Donepezil: Complete Drug Monograph

Pharmacokinetic Profile

Half-Life

~70 h (range 60–104 h; longer in elderly)

Metabolism

Hepatic via CYP3A4 & CYP2D6; glucuronidation

Protein Binding

96% (albumin ~75%, alpha-1-acid glycoprotein ~21%)

Bioavailability

100% (relative oral)

Volume of Distribution

12–16 L/kg (steady state)

Clinical Information

Drug Class

Reversible acetylcholinesterase (AChE) inhibitor; piperidine derivative

Available Doses

5 mg, 10 mg, 23 mg tablets; 5 mg, 10 mg ODT; transdermal 5 mg, 10 mg

Route

Oral; Transdermal

Renal Adjustment

Not required (clearance unchanged in renal impairment)

Hepatic Adjustment

No formal adjustment; clearance reduced ~20% in stable cirrhosis

Pregnancy

May cause fetal harm based on animal data; use only if clearly needed

Lactation

Unknown if excreted in human milk; weigh benefits vs risks

Schedule

Not a controlled substance

Generic Available

Yes (5 mg, 10 mg tablets and ODT)

Indications for Donepezil

Indication	Approved Population	Therapy Type	Status
Mild to moderate Alzheimer disease dementia	Adults	Monotherapy or with memantine	FDA Approved
Moderate to severe Alzheimer disease dementia (includes severe)	Adults	Monotherapy or with memantine	FDA Approved

Donepezil was first approved by the FDA in 1996 for mild to moderate Alzheimer disease, with approval for severe disease following in 2006. The 23 mg tablet was approved in 2010 for moderate to severe stages. Donepezil does not alter the underlying neurodegenerative pathology of Alzheimer disease but has demonstrated efficacy in slowing symptom progression by improving cognition and global function. It remains one of the most widely prescribed cholinesterase inhibitors worldwide and can be used alongside memantine (an NMDA antagonist) as combination therapy.

Off-Label Uses

Dementia with Lewy bodies (DLB) — 5–10 mg daily. Approved in Japan for DLB; used off-label elsewhere. Phase 2 and 3 RCTs demonstrate improvements in cognition, hallucinations, and caregiver burden (Mori et al., 2012; Ikeda et al., 2015). Evidence quality: Moderate.

Parkinson disease dementia — 5–10 mg daily. Some evidence of cognitive and executive function improvement (Dubois et al., 2012), though trial results are mixed. Evidence quality: Low.

Vascular dementia — 5–10 mg daily. Two large RCTs showed modest cognitive improvement but FDA application was rejected; limited effect on global functioning. Evidence quality: Low.

Traumatic brain injury — 5–10 mg daily. Emerging evidence for memory dysfunction improvement. Evidence quality: Very Low.

Dose

Dosing

Donepezil Dosing by Clinical Scenario — Adults

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Mild to moderate Alzheimer disease — initial therapy	5 mg once daily	5–10 mg once daily	10 mg/day	Do not increase to 10 mg until patient has been on 5 mg for 4–6 weeks Higher GI adverse events with 1-week titration vs 6-week titration
Moderate to severe Alzheimer disease — dose escalation	5 mg once daily	10–23 mg once daily	23 mg/day	Must be on 10 mg/day for at least 3 months before escalating to 23 mg 23 mg tablet must be swallowed whole; do not split, crush, or chew
Severe Alzheimer disease	5 mg once daily	10–23 mg once daily	23 mg/day	Same titration approach; higher rates of GI adverse effects and weight loss at 23 mg
Combination with memantine	5 mg once daily	10 mg once daily + memantine	23 mg/day	Fixed-dose combination (Namzaric: memantine ER 28 mg / donepezil 10 mg) also available No pharmacokinetic interaction between the two agents
Lewy body dementia (off-label)	3–5 mg once daily	5–10 mg once daily	10 mg/day	Approved in Japan for DLB; titrate slowly due to sensitivity in this population Monitor for worsening parkinsonism
Low body weight (<50 kg / <110 lb)	5 mg once daily	5 mg once daily	10 mg/day	Higher plasma levels may increase adverse effects; titrate cautiously

Clinical Pearl: Titration Speed Matters

In the pivotal trials, patients titrated from 5 mg to 10 mg over one week experienced nausea (19%), diarrhea (15%), and insomnia (14%). When the same dose escalation was spread over six weeks, rates dropped to levels comparable to the 5 mg group (nausea 6%, diarrhea 9%, insomnia 6%). The FDA label now recommends waiting 4–6 weeks before escalating from 5 mg to 10 mg (FDA PI). Some clinicians prefer an even more gradual approach, starting at 2.5 mg (half tablet) for the first 1–2 weeks in frail elderly patients.

