rivastigmine does not affect CYP2C9 or warfarin PK
EffectNo effect on prothrombin time or INR in dedicated study
ManagementNo dosage adjustment needed; routine INR monitoring as standard of care
FDA PI (Healthy volunteer study)
Mon

Monitoring

  • Cognitive function Baseline, then every 3–6 months
    Routine     Use standardised tools (MMSE, MoCA) to assess whether therapy is providing benefit. If no stabilisation or improvement after 3–6 months at target dose, reassess continuation of treatment.
  • Body weight Each visit during titration, then every 3 months
    Routine     Significant weight loss (≥7% baseline) occurred in 18–26% of patients on high oral doses. Assess nutritional status; consider dietitian referral if weight loss is progressive.
  • GI tolerability Each visit during titration
    Routine     Ask about nausea, vomiting, diarrhea, and appetite at each dose escalation. Hold and re-titrate if symptoms are intolerable. Consider switching to transdermal patch for persistent GI effects.
  • Heart rate & ECG Baseline; then as clinically indicated
    Trigger-based     Vagotonic effects may cause bradycardia, especially in patients with pre-existing sick sinus syndrome, supraventricular conduction defects, or concurrent use of beta-blockers. Obtain ECG if syncope or dizziness is reported.
  • Motor function (PDD) Every 3 months in PDD patients
    Routine     Worsening of parkinsonian symptoms (particularly tremor) has been observed. Monitor with UPDRS if available. Although motor score deterioration was not significant in the EXPRESS trial, individual patients may be affected.
  • Patch application sites At each patch change; review at clinic visits
    Routine     Inspect for application-site erythema, oedema, or vesicles. Rotate sites every 24 h; do not reuse the same site within 14 days. Discontinue if reaction spreads beyond patch area or does not resolve within 48 h of removal.
  • Hepatic function Baseline in at-risk patients
    Trigger-based     Oral clearance is 60–65% lower in hepatically impaired patients. Baseline liver function tests in patients with known liver disease; adjust dose accordingly.
CI

Contraindications & Cautions

Absolute Contraindications

  • Known hypersensitivity to rivastigmine, other carbamate derivatives, or any component of the formulation
  • Previous allergic contact dermatitis to the rivastigmine transdermal patch, in the absence of negative allergy testing confirming it is safe to retry

Relative Contraindications (Specialist Input Recommended)

  • Sick sinus syndrome or supraventricular conduction disorders: Vagotonic effects may worsen bradycardia; cardiology input recommended before initiating
  • Active peptic ulcer disease or GI bleeding: Cholinesterase inhibition increases gastric acid secretion; gastroenterology clearance advisable
  • Severe hepatic impairment (Child-Pugh C): No dosing data available; significantly reduced clearance expected
  • Body weight <50 kg with history of severe GI intolerance: Substantially higher drug exposure increases toxicity risk

Use with Caution

  • Asthma or COPD: Cholinergic stimulation may cause bronchoconstriction
  • Urinary obstruction: Cholinomimetic effects may exacerbate retention symptoms
  • History of seizures: Cholinergic agents have theoretical pro-convulsant potential; seizures also occur as part of AD progression
  • Concurrent NSAID use: Monitor for GI bleeding; gastroprotection recommended
  • Planned surgery requiring general anaesthesia: Inform anaesthetist; rivastigmine may potentiate succinylcholine-type muscle relaxants
FDA Safety Communication Medication Errors with Rivastigmine Transdermal Patch

Post-marketing reports have documented serious adverse events — including hospitalisation and, rarely, death — resulting from medication errors with the transdermal patch. The most common error is failure to remove the old patch before applying a new one, leading to accidental overdose. Caregivers must be educated to remove the previous day’s patch before placing a new one and to apply only one patch at a time. Each used patch should be folded adhesive-side together and disposed of safely.

Pt

Patient Counselling

Purpose of Therapy

Rivastigmine is prescribed to help preserve memory, thinking, and the ability to perform daily activities in people with Alzheimer’s disease or Parkinson’s disease dementia. It works by boosting the levels of a chemical messenger in the brain called acetylcholine. It does not cure the underlying disease, but it may slow the rate of cognitive decline and maintain independence for a longer period. Caregivers play a central role in ensuring the medication is taken correctly and in reporting any new symptoms to the prescribing clinician.

How to Take

Capsules: Take with food in the morning and evening. Swallow whole with water. Patch: Apply once daily to clean, dry, hairless skin on the upper back, chest, or upper arm. Press firmly for 30 seconds. Remove the old patch before applying a new one. Rotate application sites and do not reuse the same area for 14 days. Replace the patch at the same time each day.

Nausea & Vomiting
Tell patient Stomach upset is common when the dose is being increased and usually improves over 1–2 weeks at a stable dose. Always take with food. If you are sick (vomiting) repeatedly, stop taking the medicine and contact your doctor before restarting — do not restart at the same dose on your own.
Call prescriber If vomiting persists beyond 24 hours, if unable to keep fluids down, or if therapy has been missed for more than 3 days.
Weight Loss & Appetite
Tell patient Reduced appetite is a known effect. Eat small frequent meals rather than three large ones. Caregivers should weigh the patient regularly and note trends.
Call prescriber If weight loss exceeds 5% of body weight, or if the patient refuses most meals for more than a few days.
Dizziness & Drowsiness
Tell patient Dizziness may occur, especially early in treatment. Avoid driving, using machinery, or performing hazardous activities until you know how this medicine affects you. Rise slowly from sitting or lying positions.
Call prescriber If fainting (syncope) occurs, or if dizziness does not improve after the first few weeks.
Patch Application (Transdermal Formulation)
Tell patient Apply only one patch at a time. Always remove the old patch before applying a new one. Rotate the site each day. Fold used patches in half (sticky side inward) and dispose of safely out of reach of children and pets. Do not cut or damage the patch.
Call prescriber If a skin reaction (redness, blisters, swelling) occurs at the patch site that does not improve within 48 hours of patch removal, or if the reaction spreads beyond the patch area.
Treatment Interruptions
Tell patient If you miss doses for 3 days or fewer, you can restart at your current dose. If you miss more than 3 days, do NOT restart at your previous dose — call your doctor first. Restarting at a high dose without re-titrating can cause severe vomiting.
Call prescriber If treatment has been interrupted for more than 3 days for any reason, including hospitalisation.
Surgery or Dental Procedures
Tell patient Inform the anaesthetist or surgeon that you are taking rivastigmine, as it may interact with certain muscle-relaxant drugs used during surgery.
Call prescriber Before any planned surgery requiring general anaesthesia.
Ref

