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Drug Monograph

Lamotrigine (Lamictal)

lamotrigine

Phenyltriazine Antiepileptic / Mood Stabiliser · Oral
Pharmacokinetic Profile
Half-Life
25–33 h (monotherapy)
Metabolism
Hepatic glucuronidation (UGT1A4)
Protein Binding
~55%
Bioavailability
~98%
Volume of Distribution
0.9–1.3 L/kg
Clinical Information
Drug Class
Phenyltriazine anticonvulsant / mood stabiliser
Available Doses
Tabs: 25, 100, 150, 200 mg; Chewable: 2, 5, 25 mg; ODT: 25, 50, 100, 200 mg; XR: 25–300 mg
Route
Oral only
Renal Adjustment
Reduced maintenance may be needed
Hepatic Adjustment
Required (moderate/severe)
Pregnancy
Monitor levels; registry data available
Lactation
Excreted in breast milk
Black Box Warning
SJS/TEN — serious rash risk
Generic Available
Yes
Rx

Indications

IndicationApproved PopulationTherapy TypeStatus
Partial-onset seizures≥2 yearsAdjunctiveFDA Approved
Primary generalized tonic-clonic seizures≥2 yearsAdjunctiveFDA Approved
Generalized seizures of Lennox-Gastaut syndrome≥2 yearsAdjunctiveFDA Approved
Partial-onset seizures — conversion to monotherapy≥16 yearsMonotherapy (conversion from CBZ, PHT, PB, primidone, or VPA)FDA Approved
Bipolar I disorder — maintenanceAdultsMonotherapy or adjunctive (delays mood episodes)FDA Approved

Lamotrigine is a broad-spectrum antiepileptic drug and mood stabiliser with dual indications in epilepsy and bipolar I disorder. In epilepsy it is effective across focal and generalised seizure types and is one of the few AEDs with robust evidence for Lennox-Gastaut syndrome. In bipolar disorder, lamotrigine is used exclusively for maintenance treatment to delay mood episodes — it has no established efficacy for acute mania, mixed episodes, or acute depression at standard doses.

Off-Label Uses

Unipolar depression (treatment-resistant) — Used as augmentation to antidepressants in refractory major depressive disorder. Evidence quality: Low–Moderate (small RCTs with mixed results; no FDA approval).

Neuropathic pain / trigeminal neuralgia — Small controlled trials suggest benefit in trigeminal neuralgia and central post-stroke pain. Evidence quality: Low (insufficient evidence per Cochrane 2013 review; not recommended in most neuropathic pain guidelines).

Dose

Dosing

Critical: Dosing Depends on Concomitant Medications

Lamotrigine dosing varies dramatically based on whether the patient is taking valproate (which doubles lamotrigine levels), enzyme-inducing AEDs (carbamazepine, phenytoin, phenobarbital, primidone — which halve lamotrigine levels), or neither. Using the wrong titration schedule is the most common cause of serious rash. Always verify concomitant medication status before prescribing.

Epilepsy — Adjunctive Therapy (Adults and Adolescents >12 Years)

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
Adjunctive with valproate (VPA)25 mg every other day × 2 wk, then 25 mg daily × 2 wk100–200 mg/day200 mg/dayIncrease by 25–50 mg/day q1–2 wk from week 5
VPA inhibits glucuronidation; doubles LTG levels
Adjunctive without VPA or enzyme inducers25 mg daily × 2 wk, then 50 mg daily × 2 wk225–375 mg/day375 mg/dayIncrease by 50 mg/day q1–2 wk from week 5
Give in 2 divided doses
Adjunctive with enzyme inducers (CBZ, PHT, PB, primidone) without VPA50 mg daily × 2 wk, then 100 mg/day × 2 wk300–500 mg/day500 mg/dayIncrease by 100 mg/day q1–2 wk from week 5
Give in 2 divided doses; enzyme inducers reduce LTG ~40%
Conversion to monotherapy (from inducer)Achieve 500 mg/day per adjunctive schedule, then taper concomitant AED by 20%/wk over 4 weeks500 mg/dayTarget monotherapy dose is 500 mg/day in 2 divided doses
FDA PI Table 4 provides VPA conversion steps separately

