Memantine: Complete Drug Monograph & Prescribing Guide

Pharmacokinetic Profile

Half-Life

60–80 h

Metabolism

Partial hepatic (not CYP450); renal elimination predominates

Protein Binding

45%

Bioavailability

~100%

Volume of Distribution

9–11 L/kg

Clinical Information

Drug Class

NMDA receptor antagonist (uncompetitive, low-to-moderate affinity)

Available Doses

IR tabs: 5, 10 mg; XR caps: 7, 14, 21, 28 mg; Soln: 2 mg/mL

Route

Oral

Renal Adjustment

Severe (CrCl 5–29): IR max 5 mg BID; XR max 14 mg/day

Hepatic Adjustment

Mild–moderate: no adjustment; Severe: use with caution

Pregnancy

Animal data: developmental toxicity at high doses; no human studies

Lactation

Unknown if excreted in human milk

Schedule

Rx only (not scheduled)

Generic Available

Yes

Memantine Indications

Indication	Approved Population	Therapy Type	Status
Moderate-to-severe dementia of the Alzheimer’s type	Adults	Monotherapy or adjunctive with AChE inhibitor	FDA Approved

Memantine is the only FDA-approved drug for Alzheimer’s disease that works outside the cholinergic system. Unlike acetylcholinesterase inhibitors (donepezil, rivastigmine, galantamine), which target mild-to-moderate disease, memantine is indicated for the moderate-to-severe stage. It is frequently prescribed in combination with a cholinesterase inhibitor, most commonly donepezil, and the fixed-dose combination product Namzaric (memantine XR + donepezil) is available for this purpose. In pivotal trials, memantine demonstrated significant improvements on both cognitive (SIB) and functional (ADCS-ADL) measures relative to placebo.

Off-Label Uses

Vascular dementia: The Latvian Study 3 included patients with vascular dementia and showed functional benefit. Some international guidelines support use in vascular dementia. Evidence quality: Moderate.

Dementia with Lewy bodies (DLB): Limited RCT data; some clinical benefit reported in open-label studies. Evidence quality: Low.

Neuropathic pain, fibromyalgia, OCD (augmentation): Small studies with inconsistent results; not routinely recommended. Evidence quality: Low to Very Low.

Autism spectrum disorder (paediatric): Two controlled trials (n = 578) in children aged 6–12 years failed to demonstrate efficacy. Not recommended.

Dose

Memantine Dosing

Dosing by Clinical Scenario

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Moderate-to-severe AD — IR tablet initiation	5 mg once daily	10 mg BID (20 mg/day)	10 mg BID (20 mg/day)	Titrate in 5 mg increments: 5 mg QD → 5 mg BID → 5 mg AM + 10 mg PM → 10 mg BID; minimum 1 week between increases May be taken with or without food
Moderate-to-severe AD — XR capsule initiation	7 mg once daily	28 mg once daily	28 mg once daily	Titrate in 7 mg increments weekly: 7 → 14 → 21 → 28 mg/day XR capsules may be opened and sprinkled on applesauce
Add-on to stable AChE inhibitor (donepezil)	5 mg QD (IR) or 7 mg QD (XR)	20 mg/day (IR) or 28 mg/day (XR)	Same as monotherapy	No dose adjustment needed for either drug; memantine does not affect donepezil PK or vice versa Study 2 demonstrated benefit of adding memantine to donepezil (FDA PI)
Switching from IR to XR	IR 10 mg BID (20 mg/day) → XR 28 mg QD the following day		28 mg/day	Begin XR the day after the last IR dose
Treatment interruption — restart	5 mg QD (IR) or 7 mg QD (XR)	Re-titrate to target	Same as original target	If missed several days, resume at lower doses and re-titrate

Special Population Adjustments

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Severe renal impairment (CrCl 5–29 mL/min)	5 mg QD (IR)	5 mg BID (10 mg/day) or 14 mg/day (XR)	10 mg/day (IR) or 14 mg/day (XR)	AUC increased ~115%, t½ nearly doubled; reduce target dose by 50%
Mild–moderate renal impairment	No adjustment needed			AUC increased only 4–60%; standard doses appropriate
Mild–moderate hepatic impairment	No adjustment needed			No change in exposure (moderate impairment); t½ increased ~16%
Severe hepatic impairment	Use with caution; not studied			Minimal hepatic metabolism, but no safety data in this population

Clinical Pearl: Tolerability Advantage

Memantine has a remarkably favourable tolerability profile compared with cholinesterase inhibitors. In pooled controlled trials, the discontinuation rate due to adverse events was the same in the memantine group (10.1%) as in the placebo group (11.5%), and no individual adverse reaction led to discontinuation in 1% or more of memantine-treated patients at a rate exceeding placebo. This makes memantine one of the best-tolerated CNS drugs in elderly patients and is a key advantage over the GI-intolerance-prone cholinesterase inhibitors.

