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Drug Monograph

Cannabidiol (Epidiolex)

cannabidiol — plant-derived purified cannabinoid antiseizure medication

Antiseizure Medication (ASM) · Oral Solution · Not a Controlled Substance
Pharmacokinetic Profile
Half-Life
56–61 h (steady state)
Metabolism
CYP2C19, CYP3A4; UGT1A7, UGT1A9, UGT2B7
Protein Binding
>94%
Bioavailability
Highly variable; food increases AUC 3–4-fold
Volume of Distribution
20,963–42,849 L (apparent)
Clinical Information
Drug Class
Cannabinoid Antiseizure Medication
Available Doses
100 mg/mL oral solution (60 mL and 100 mL bottles)
Route
Oral solution (also via NG/G-tube)
Renal Adjustment
Not studied; minor renal clearance
Hepatic Adjustment
Required for moderate & severe impairment; see dosing table
Pregnancy
Potential fetal harm (animal data)
Lactation
Unknown in human milk
Schedule / Legal Status
Not a controlled substance (descheduled April 2020)
Generic Available
No
Rx

Indications

IndicationApproved PopulationTherapy TypeStatus
Seizures associated with Lennox-Gastaut syndrome (LGS)≥1 year of ageAdjunctiveFDA Approved
Seizures associated with Dravet syndrome (DS)≥1 year of ageAdjunctiveFDA Approved
Seizures associated with tuberous sclerosis complex (TSC)≥1 year of ageAdjunctiveFDA Approved

Cannabidiol was the first plant-derived, pharmaceutical-grade cannabinoid approved by the FDA. The initial approval in June 2018 covered LGS and DS in patients 2 years and older. The TSC indication was added in 2020, and the age range was subsequently expanded to patients 1 year of age and older based on additional clinical data. Epidiolex was initially classified as Schedule V but was fully descheduled by the DEA in April 2020 after data confirmed negligible abuse potential. It remains the only FDA-approved prescription cannabidiol product and should not be confused with unregulated over-the-counter CBD products, which lack the same manufacturing controls and clinical evidence.

Off-Label Uses

Other treatment-resistant epilepsy syndromes: Open-label data and expanded access programs suggest benefit in CDKL5 deficiency, Aicardi syndrome, and other refractory epilepsies, but no controlled trial evidence supports these uses. Evidence quality: Low.

Anxiety disorders: Preliminary clinical trials in adults show anxiolytic effects at single doses of 300–600 mg; no FDA-approved indication exists. Evidence quality: Low.

Dose

Dosing

Dosing by Clinical Scenario

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
LGS or DS — adjunctive therapy2.5 mg/kg BID (5 mg/kg/day)5 mg/kg BID (10 mg/kg/day)10 mg/kg BID (20 mg/kg/day)Increase to 10 mg/kg/day after 1 week; further increases in weekly increments of 5 mg/kg/day
20 mg/kg/day gives modestly greater efficacy but more adverse effects
TSC — adjunctive therapy2.5 mg/kg BID (5 mg/kg/day)12.5 mg/kg BID (25 mg/kg/day)12.5 mg/kg BID (25 mg/kg/day)Increase weekly by 2.5 mg/kg BID (5 mg/kg/day) to target; faster titration every other day if clinically warranted
Doses below 25 mg/kg/day not studied for TSC efficacy
Moderate hepatic impairment (Child-Pugh B)1.25 mg/kg BID (2.5 mg/kg/day)LGS/DS: 2.5–5 mg/kg BID; TSC: 6.25 mg/kg BIDLGS/DS: 10 mg/kg/day; TSC: 12.5 mg/kg/dayAll doses halved vs normal; slower titration may be needed
AUC 2.5–5.2-fold higher vs healthy controls
Severe hepatic impairment (Child-Pugh C)0.5 mg/kg BID (1 mg/kg/day)LGS/DS: 1–2 mg/kg BID; TSC: 2.5 mg/kg BIDLGS/DS: 4 mg/kg/day; TSC: 5 mg/kg/dayDoses reduced to approximately one-fifth of normal
Consider not initiating if evidence of significant liver injury at baseline
Concomitant strong CYP3A4/2C19 inducers (e.g., rifampin)Standard starting doseUp to 2-fold increase based on responseUp to 2x standard maxRifampin reduces CBD AUC by ~32% and active metabolite 7-OH-CBD by ~63%
Adjust based on clinical response and tolerability
Clinical Pearl: Food Effect and Dosing Consistency

Cannabidiol absorption is highly food-dependent: a high-fat meal increases Cmax 5-fold and AUC 4-fold compared to the fasted state. Even low-fat meals and milk produce 3-fold increases. This variability can lead to unpredictable efficacy and toxicity. Advise patients and caregivers to dose Epidiolex consistently with respect to meals at every administration to minimize pharmacokinetic fluctuations. The PI does not mandate fed or fasted administration, but consistency is critical.