Bipolar I Disorder — Maintenance (Adults)

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
Bipolar maintenance with valproate25 mg QOD × 2 wk → 25 mg daily × 2 wk → 50 mg × 1 wk100 mg/day100 mg/dayVery slow titration essential
Target reached at week 6
Bipolar maintenance without VPA or inducers25 mg daily × 2 wk → 50 mg daily × 2 wk → 100 mg × 1 wk200 mg/day200 mg/dayNo additional benefit demonstrated above 200 mg/day
Target reached at week 6
Bipolar maintenance with enzyme inducers, no VPA50 mg daily × 2 wk → 100 mg daily × 2 wk → 200 mg × 1 wkup to 400 mg/day400 mg/dayGive in divided doses
Target reached at week 7

Hepatic Impairment Dosing

Hepatic FunctionStarting DoseMaintenance DoseMaximum DoseNotes
Mild (Child-Pugh A)No adjustment neededStandard dosing per indication
Moderate or severe without ascitesReduce initial, escalation, and maintenance doses by ~25%Adjust based on clinical response
Severe with ascitesReduce initial, escalation, and maintenance doses by ~50%Adjust based on clinical response
Clinical Pearl: Restarting After Discontinuation

If lamotrigine has been stopped for more than 5 half-lives (which varies by concomitant medications — approximately 3 days with enzyme inducers, 5–7 days as monotherapy, or 10–12 days with valproate), restart from the initial titration schedule. This is critical because rapid re-titration after a gap increases the risk of serious rash.

PK

Pharmacology

Mechanism of Action

Lamotrigine stabilises neuronal membranes by blocking voltage-sensitive sodium channels in a use- and voltage-dependent manner, thereby inhibiting the presynaptic release of excitatory neurotransmitters, principally glutamate. This selective reduction in pathological high-frequency firing — while preserving normal neuronal activity — underlies both its antiepileptic and mood-stabilising properties. Lamotrigine also has weak inhibitory effects on 5-HT3 receptors and high-voltage-activated calcium channels (N- and P/Q-type), though the clinical significance of these secondary actions is not fully established. Unlike many conventional AEDs, lamotrigine does not meaningfully interact with GABA receptors or alter GABA levels in the brain.

ADME Profile

ParameterValueClinical Implication
AbsorptionBioavailability ~98%; Tmax ~2.5 h (range 1.4–4.8 h); not affected by food; no first-pass metabolismRapid and nearly complete absorption; can be taken with or without food
DistributionVd 0.9–1.3 L/kg; protein binding ~55%; crosses placenta (cord:maternal ratio ~1.0); breast milk:serum ratio ~0.6Moderate tissue penetration; brain concentrations approximate total plasma levels; significant placental transfer
MetabolismPrimarily UGT1A4-mediated glucuronidation; major metabolite is inactive 2-N-glucuronide (76% of dose); minor 5-N-glucuronide (10%); no significant CYP450 involvementHalf-life dramatically altered by UGT inducers (CBZ, PHT, OCP) and inhibitors (VPA); dosing must account for concomitant medications
Eliminationt½: 25–33 h monotherapy; 14–15 h with enzyme inducers; 48–59 h with VPA; ~86% excreted in urine as metabolites; ~10% unchangedSteady state: ~5 days monotherapy, ~3 days with inducers, ~10 days with VPA; taper over ≥2 weeks to discontinue
SE