Pharmacology

Mechanism of Action

In Alzheimer’s disease, chronic pathological overactivation of NMDA-type glutamate receptors by tonically elevated glutamate levels contributes to excitotoxic neuronal damage and symptom progression. Memantine is a low-to-moderate affinity, uncompetitive (open-channel) NMDA receptor antagonist that binds preferentially to NMDA receptor-operated cation channels. Its voltage-dependent kinetics and rapid off-rate allow it to block pathological tonic activation of NMDA receptors while preserving normal phasic synaptic signalling necessary for learning and memory. This “gentle blockade” contrasts with high-affinity NMDA antagonists (e.g., ketamine, MK-801), which impair physiological neurotransmission. Memantine also exhibits antagonistic activity at the 5-HT3 receptor and weak blockade of nicotinic acetylcholine receptors, though the clinical relevance of these secondary actions at therapeutic doses is uncertain. There is no evidence that memantine prevents or slows the underlying neurodegeneration.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Complete absorption; bioavailability ~100%; Tmax 3–7 h (IR), 9–12 h (XR); food has no effect on absorption; linear PK over therapeutic range	Can be taken with or without food; reliable oral delivery regardless of feeding status
Distribution	Vd 9–11 L/kg; plasma protein binding 45%; crosses BBB readily (CSF/serum ratio ~0.52); widely distributed to tissues	Large Vd indicates extensive tissue penetration; low-moderate protein binding makes displacement interactions unlikely
Metabolism	Partial hepatic metabolism (not via CYP450); ~48% excreted unchanged in urine; metabolites (N-glucuronide, 6-hydroxy memantine, 1-nitroso-deaminated memantine) have minimal NMDA antagonist activity	CYP450-independent metabolism confers an exceptionally low drug interaction potential; no dose adjustment needed for hepatic impairment (mild–moderate)
Elimination	t½ 60–80 h; predominantly renal; active tubular secretion moderated by pH-dependent tubular reabsorption; clearance reduced ~80% at urine pH 8; 74% of dose excreted as parent + N-glucuronide conjugate	Very long half-life supports once-daily XR dosing and provides stable plasma levels; alkaline urine markedly reduces clearance — critical interaction with urine-alkalinising conditions

Side Effects

Memantine is among the best-tolerated treatments for Alzheimer’s disease. Adverse reaction data below are from eight pooled, double-blind, placebo-controlled trials (FDA PI Table 1; n = 940 memantine vs n = 922 placebo; treatment up to 28 weeks). The overall discontinuation rate due to adverse events was identical to placebo (10.1% vs 11.5%).

≥5%Most Common (≥5% and higher than placebo)

Adverse Effect	Incidence	Clinical Note
Dizziness	7% (vs 5% placebo)	Most frequently reported; usually transient during titration
Headache	6% (vs 3% placebo)	Mild; does not typically require treatment discontinuation
Confusion	6% (vs 5% placebo)	Difficult to distinguish from disease progression; evaluate if new-onset
Constipation	5% (vs 3% placebo)	Encourage adequate fluid intake and dietary fibre; rule out anticholinergic burden

2–4%Common

Adverse Effect	Incidence	Clinical Note
Hypertension	4% (vs 2% placebo)	Monitor blood pressure at each visit; clinical significance modest
Coughing	4% (vs 3% placebo)	Non-specific; evaluate for respiratory infection in elderly population
Pain	3% (vs 1% placebo)	Unspecified body pain; assess for musculoskeletal or other causes
Back pain	3% (vs 2% placebo)	Common in elderly; unlikely drug-related but recorded as treatment-emergent
Vomiting	3% (vs 2% placebo)	Much lower incidence than cholinesterase inhibitors (20–47%)
Somnolence	3% (vs 2% placebo)	Advise caution with driving; may compound cognitive slowing
Hallucination	3% (vs 2% placebo)	May also reflect disease progression; evaluate triggers and onset
Fatigue	2% (vs 1% placebo)	Generally mild; assess functional impact
Dyspnea	2% (vs 1% placebo)	Evaluate for cardiac or pulmonary causes in elderly patients