Pharmacology

Mechanism of Action

Donepezil is a reversible, non-competitive inhibitor of acetylcholinesterase (AChE), the enzyme responsible for hydrolysing acetylcholine (ACh) in the synaptic cleft. By blocking AChE, donepezil increases the concentration and duration of action of ACh at cholinergic synapses throughout the brain, partially compensating for the loss of cholinergic neurons that characterises Alzheimer disease. Donepezil is highly selective for AChE over butyrylcholinesterase, with approximately 1,250-fold greater affinity for the former. This selectivity may contribute to its relatively favourable peripheral side-effect profile compared with non-selective agents. Donepezil also readily crosses the blood-brain barrier, achieving brain concentrations approximately twice those observed in plasma.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	100% relative oral bioavailability; Tmax 3–4 h (5/10 mg), ~8 h (23 mg); not affected by food or timing of administration; ODT bioequivalent to standard tablets	Once-daily dosing convenient; 23 mg tablet designed for slower absorption with higher Cmax (~2-fold vs 10 mg); take with or without food
Distribution	Vd 12–16 L/kg at steady state; 96% protein-bound (albumin ~75%, alpha-1-acid glycoprotein ~21%); crosses blood-brain barrier; brain:plasma ratio ~2:1	Large Vd reflects extensive tissue distribution; high CNS penetration underlies therapeutic effect; steady state reached in ~15 days
Metabolism	Hepatic via CYP3A4 and CYP2D6; also glucuronidation; produces 4 major metabolites (2 active); CYP2D6 has minor role (~17% clearance reduction with CYP2D6 inhibitors)	CYP3A4 inhibitors (e.g., ketoconazole) increase donepezil exposure by ~36%; CYP3A4 inducers may reduce levels; low affinity for CYP enzymes means minimal impact on other drugs
Elimination	t½ ~70 h; CL/F 0.13–0.19 L/hr/kg; 57% renally excreted (17% unchanged), 15–20% in feces; linear PK over 1–10 mg range	Long half-life supports once-daily dosing and allows 4–7-fold accumulation at steady state; clearance unchanged in moderate renal impairment; decreased ~20% in alcoholic cirrhosis

Side Effects

Adverse effect data below are drawn from pooled pivotal clinical trials of donepezil in mild to moderate Alzheimer disease (5 mg and 10 mg with 1-week titration vs placebo) and the 23 mg vs 10 mg controlled trial in moderate to severe disease. Most adverse effects are cholinomimetic in nature, dose-related, and often transient.

≥10% Very Common (10 mg, 1-Week Titration)

Adverse Effect	Incidence	Clinical Note
Nausea	19% vs 6% placebo	Most common complaint; rate drops to 6% with 6-week titration; often resolves within 1–3 weeks without dose modification
Diarrhea	15% vs 5% placebo	Cholinomimetic mechanism; encourage adequate hydration; usually transient
Insomnia	14% vs 6% placebo	May be reduced by switching to morning dosing (not in FDA label, but widely used clinically)

1–10% Common

Adverse Effect	Incidence	Clinical Note
Vomiting	8% (10 mg) vs 3% placebo; 9% (23 mg) vs 3% (10 mg)	Dose-related; may indicate need for slower titration; ensure adequate fluid intake
Muscle cramps	8% (10 mg) vs 2% placebo	Cholinomimetic effect on neuromuscular junction; usually nocturnal
Fatigue / asthenia	8% (10 mg) vs 3% placebo	May overlap with Alzheimer disease symptoms; assess for other causes
Anorexia / decreased appetite	7% (10 mg) vs 2% placebo; 5% (23 mg) vs 2% (10 mg)	Monitor weight regularly; more pronounced at 23 mg
Weight loss	5% (23 mg) vs 3% (10 mg)	8.4% of patients on 23 mg lost ≥7% body weight vs 4.9% on 10 mg; clinically important in frail elderly
Dizziness	5% (23 mg) vs 3% (10 mg)	Assess for orthostatic component and fall risk
Headache	4% (23 mg) vs 3% (10 mg)	Usually transient; exclude other causes in elderly
Ecchymosis	4–5%	Reported in pivotal trials; may reflect increased fall risk in elderly population
Urinary incontinence	3% (23 mg) vs 1% (10 mg)	Cholinomimetic effect on bladder smooth muscle; may worsen pre-existing incontinence