Side Effects

≥10% Very Common (Adjunctive Epilepsy Trials)
Adverse EffectIncidenceClinical Note
Dizziness38%Dose-related; more common with concomitant carbamazepine; often improves with dose adjustment
Headache29%Comparable to placebo in some trials; rarely requires discontinuation
Diplopia28%Dose-related; significantly higher with concomitant CBZ (pharmacodynamic interaction)
Ataxia22%Dose-related; assess fall risk in elderly; often improves at lower doses
Nausea19%Dose-related; take with food if troublesome
Blurred vision16%Dose-related; more frequent with CBZ co-administration
Somnolence14%Less sedating than many AEDs; some patients report an alerting effect
Rash (non-serious)~10%Most rashes are benign maculopapular; cannot reliably distinguish from serious rash — discontinue at first sign
1–10% Common
Adverse EffectIncidenceClinical Note
Vomiting9%Dose-related; frequently resolves with continued treatment
Insomnia6%Can reflect alerting effect; consider AM dosing if problematic
Tremor4%Usually mild postural tremor; differentiate from underlying condition
Depression4%Monitor in bipolar patients; suicidality screening at each visit
Anxiety4%May be indication-related rather than drug-related
Coordination abnormality4%Overlaps with ataxia; assess driving safety
Serious Serious (Regardless of Frequency)
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Stevens-Johnson syndrome / TEN0.08–0.3% adults; 0.3–0.8% pediatric2–8 weeks (nearly all cases)Discontinue immediately at first sign of rash unless clearly not drug-related; do not rechallenge
DRESS / Multiorgan hypersensitivityRare; fatalities reported (2/3,796 adults; 4/2,435 pediatric in trials)Weeks after initiationDiscontinue if no alternative etiology; presents with fever, rash, lymphadenopathy, organ involvement
Hemophagocytic lymphohistiocytosis (HLH)Very rare (postmarketing)8–24 daysEvaluate immediately for extreme systemic inflammation (high ferritin, cytopenias, hepatosplenomegaly); discontinue
Cardiac conduction abnormalitiesRisk in patients with structural heart disease (in vitro Na channel blockade)VariableWeigh benefit vs arrhythmia risk in patients with clinically significant cardiac disease
Blood dyscrasias (neutropenia, thrombocytopenia, pancytopenia)RareVariableMonitor for unexpected infection, bruising, or bleeding; obtain CBC
Aseptic meningitisRare (postmarketing)1 day to 6 weeksDiscontinue; symptoms include headache, fever, nuchal rigidity, photophobia; recurs rapidly on rechallenge
Suicidality (AED class effect)0.43% (vs 0.24% placebo)As early as 1 weekMonitor for emergence of depression, suicidal thoughts, mood changes
Discontinuation Discontinuation Rates
Adjunctive Therapy (Adults)
11%
Top reasons: Rash (3.0%), dizziness (2.8%), headache (2.5%)
Monotherapy (Adults)
10%
Top reasons: Rash (4.5%), headache (3.1%), asthenia (2.4%)
Managing Rash Risk

Rash is the single most important safety concern with lamotrigine. Risk is highest with rapid dose escalation, concomitant valproate (1% hospitalisation rate with VPA vs 0.16% without), and in pediatric patients (0.3–0.8%). All rashes should be treated as potentially serious until proven otherwise — there is no reliable way to distinguish benign from dangerous rashes at onset. Patients should be instructed to contact their prescriber immediately upon noticing any skin change.

Int

Drug Interactions

Lamotrigine is metabolised almost exclusively by UGT-mediated glucuronidation. It does not significantly induce or inhibit CYP450 enzymes. However, its clearance is profoundly affected by drugs that induce or inhibit UGT, making concomitant medication status the primary determinant of dosing. Lamotrigine also inhibits organic cation transporter 2 (OCT2), which may affect renal clearance of OCT2 substrates.