SeriousSerious Adverse Effects (Regardless of Frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Stevens-Johnson syndrome	Very rare (post-marketing)	Variable	Discontinue immediately; emergency dermatological care; do not rechallenge
Agranulocytosis / pancytopenia / TTP	Very rare (post-marketing)	Variable	Urgent FBC; haematology referral; discontinue memantine
Congestive cardiac failure	Rare (post-marketing)	Variable	Cardiac evaluation; manage per standard heart failure guidelines
Hepatitis	Rare (post-marketing)	Variable	Check LFTs; discontinue if hepatitis confirmed
Acute renal failure	Rare (post-marketing)	Variable	Monitor renal function; hold memantine; evaluate for reversible causes
Suicidal ideation	Very rare (post-marketing)	Variable	Psychiatric assessment; ensure safe environment; consider discontinuation
Seizures	0.2% (vs 0.5% placebo)	Any time	Lower rate than placebo in trials; evaluate independently from memantine; seizures may reflect AD progression

DiscontinuationDiscontinuation Rates

Memantine (Pooled Controlled Trials)

10.1% vs 11.5% placebo

N = 940 memantine, 922 placebo. No individual adverse reaction caused discontinuation in ≥1% of memantine patients at a rate higher than placebo. This is a defining feature of memantine’s tolerability profile.

Comparison with AChE Inhibitors

Dramatically lower

AChE inhibitor DC rates: donepezil ~9%, rivastigmine ~15%, galantamine ~10.6% (all vs 2–5% placebo). Memantine DC rate = placebo.

Key Tolerability Advantage

Unlike cholinesterase inhibitors, memantine does not cause significant nausea, vomiting, or diarrhoea. It lacks the cholinergic GI effects that drive much of the treatment discontinuation seen with donepezil, rivastigmine, and galantamine. This makes it particularly suitable for frail elderly patients or those who have failed cholinesterase inhibitor therapy due to GI intolerance.

Int

Drug Interactions

Memantine has an exceptionally clean drug interaction profile. It does not inhibit or induce any CYP450 isoenzyme and does not affect the pharmacokinetics of warfarin, bupropion, donepezil, or metformin. Its primary interaction risk is pharmacokinetic: because ~48% is excreted unchanged by renal tubular secretion, drugs or conditions that alkalinise urine can dramatically reduce memantine clearance (up to 80% reduction at pH 8).

MajorUrine-alkalinising agents (carbonic anhydrase inhibitors, sodium bicarbonate)

MechanismAlkaline urine pH enhances tubular reabsorption, reducing renal clearance by ~80% at pH 8

EffectMarkedly increased memantine plasma levels and risk of adverse effects

ManagementUse with caution; monitor for CNS effects (confusion, dizziness); also be aware of dietary changes (vegetarian diets) and clinical states (UTIs, renal tubular acidosis) that alkalinise urine

FDA PI

ModerateOther NMDA antagonists (amantadine, ketamine, dextromethorphan)

MechanismAdditive pharmacodynamic NMDA receptor blockade

EffectPotential for increased CNS adverse effects (confusion, hallucinations, psychosis)

ManagementCombination not systematically evaluated; use with caution; monitor closely for CNS toxicity

FDA PI

ModerateDrugs using renal cationic transport (cimetidine, ranitidine, quinidine, nicotine, HCTZ, metformin)

MechanismCompetition for renal tubular cationic secretion system

EffectTheoretical potential for altered plasma levels of both agents; clinical studies with HCTZ/triamterene and metformin showed no significant effect on memantine

ManagementGenerally safe based on available data; monitor if adding multiple cationic drugs

FDA PI (PK studies)

MinorDonepezil (and other AChE inhibitors)

MechanismNo pharmacokinetic interaction; memantine does not affect AChE inhibition by donepezil in vitro

EffectNo change in PK of either drug; similar adverse event profile when combined

ManagementNo dose adjustment needed; safe and common combination for moderate-to-severe AD

FDA PI (Clinical study + in vitro)

MinorWarfarin

MechanismNo PK or PD interaction; memantine does not affect warfarin levels or INR

EffectNo clinically significant interaction

ManagementNo dose adjustment; routine INR monitoring as standard of care

FDA PI (PK study)

MinorBupropion

MechanismNo effect on CYP2B6-mediated bupropion metabolism

EffectNo change in bupropion or hydroxybupropion PK

ManagementNo dose adjustment needed

FDA PI (PK study)