Serious Serious (Regardless of Frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Bradycardia / heart block	Uncommon (~1–2%)	Days to weeks; any time	ECG if symptomatic; hold donepezil if HR <50 bpm or symptomatic bradycardia; avoid combining with other rate-slowing agents
Syncope	~1–2%	Variable; may coincide with bradycardia	Cardiac evaluation; fall risk assessment; consider alternative cholinesterase inhibitor
GI bleeding / peptic ulcer	Rare	Any time; higher risk with NSAID co-use	Monitor for melena/haematemesis; co-prescribe PPI if NSAID required; discontinue if active bleeding
Seizures	Rare	Any time	May be indistinguishable from Alzheimer-related seizures; neurology review; consider discontinuation
QTc prolongation	Rare (post-marketing)	Variable	Avoid co-administration with other QT-prolonging drugs; ECG monitoring if risk factors present
Rhabdomyolysis	Very rare (post-marketing)	Variable	Check CK if myalgia with dark urine; discontinue donepezil and hydrate aggressively
Neuroleptic malignant syndrome	Very rare (post-marketing)	Variable	Immediate discontinuation; ICU care; supportive measures

Discontinuation Discontinuation Rates

Mild–Moderate AD (5 mg & 10 mg)

5% (5 mg) / 13% (10 mg) vs ~5% placebo

Top reasons: Nausea (2%), diarrhea (2%), anorexia (2%)

Moderate–Severe AD (23 mg vs 10 mg)

19% vs 8% (10 mg)

Top reasons: Vomiting, nausea, diarrhea, anorexia; most discontinuations in first month

Reason for Discontinuation (Severe AD)	Incidence	Context
Anorexia	2% vs 1% placebo	Overlaps with weight loss concern
Nausea	2% vs <1% placebo	Cholinomimetic; dose-related
Diarrhea	2% vs 0% placebo	Usually resolves with continued treatment
Urinary tract infection	2% vs 1% placebo	May reflect incontinence and related hygiene issues

Managing GI Side Effects — The Most Common Treatment-Limiting Problem

Nausea, vomiting, and diarrhea are the most frequent reasons patients stop donepezil. These effects are cholinomimetic, dose-dependent, and strongly influenced by titration speed. Strategies to improve tolerability include extending the titration from 5 mg to 10 mg over 6 weeks rather than 1 week, switching from bedtime to morning dosing if nightmares or insomnia occur, and ensuring the patient takes the medication with food despite it not being required pharmacokinetically. If GI symptoms are intolerable, switching to a transdermal formulation or an alternative cholinesterase inhibitor (rivastigmine patch, galantamine ER) may be considered.

Int

Drug Interactions

Donepezil is metabolised by CYP3A4 and CYP2D6, but its affinity for these enzymes is low. In clinical studies, CYP3A4 inhibitors produced only modest increases in donepezil exposure (~36% with ketoconazole), and CYP2D6 inhibitors had even smaller effects (~17% clearance reduction). The more clinically important interactions are pharmacodynamic, involving cholinergic and cardiac pathways.

MajorAnticholinergic Agents (oxybutynin, tolterodine, diphenhydramine, TCAs)

MechanismDirect pharmacological antagonism of donepezil at muscarinic receptors

EffectReduced donepezil efficacy; cognitive worsening; negates therapeutic benefit

ManagementAvoid concurrent anticholinergics; use mirabegron for overactive bladder; use non-anticholinergic alternatives

FDA PI

MajorSuccinylcholine & Neuromuscular Blocking Agents

MechanismCholinesterase inhibition exaggerates succinylcholine-type muscle relaxation

EffectProlonged neuromuscular blockade during anaesthesia

ManagementInform anaesthesiologist; dose adjustment of relaxant may be needed

FDA PI

ModerateBeta-Blockers & Rate-Slowing Agents

MechanismAdditive vagotonic effects on sinoatrial and atrioventricular nodes

EffectIncreased risk of symptomatic bradycardia, syncope, heart block

ManagementMonitor heart rate at initiation; ECG if symptomatic; consider alternative antihypertensive