Major Valproate (VPA)
MechanismVPA inhibits UGT-mediated glucuronidation of lamotrigine
EffectLamotrigine levels increase >2-fold; half-life extends to 48–59 h; increased risk of serious rash
ManagementUse VPA-specific dosing schedule (25 mg QOD start); maximum 200 mg/day for epilepsy, 100 mg/day for bipolar
FDA PI
Major Carbamazepine / Phenytoin / Phenobarbital / Primidone
MechanismEnzyme induction of UGT glucuronidation
EffectLamotrigine clearance increases ~40%; half-life shortens to 14–15 h
ManagementUse enzyme-inducer dosing schedule (50 mg/day start); higher maintenance doses required (300–500 mg/day)
FDA PI
Major Estrogen-Containing Oral Contraceptives
MechanismEthinylestradiol induces UGT glucuronidation of lamotrigine (progestogens have no effect)
EffectLamotrigine levels decrease ~50%; fluctuate during pill-free week
ManagementMay need to increase maintenance dose up to 2-fold when starting OCP; decrease by ~50% when stopping OCP
FDA PI
Moderate Rifampin / Lopinavir-Ritonavir
MechanismInduction of UGT glucuronidation
EffectLamotrigine levels decrease ~40–50%
ManagementFollow enzyme-inducer dosing schedule
FDA PI
Moderate Atazanavir/Ritonavir
MechanismUGT induction
EffectLamotrigine exposure decreases ~32%
ManagementDose escalation per standard schedule; may need to increase maintenance dose if added to stable lamotrigine
FDA PI
Minor OCT2 Substrates (e.g., dofetilide, metformin)
MechanismLamotrigine inhibits OCT2, potentially reducing renal clearance of OCT2 substrates
EffectPossible increased levels of narrow-therapeutic-index OCT2 substrates
ManagementCoadministration with narrow-therapeutic-index OCT2 substrates not recommended (FDA PI)
FDA PI
Mon

Monitoring

  • Skin / Rash First 8 weeks intensively
    Routine     Instruct patients and caregivers to report ANY rash immediately. Nearly all life-threatening rashes occur within the first 2–8 weeks. Discontinue at first sign of rash unless clearly not drug-related. Risk factors: concomitant VPA, exceeding recommended titration rate, HLA-B*1502 allele (Han Chinese and Thai ancestry).
  • Mood / Suicidality Each visit
    Routine     Assess for new or worsening depression, suicidal ideation, and clinical worsening of bipolar disorder. AED class warning applies. Particularly important during titration and dose changes.
  • Hepatic Function Baseline; if symptomatic
    Trigger-based     Isolated liver failure and hepatic failure as part of multiorgan hypersensitivity have been reported. Obtain LFTs if patient develops signs suggestive of hepatic dysfunction (jaundice, dark urine, fatigue, anorexia).
  • Lamotrigine Levels Concomitant medication changes; pregnancy
    Trigger-based     No established therapeutic range. However, TDM is useful when adding or removing drugs affecting UGT (especially VPA, OCP, enzyme inducers) and during pregnancy (clearance increases up to 2-fold). Proposed reference range: 3–14 mcg/mL (epilepsy).
  • CBC If symptomatic
    Trigger-based     Blood dyscrasias (neutropenia, thrombocytopenia, pancytopenia) may occur with or without hypersensitivity syndrome. Monitor for signs of anemia, unexpected infection, or bleeding.
  • HLA-B*1502 Testing Before initiation (specific populations)
    Trigger-based     Consider HLA-B*1502 testing in patients of Han Chinese or Thai ancestry before starting lamotrigine. Positive allele status confers 2–3-fold increased risk of SJS/TEN. However, genotyping has limitations and should not replace clinical vigilance.
CI

Contraindications & Cautions

Absolute Contraindications

  • Known hypersensitivity to lamotrigine or any formulation ingredient — including prior SJS/TEN, angioedema, acute urticaria, extensive pruritus, or mucosal ulceration attributed to lamotrigine

Relative Contraindications (Specialist Input Recommended)

  • Prior rash with lamotrigine (non-serious) — Do not restart unless benefits clearly outweigh risks; if restarting, use initial titration schedule regardless of previous dose
  • Clinically significant structural or functional heart disease — In vitro data show lamotrigine inhibits cardiac sodium channels; could cause serious arrhythmias in patients with underlying cardiac disorders (FDA PI Section 5.4; added to labelling based on in vitro data)
  • HLA-B*1502 positive status — 2–3-fold increased risk of SJS/TEN; weigh risks vs benefits carefully