Mon

Monitoring

Cognitive functionBaseline, then every 3–6 months
RoutineUse SIB (for moderate-severe) or MMSE/MoCA. Memantine targets functional stabilisation rather than cognitive improvement; reassess if progressive decline despite treatment.
Renal functionBaseline, then annually or if clinical change
RoutineTarget dose must be halved in severe renal impairment (CrCl 5–29 mL/min). Long half-life (60–80 h) means accumulation occurs slowly; reassess dose if renal function declines.
Urine pHAs clinically indicated
Trigger-basedClearance drops ~80% at pH 8. Assess in patients with recurrent UTIs, renal tubular acidosis, drastic dietary changes, or concurrent use of carbonic anhydrase inhibitors or sodium bicarbonate.
Blood pressureEach visit
RoutineHypertension was reported in 4% vs 2% placebo. Monitor at each visit, especially in patients with pre-existing cardiovascular disease.
Neuropsychiatric symptomsEach visit
RoutineHallucinations (3%), confusion (6%), and somnolence (3%) may occur. Differentiate drug-related effects from disease progression. Post-marketing reports of suicidal ideation warrant vigilance.
Bowel functionEach visit during titration
RoutineConstipation (5%) is more common than with placebo. Ensure adequate hydration and fibre; especially relevant in patients already taking anticholinergic medications.

Contraindications & Cautions

Absolute Contraindications

Known hypersensitivity to memantine hydrochloride or any excipient in the formulation

Relative Contraindications (Specialist Input Recommended)

Severe renal impairment (CrCl 5–29 mL/min): Dose must be halved; monitor closely for accumulation
Conditions that alkalinise urine: Renal tubular acidosis, severe UTIs, chronic use of carbonic anhydrase inhibitors or sodium bicarbonate; clearance may drop by up to 80%
Severe hepatic impairment: Not studied; use with caution

Use with Caution

History of seizures: Seizure incidence in trials was lower on memantine (0.2%) than placebo (0.5%), but theoretical risk remains; monitor
Cardiovascular disease: Hypertension reported at higher rate; post-marketing cases of congestive cardiac failure
Concurrent use of other NMDA antagonists: Amantadine, ketamine, dextromethorphan; additive CNS effects possible
Genitourinary conditions: Conditions affecting urine pH or renal tubular function may alter memantine clearance

FDA Safety Communication Urine pH-Dependent Clearance

The clearance of memantine is reduced by approximately 80% under alkaline urine conditions (pH 8). Drugs such as carbonic anhydrase inhibitors and sodium bicarbonate, clinical states such as renal tubular acidosis and severe urinary tract infections, and drastic dietary changes (e.g., shift to a vegetarian diet) can alkalinise urine and lead to memantine accumulation with increased risk of adverse effects. Clinicians should be aware of this pharmacokinetic vulnerability when prescribing memantine to patients with any of these risk factors.

Patient Counselling

Purpose of Therapy

Memantine is prescribed to help manage the symptoms of moderate-to-severe Alzheimer’s disease. It works differently from other Alzheimer’s medicines (such as donepezil) by blocking a chemical in the brain called glutamate that, when overactive, can damage nerve cells. Memantine does not cure Alzheimer’s disease or stop it from getting worse, but it may help maintain daily functioning and slow the worsening of symptoms. It can be taken alongside other Alzheimer’s medicines.

How to Take

IR tablets: Take twice daily with or without food. XR capsules: Take once daily. Swallow whole, or open and sprinkle on applesauce then swallow immediately without chewing. Oral solution: Measure dose using the provided dosing device.

Dose Titration

Tell patientYour doctor will gradually increase the dose over several weeks to reduce the chance of side effects. Do not increase the dose faster than instructed.

Call prescriberIf side effects such as dizziness, confusion, or headache worsen during dose increases.

Dizziness & Confusion

Tell patientDizziness and confusion may occur, especially early in treatment. Avoid driving or operating machinery until you know how memantine affects you. Rise slowly from sitting or lying positions.

Call prescriberIf dizziness is severe, if confusion worsens noticeably, or if hallucinations develop.

Constipation

Tell patientDrink plenty of fluids and eat high-fibre foods to help prevent constipation. Gentle exercise may also help.

Call prescriberIf constipation persists for more than a few days or is accompanied by abdominal pain.

Missed Doses

Tell patientIf you miss a single dose, do not take a double dose. Take the next dose as scheduled. If you miss several days, contact your doctor before resuming — you may need to restart at a lower dose.

Call prescriberWhenever treatment has been interrupted for several days or more.