FDA PI

ModerateKetoconazole & Strong CYP3A4 Inhibitors

MechanismInhibition of CYP3A4-mediated donepezil metabolism

EffectKetoconazole increased donepezil AUC and Cmax by 36% in a formal PK study

ManagementMonitor for increased cholinergic side effects; dose reduction rarely needed due to wide therapeutic margin

FDA PI / PK Study

ModerateNSAIDs

MechanismCholinesterase inhibitors increase gastric acid secretion; NSAIDs impair mucosal protection

EffectIncreased risk of GI bleeding and peptic ulceration

ManagementUse with gastroprotection (PPI); monitor for signs of GI bleeding

Lexicomp

ModerateCYP3A4 Inducers (rifampicin, phenytoin, carbamazepine)

MechanismEnhanced CYP3A4-mediated metabolism of donepezil

EffectReduced donepezil plasma levels and potential loss of efficacy

ManagementMonitor cognitive function; dose adjustment or alternative cholinesterase inhibitor may be needed

FDA PI

MinorCholinergic Agonists (bethanechol, pilocarpine)

MechanismAdditive cholinergic stimulation

EffectPotentiation of cholinomimetic effects (salivation, lacrimation, bradycardia)

ManagementUse with caution; monitor for excessive cholinergic effects

FDA PI

MinorMemantine

MechanismNo pharmacokinetic interaction (different metabolic pathways)

EffectComplementary mechanisms; combination is standard of care in moderate–severe AD

ManagementSafe to combine; no dose adjustment needed for either agent

FDA PI (Namzaric)

Mon

Monitoring

Cognitive FunctionBaseline, 3–6 months, then annually
RoutineUse validated tools (MMSE, MoCA, ADAS-Cog) to assess treatment response. If no measurable benefit after 3–6 months of optimised dosing, reassess whether continuation is appropriate. Expect stabilisation rather than improvement in most patients.
Heart RateBaseline, after dose changes
RoutineDonepezil has vagotonic properties that can cause bradycardia or heart block, even in patients without known cardiac disease. Check pulse at each visit. ECG if symptomatic bradycardia, syncope, or concomitant use of beta-blockers or calcium channel blockers.
Body WeightEvery 3 months
RoutineWeight loss occurs in up to 8.4% of patients on 23 mg. Clinically significant in already frail elderly patients. Track weight trends and assess nutritional intake. Reduce dose if unexplained weight loss >5% occurs.
GI SymptomsFirst 4–6 weeks, then as needed
RoutineAssess nausea, vomiting, diarrhea, and appetite at each visit during titration. Most GI effects are transient and resolve within 1–3 weeks. If persistent, consider slower titration, morning dosing, or switch to alternative.
Behavioural SymptomsEach visit
RoutineAssess for agitation, aggression, hallucinations, and sleep disturbances. Donepezil can occasionally worsen behavioural symptoms in some patients. In DLB patients specifically, monitor for worsening parkinsonism.
GI BleedingIf NSAID co-use or GI history
Trigger-basedCholinesterase inhibitors increase gastric acid secretion. Monitor for occult or overt GI bleeding in patients with peptic ulcer history or concurrent NSAID/antiplatelet use. Consider PPI co-prescription.
Respiratory StatusIf asthma or COPD history
Trigger-basedCholinomimetic action may increase bronchial secretions and airway reactivity. Use with caution and monitor respiratory symptoms in patients with obstructive lung disease.

Contraindications & Cautions

Absolute Contraindications

Known hypersensitivity to donepezil hydrochloride or piperidine derivatives (FDA PI).
History of allergic contact dermatitis with donepezil transdermal system (Adlarity PI).

Relative Contraindications (Specialist Input Recommended)

Sick sinus syndrome or other supraventricular conduction abnormalities — vagotonic effects may precipitate symptomatic bradycardia or heart block.
Active peptic ulcer disease or upper GI bleeding — cholinesterase inhibitors increase gastric acid secretion.
Pregnancy — animal data suggest potential fetal harm; no adequate human studies.

Use with Caution

Asthma or COPD — cholinomimetic activity may exacerbate bronchoconstriction.
Seizure history — cholinomimetics may lower the seizure threshold; however, seizure activity may also reflect Alzheimer disease itself.
Bladder outflow obstruction — cholinomimetic effects may worsen urinary retention.
Low body weight (<50 kg) — higher plasma concentrations may increase the risk of adverse effects; consider maintaining at 5 mg.
Hepatic impairment — clearance reduced by approximately 20% in stable cirrhosis; formal dose adjustment not required but monitor more closely.
Concurrent use of anticholinergic medications — negates the therapeutic benefit of donepezil.