Use with Caution

  • Concomitant valproate — Doubles lamotrigine levels and increases serious rash risk; requires special dosing schedule
  • Hepatic impairment (moderate/severe) — Dose reduction required; half-life can extend to 100 hours with severe disease plus ascites
  • Renal impairment (significant) — Limited data; reduced maintenance doses may be appropriate; use with caution in severe renal impairment
  • Pregnancy — Clearance may increase up to 2-fold during pregnancy; levels should be monitored; animal data suggest potential fetal harm
FDA Boxed Warning Serious Skin Rashes Including Stevens-Johnson Syndrome and Toxic Epidermal Necrolysis

Lamotrigine can cause serious rashes requiring hospitalisation and discontinuation of treatment. The incidence is approximately 0.3–0.8% in pediatric patients (aged 2–17 years) and 0.08–0.3% in adults. One rash-related death occurred in a prospectively followed cohort of 1,983 pediatric patients. Rare cases of TEN and rash-related death have been reported in postmarketing experience. Risk factors include concomitant valproate, exceeding recommended initial dose or dose escalation rate, and HLA-B*1502 allele. Nearly all life-threatening rashes occur within 2–8 weeks of treatment initiation. Discontinue at the first sign of rash unless the rash is clearly not drug-related.

Pt

Patient Counselling

Purpose of Therapy

Lamotrigine helps control seizures or stabilise mood by reducing abnormal electrical activity in the brain. For epilepsy, it reduces the frequency and severity of seizures. For bipolar disorder, it helps prevent future episodes of depression and mania when taken consistently as a maintenance treatment — it is not used to treat acute mood episodes.

How to Take

Lamotrigine can be taken with or without food. The dose must be increased very slowly over several weeks according to a specific schedule provided by the prescriber. Do not increase the dose faster than instructed, even if seizures continue, as doing so significantly increases the risk of a serious skin reaction. Tablets should be swallowed whole; chewable tablets can be chewed, dissolved in water, or swallowed whole. Always visually inspect tablets to confirm you have received the correct medication and strength — medication mix-ups with similarly named drugs have been reported.

Skin Rash (Most Critical)
Tell patient A rash can develop, particularly in the first 2–8 weeks. Most rashes are harmless, but a small number can become life-threatening. There is no reliable way to tell early on whether a rash will become serious.
Call prescriber Immediately if ANY rash develops, regardless of how minor it appears. Seek emergency care if the rash is accompanied by fever, swollen lymph nodes, mouth sores, blistering, or peeling skin.
Dizziness, Vision Changes & Coordination
Tell patient Dizziness, double vision, and unsteadiness are the most common side effects and are usually dose-related. They often improve over time or with dose adjustment. Avoid driving or operating machinery until you know how lamotrigine affects you.
Call prescriber If dizziness, double vision, or coordination problems are severe, persistent, or worsen after a dose increase.
Contraception & Pregnancy
Tell patient Estrogen-containing birth control pills can halve lamotrigine levels, potentially causing seizure breakthroughs or mood instability. Stopping the pill can double lamotrigine levels, causing increased side effects. Inform your prescriber before starting, stopping, or changing any hormonal contraceptive. If you become pregnant, contact your prescriber immediately — lamotrigine levels change during pregnancy and close monitoring is needed.
Call prescriber Before starting or stopping any hormonal contraceptive; immediately if pregnancy is confirmed or planned.
Do Not Stop Suddenly
Tell patient Stopping lamotrigine abruptly can trigger breakthrough seizures or status epilepticus. The dose should always be tapered gradually (over at least 2 weeks) under medical supervision.
Call prescriber Before making any changes to your dosing schedule. If you run out of medication, seek an urgent supply to avoid missing doses.
Ref