Medications & Supplements

Tell patientInform your doctor about all medicines you take, especially sodium bicarbonate (baking soda), medicines for glaucoma, cough medicines containing dextromethorphan, or medicines used for Parkinson’s disease (amantadine). These may interact with memantine.

Call prescriberBefore starting any new prescription or over-the-counter medication.

Ref

Sources

Regulatory (PI / SmPC)

Namenda (memantine hydrochloride) tablets — FDA-approved Prescribing Information. Allergan (AbbVie). Revised November 2018. accessdata.fda.govPrimary source for IR tablet dosing, adverse reactions (Table 1, pooled n=1,862), pharmacokinetics, drug interactions, and clinical trial data (Studies 1–3).
Namenda XR (memantine hydrochloride) extended-release capsules — FDA-approved Prescribing Information. Revised 2014. accessdata.fda.govSource for XR capsule dosing, PK of extended-release formulation, renal dose adjustment (14 mg/day target for severe impairment), and paediatric ASD study data.

Key Clinical Trials

Reisberg B, Doody R, Stöffler A, Schmitt F, Ferris S, Möbius HJ; Memantine Study Group. Memantine in moderate-to-severe Alzheimer’s disease. N Engl J Med. 2003;348(14):1333–1341. doi:10.1056/NEJMoa013128Landmark 28-week RCT (Study 1, n=252) demonstrating significant benefit on SIB (+5.7 points) and ADCS-ADL (+3.4 points) in moderate-to-severe AD.
Tariot PN, Farlow MR, Grossberg GT, Graham SM, McDonald S, Gergel I; Memantine Study Group. Memantine treatment in patients with moderate to severe Alzheimer disease already receiving donepezil: a randomized controlled trial. JAMA. 2004;291(3):317–324. doi:10.1001/jama.291.3.317Pivotal 24-week add-on trial (Study 2, n=404) showing benefit of adding memantine to stable donepezil; SIB +3.3, ADCS-ADL +1.6 points vs placebo/donepezil.
Winblad B, Poritis N. Memantine in severe dementia: results of the 9M-Best Study (benefit and efficacy in severely demented patients during treatment with memantine). Int J Geriatr Psychiatry. 1999;14(2):135–146. doi:10.1002/(SICI)1099-1166(199902)14:2<135::AID-GPS906>3.0.CO;2-012-week Latvian study (Study 3, n=166) in severe dementia showing significant benefit on BGP care dependency and CGI-C.
Peskind ER, Potkin SG, Pomara N, et al. Memantine treatment in mild to moderate Alzheimer disease: a 24-week randomized, controlled trial. Am J Geriatr Psychiatry. 2006;14(8):704–715. doi:10.1097/01.JGP.0000224350.82719.8324-week RCT examining memantine in mild-to-moderate AD; showed significant benefit on ADAS-cog but not CIBIC-plus.
van Dyck CH, Schmitt FA, Olin JT. A responder analysis of memantine treatment in patients with Alzheimer disease maintained on donepezil. Am J Geriatr Psychiatry. 2006;14(5):428–437. doi:10.1097/01.JGP.0000203151.17311.38Responder analysis of the Tariot 2004 trial; characterises clinical response patterns in combination therapy.

Guidelines

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/ng97UK guideline recommending memantine for moderate-to-severe AD, including in combination with an AChE inhibitor.

Mechanistic / Basic Science

Lipton SA. Paradigm shift in neuroprotection by NMDA receptor blockade: memantine and beyond. Nat Rev Drug Discov. 2006;5(2):160–170. doi:10.1038/nrd1958Seminal review of memantine’s uncompetitive, open-channel NMDA antagonism and the concept of preserving physiological signalling while blocking excitotoxicity.
Parsons CG, Stöffler A, Danysz W. Memantine: a NMDA receptor antagonist that improves memory by restoration of homeostasis in the glutamatergic system — too little activation is bad, too much is even worse. Neuropharmacology. 2007;53(6):699–723. doi:10.1016/j.neuropharm.2007.07.013Comprehensive review of memantine pharmacology covering receptor kinetics, selectivity, and dose-response relationships.

Pharmacokinetics / Special Populations

Noetzli M, Eap CB. Pharmacodynamic, pharmacokinetic and pharmacogenetic aspects of drugs used in the treatment of Alzheimer’s disease. Clin Pharmacokinet. 2013;52(4):225–241. doi:10.1007/s40262-013-0038-9PK review covering memantine absorption, distribution, renal elimination, pH-dependent clearance, and renal impairment dose adjustments.

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