FDA Safety Warning Nausea, Vomiting, and Weight Loss

Donepezil can cause clinically significant nausea and vomiting, particularly at the 23 mg dose level. These effects may be severe enough to result in dehydration in elderly patients. Weight loss of ≥7% of baseline body weight occurred in 8.4% of patients on 23 mg/day in the pivotal trial. The FDA PI advises that patients should be closely monitored for these effects, especially during dose escalation (FDA PI).

FDA Safety Warning Cardiovascular Effects

As a cholinesterase inhibitor, donepezil has vagotonic effects on the sinoatrial and atrioventricular nodes that may manifest as bradycardia or heart block in patients with and without known underlying cardiac conduction abnormalities. Syncopal episodes have been reported. Particular caution is warranted in patients with sick sinus syndrome or those receiving concurrent beta-blockers (FDA PI).

Patient Counselling

Purpose of Therapy

Donepezil is prescribed to help improve memory, thinking, and the ability to perform daily activities in people with Alzheimer disease. It works by boosting the levels of a natural chemical messenger (acetylcholine) in the brain that is reduced in Alzheimer disease. It is important for patients and caregivers to understand that donepezil does not cure or stop the progression of Alzheimer disease, but it may slow the worsening of symptoms for a period of time.

How to Take

Donepezil is taken once daily. The standard tablets (5 mg, 10 mg) can be taken with or without food, at any time of day, though bedtime dosing is the traditional recommendation. The 23 mg tablet must be swallowed whole and should never be split, crushed, or chewed. The orally disintegrating tablet (ODT) should be placed on the tongue, allowed to dissolve, and followed with water. If a dose is missed, take it as soon as remembered; if multiple days are missed (more than 7 days), contact the prescriber before restarting.

Nausea, Vomiting & Diarrhea

Tell patientStomach upset is the most common side effect, especially during the first few weeks or after a dose increase. It usually improves on its own. Taking the medication with food or asking the doctor about a slower dose increase can help. Stay well hydrated.

Call prescriberIf nausea or vomiting is severe, if you cannot keep food or fluids down, or if you notice dark/bloody stools (which may indicate GI bleeding).

Sleep Disturbance & Nightmares

Tell patientSome patients experience insomnia, vivid dreams, or nightmares when taking donepezil at bedtime. Switching to a morning dose often resolves this. Discuss timing with your doctor.

Call prescriberIf sleep problems persist despite switching to morning dosing, or if nightmares are distressing.

Dizziness & Fainting

Tell patientDonepezil can slow the heart rate, which may cause dizziness or fainting, especially when standing up. Rise slowly from sitting or lying positions. Ensure the home environment is fall-proofed.

Call prescriberIf you experience a fainting episode, feel your heart beating unusually slowly, or have repeated dizziness.

Weight & Appetite

Tell patientLoss of appetite and weight loss can occur, particularly at the 23 mg dose. Weigh yourself weekly and eat small, frequent meals if appetite is reduced. Nutritional supplements may help maintain weight.

Call prescriberIf unintended weight loss exceeds 5 pounds in a month, or if you cannot eat enough to maintain your weight.

Surgery & Dental Procedures

Tell patientAlways inform your surgeon, anaesthesiologist, or dentist that you are taking donepezil before any procedure that requires anaesthesia. Donepezil can interact with certain muscle relaxants used during surgery.

Call prescriberBefore any scheduled procedure so the team can plan accordingly.

Caregiver Involvement

Tell patientBecause Alzheimer disease affects memory and judgment, it is important that a caregiver or family member helps with medication administration, monitors for side effects, and attends follow-up appointments.

Call prescriberIf the caregiver notices worsening confusion, new behavioural changes, or inability to tolerate the medication.

Ref

Sources

Regulatory (PI / SmPC)

ARICEPT (donepezil hydrochloride) tablets / ODT — Full Prescribing Information. Eisai Inc. / FDA. FDA Label (2018) Primary source for approved indications, dosing (5, 10, 23 mg), pharmacokinetics, adverse reactions tables, drug interactions, and contraindications.
ARICEPT 23 mg — Full Prescribing Information. Eisai Inc. / FDA. FDA Label (2010) Source for 23 mg-specific adverse reactions, 23 mg vs 10 mg comparative trial data, and weight loss findings.
Namzaric (memantine HCl extended-release / donepezil HCl) — Full Prescribing Information. Allergan / FDA. FDA Label (2017) Source for combination therapy pharmacokinetics; confirms no interaction between memantine and donepezil.