Sources

Regulatory (PI / SmPC)
  1. GlaxoSmithKline. LAMICTAL (lamotrigine) prescribing information. Revised 10/2025. Reference ID: 5675542. FDA Label Primary regulatory source for all indications, dosing tables, adverse reactions, boxed warning, and pharmacokinetics cited in this monograph.
  2. GlaxoSmithKline. LAMICTAL XR (lamotrigine) extended-release tablets prescribing information. GSK PI Extended-release formulation PI; approved for partial-onset seizures in patients 13 years and older, and PGTC in patients 13 years and older with idiopathic generalized epilepsy.
Key Clinical Trials
  1. Messenheimer J, Mullens EL, Giorgi L, et al. Safety review of adult clinical trial experience with lamotrigine. Drug Saf. 1998;18(4):281–296. DOI Comprehensive safety review of lamotrigine across clinical trials including rash incidence data and discontinuation rates.
  2. Bowden CL, Calabrese JR, Sachs G, et al. A placebo-controlled 18-month trial of lamotrigine and lithium maintenance treatment in recently manic or hypomanic patients with bipolar I disorder. Arch Gen Psychiatry. 2003;60(4):392–400. DOI Pivotal RCT establishing lamotrigine efficacy for bipolar I maintenance, demonstrating delay in time to intervention for mood episodes.
  3. Calabrese JR, Bowden CL, Sachs G, et al. A placebo-controlled 18-month trial of lamotrigine and lithium maintenance treatment in recently depressed patients with bipolar I disorder. J Clin Psychiatry. 2003;64(9):1013–1024. DOI Companion pivotal trial to Bowden 2003, focusing on recently depressed bipolar I patients; demonstrated delay in depressive episodes.
  4. Brodie MJ, Richens A, Yuen AW. Double-blind comparison of lamotrigine and carbamazepine in newly diagnosed epilepsy. Lancet. 1995;345(8948):476–479. DOI Head-to-head trial demonstrating comparable efficacy to carbamazepine in newly diagnosed epilepsy with superior tolerability.
Guidelines
  1. Glauser T, Ben-Menachem E, Bourgeois B, et al. Updated ILAE evidence review of antiepileptic drug efficacy and effectiveness as initial monotherapy for epileptic seizures and syndromes. Epilepsia. 2013;54(3):551–563. DOI ILAE guideline supporting lamotrigine as a first-line option for initial monotherapy in focal and generalised seizures.
  2. Yatham LN, Kennedy SH, Parikh SV, et al. Canadian Network for Mood and Anxiety Treatments (CANMAT) and International Society for Bipolar Disorders (ISBD) 2018 guidelines for the management of patients with bipolar disorder. Bipolar Disord. 2018;20(2):97–170. DOI International guideline recommending lamotrigine as a first-line maintenance agent for bipolar I disorder, particularly for preventing depressive episodes.
Mechanistic / Basic Science
  1. Xie X, Lancaster B, Bhatt K, et al. Interaction of the antiepileptic drug lamotrigine with recombinant rat brain type IIA Na+ channels and with native Na+ channels in rat hippocampal neurones. Pflugers Arch. 1995;430(3):437–446. DOI Key mechanistic study demonstrating use-dependent sodium channel blockade as the primary mechanism of action of lamotrigine.
Pharmacokinetics / Special Populations
  1. Rambeck B, Wolf P. Lamotrigine clinical pharmacokinetics. Clin Pharmacokinet. 1993;25(6):433–443. DOI Comprehensive PK review establishing key pharmacokinetic parameters including half-life variability with concomitant AEDs.
  2. Garnett WR. Lamotrigine: pharmacokinetics. J Child Neurol. 1997;12(Suppl 1):S10–S15. DOI Detailed review of lamotrigine PK in adults and children, including effects of enzyme inducers and inhibitors on half-life.
  3. Pennell PB, Peng L, Newport DJ, et al. Lamotrigine in pregnancy: clearance, therapeutic drug monitoring, and seizure frequency. Neurology. 2008;70(22 Pt 2):2130–2136. DOI Key study demonstrating up to 2-fold increase in lamotrigine clearance during pregnancy, supporting the need for therapeutic drug monitoring.
  4. Sabers A, Buchholt JM, Uldall P, et al. Lamotrigine plasma levels reduced by oral contraceptives. Epilepsy Res. 2001;47(1-2):151–154. DOI Study documenting the ~50% reduction in lamotrigine levels caused by estrogen-containing oral contraceptives.