Sources

Regulatory (PI / SmPC)
  1. Exelon (rivastigmine tartrate) Capsules and Oral Solution — FDA-approved Prescribing Information. Novartis Pharmaceuticals. Revised 2018. accessdata.fda.gov Primary source for oral rivastigmine dosing, adverse reactions, pharmacokinetics, and drug interactions.
  2. Exelon Patch (rivastigmine transdermal system) — FDA-approved Prescribing Information. Novartis Pharmaceuticals. Revised 2015. accessdata.fda.gov Source for transdermal patch dosing, switching from oral, application-site reaction data, and severe AD indication.
  3. Rivastigmine Transdermal System — DailyMed label (Amneal Pharmaceuticals, revised July 2024). dailymed.nlm.nih.gov Most recently revised generic transdermal label; confirms current dosing and safety information.
Key Clinical Trials
  1. Emre M, Aarsland D, Albanese A, et al. Rivastigmine for dementia associated with Parkinson’s disease. N Engl J Med. 2004;351(24):2509-2518. doi:10.1056/NEJMoa041470 Landmark EXPRESS trial establishing rivastigmine efficacy in PDD; source for PDD adverse event incidence rates.
  2. Winblad B, Cummings J, Andreasen N, et al. A six-month double-blind, randomized, placebo-controlled study of a transdermal patch in Alzheimer’s disease — rivastigmine patch versus capsule (IDEAL study). Int J Geriatr Psychiatry. 2007;22(5):456-467. doi:10.1002/gps.1788 Demonstrated equivalence of 9.5 mg/24 h patch to 12 mg/day capsules with fewer GI adverse effects.
  3. Farlow MR, Grossberg GT, Sadowsky CH, et al. A 24-week, randomized, controlled trial of rivastigmine patch 13.3 mg/24 h versus 4.6 mg/24 h in severe Alzheimer’s dementia (ACTION study). CNS Neurosci Ther. 2013;19(10):745-752. doi:10.1111/cns.12158 Supported FDA approval of high-dose patch for severe AD; provided safety data in advanced disease.
  4. Henderson EJ, Lord SR, Brodie MA, et al. Rivastigmine for gait stability in patients with Parkinson’s disease (ReSPonD): a randomised, double-blind, placebo-controlled, phase 2 trial. Lancet Neurol. 2016;15(3):249-258. doi:10.1016/S1474-4422(15)00389-0 Phase 2 trial of rivastigmine for fall prevention in PD without dementia; supports off-label gait instability use.
Guidelines
  1. Seppi K, Ray Chaudhuri K, Coelho M, et al. Update on treatments for nonmotor symptoms of Parkinson’s disease — an evidence-based medicine review (MDS Evidence-Based Medicine Committee). Mov Disord. 2019;34(2):180-198. doi:10.1002/mds.27602 MDS evidence-based review classifying rivastigmine as efficacious for PDD treatment.
  2. National Institute for Health and Care Excellence (NICE). Dementia: assessment, management, and support for people living with dementia and their carers. NICE guideline [NG97]. 2018 (updated 2023). nice.org.uk/guidance/ng97 UK guideline recommending AChE inhibitors (including rivastigmine) as first-line for mild-to-moderate AD and PDD.
Mechanistic / Basic Science
  1. Polinsky RJ. Clinical pharmacology of rivastigmine: a new-generation acetylcholinesterase inhibitor for the treatment of Alzheimer’s disease. Clin Ther. 1998;20(4):634-647. doi:10.1016/S0149-2918(98)80127-6 Foundational pharmacology review covering dual AChE/BuChE inhibition and regional brain selectivity.
Pharmacokinetics / Special Populations
  1. Hossain M, Jhee SS, Shiovitz T, et al. Estimation of the absolute bioavailability of rivastigmine in patients with mild to moderate dementia of the Alzheimer’s type. Clin Pharmacokinet. 2002;41(3):225-234. doi:10.2165/00003088-200241030-00006 Definitive bioavailability study establishing ~36–72% bioavailability depending on analytical method.
  2. Emre M, Poewe W, De Deyn PP, et al. Long-term safety of rivastigmine in Parkinson disease dementia: an open-label, randomized study. Clin Neuropharmacol. 2014;37(1):9-16. doi:10.1097/WNF.0000000000000010 76-week study comparing capsule vs patch safety in PDD; provides long-term adverse event data.
  3. Poewe W, Wolters E, Emre M, et al. Long-term benefits of rivastigmine in dementia associated with Parkinson’s disease: an active treatment extension study. Mov Disord. 2006;21(4):456-461. doi:10.1002/mds.20700 48-week open-label extension of the EXPRESS trial confirming sustained cognitive benefits in PDD.