Key Clinical Trials

Rogers SL, Friedhoff LT. The efficacy and safety of donepezil in patients with Alzheimer’s disease: results of a US multicentre, randomized, double-blind, placebo-controlled trial. Dementia. 1996;7(6):293–303. doi:10.1159/000106895 Original pivotal 30-week RCT establishing donepezil 5 mg and 10 mg efficacy in mild to moderate Alzheimer disease.
Birks JS, Harvey RJ. Donepezil for dementia due to Alzheimer’s disease. Cochrane Database Syst Rev. 2018;(6):CD001190. doi:10.1002/14651858.CD001190.pub3 Comprehensive Cochrane review confirming modest but consistent cognitive and global function benefits across all AD severity stages.
Mori E, Ikeda M, Kosaka K; Donepezil-DLB Study Investigators. Donepezil for dementia with Lewy bodies: a randomized, placebo-controlled trial. Ann Neurol. 2012;72(1):41–52. doi:10.1002/ana.23557 Phase 2 RCT (n=140) in DLB demonstrating cognitive, behavioural, and global improvements at 5 and 10 mg.
Ikeda M, Mori E, Matsuo K, et al. Donepezil for dementia with Lewy bodies: a randomized, placebo-controlled, confirmatory phase III trial. Alzheimers Res Ther. 2015;7(1):4. doi:10.1186/s13195-014-0083-0 Phase 3 confirmatory trial in DLB (n=142); basis for Japan DLB approval.

Guidelines

Livingston G, Huntley J, Sommerlad A, et al. Dementia prevention, intervention, and care: 2020 report of the Lancet Commission. Lancet. 2020;396(10248):413–446. doi:10.1016/S0140-6736(20)30367-6 Lancet Commission providing evidence-based framework for dementia treatment including cholinesterase inhibitor recommendations.
Cummings J, Aisen P, Apostolova LG, et al. Aducanumab: appropriate use recommendations. J Prev Alzheimers Dis. 2021;8(4):398–410. doi:10.14283/jpad.2021.41 Provides contemporary context for cholinesterase inhibitor positioning alongside newer disease-modifying therapies.

Mechanistic / Basic Science

Prvulovic D, Schneider B. Pharmacokinetic and pharmacodynamic evaluation of donepezil for the treatment of Alzheimer’s disease. Expert Opin Drug Metab Toxicol. 2014;10(7):1039–1050. doi:10.1517/17425255.2014.915028 Detailed review of donepezil PK/PD including CYP enzyme interactions, AChE selectivity, and clinical exposure-response relationships.
StatPearls: Donepezil. Chang C, et al. NCBI Bookshelf. Updated August 2023. NCBI Bookshelf Comprehensive clinical pharmacology overview covering mechanism, off-label uses, adverse effects, and monitoring.

Pharmacokinetics / Special Populations

Tiseo PJ, Foley K, Friedhoff LT. Steady-state pharmacokinetics and safety of donepezil HCl in subjects with moderately impaired renal function. Br J Clin Pharmacol. 1998;46(Suppl 1):56–60. doi:10.1046/j.1365-2125.1998.0460s1056.x Demonstrates unchanged donepezil clearance in moderate renal impairment, supporting no dose adjustment.
Tiseo PJ, Perdomo CA, Friedhoff LT. Pharmacokinetic and pharmacodynamic profile of donepezil HCl following evening administration. Br J Clin Pharmacol. 1998;46(Suppl 1):13–18. doi:10.1046/j.1365-2125.1998.0460s1013.x Key PK study characterising linear pharmacokinetics with evening dosing, protein binding (96%), half-life (~70 h), and AChE inhibition profile.
Jackson S, Ham RJ, Wilkinson D. The safety and tolerability of donepezil in patients with Alzheimer’s disease. Br J Clin Pharmacol. 2004;58(Suppl 1):1–8. doi:10.1111/j.1365-2125.2004.01848.x Comprehensive safety review covering GI, cardiovascular, and CNS tolerability across clinical trials.