Baseline Lab Requirement

Serum transaminases (ALT and AST) and total bilirubin must be obtained in all patients before starting Epidiolex, due to the risk of hepatocellular injury. Do not initiate in patients with baseline ALT >3x ULN with bilirubin >2x ULN without prior evaluation.

PK

Pharmacology

Mechanism of Action

The precise mechanisms by which cannabidiol exerts its antiseizure effects in humans remain unknown. Notably, cannabidiol does not appear to act through cannabinoid CB1 or CB2 receptors, distinguishing it from tetrahydrocannabinol (THC) and other psychoactive cannabinoids. Preclinical research suggests multiple potential targets including modulation of intracellular calcium signaling, enhancement of adenosine-mediated signaling through equilibrative nucleoside transporter (ENT1) inhibition, activation of TRPV1 vanilloid receptors, and modulation of GPR55 signaling. The active metabolite 7-OH-CBD also demonstrates anticonvulsant activity in preclinical seizure models, while the major circulating metabolite 7-COOH-CBD (approximately 40-fold higher AUC than the parent) is not pharmacologically active against seizures.

ADME Profile

ParameterValueClinical Implication
AbsorptionTmax 2.5–5 h at steady state; less than dose-proportional increase over 5–25 mg/kg/day; high-fat meal increases Cmax 5-fold and AUC 4-foldHighly lipophilic oral solution in sesame seed oil; food effect is clinically significant — consistent dosing relative to meals is mandatory
DistributionVd/F 20,963–42,849 L; protein binding >94%Extremely large apparent Vd reflects high lipophilicity and extensive tissue distribution; highly protein-bound
MetabolismHepatic and gut metabolism via CYP2C19, CYP3A4, UGT1A7, UGT1A9, UGT2B7; active metabolite 7-OH-CBD (AUC 38% lower than parent); major metabolite 7-COOH-CBD (AUC ~40-fold higher, inactive)Dual CYP/UGT metabolism creates complex interaction profile; inhibits CYP2C19 (clinically relevant for clobazam) and intestinal P-gp (relevant for everolimus)
Eliminationt½ 56–61 h (after 7 days BID dosing); CL/F 1111 L/h; primarily fecal excretion with minor renal clearanceLong half-life supports twice-daily dosing; fecal elimination predominant; no renal dose adjustment studied or recommended
SE

Side Effects

Adverse reaction data for LGS and DS are from pooled placebo-controlled trials (Studies 1, 2, 3; n = 323 cannabidiol, n = 227 placebo). TSC data are from Study 4 (n = 75 cannabidiol 25 mg/kg/day, n = 76 placebo). Most adverse effects are dose-dependent and more prominent with concomitant valproate or clobazam.

≥10% Very Common (LGS/DS Trials)
Adverse EffectIncidence (10 / 20 mg/kg/day)Clinical Note
Somnolence23% / 25% vs 8% placeboDose-related; markedly higher with concomitant clobazam (46% vs 16% without clobazam); generally improves over time
Decreased appetite16% / 22% vs 5% placeboCan lead to weight loss; 16–18% had ≥5% weight decrease at 20 mg/kg/day; monitor growth in pediatric patients
Diarrhea9% / 20% vs 9% placeboDose-related; may be partly related to sesame oil vehicle; usually manageable
Transaminases elevated8% / 16% vs 3% placeboALT >3x ULN in 13% overall; risk substantially higher with concomitant valproate (up to 30% with VPA + clobazam); typically first 2 months
Fatigue, malaise, asthenia11% / 12% vs 4% placeboPart of the broader CNS depression spectrum with cannabidiol
Rash7% / 13% vs 3% placeboDose-related; was the most frequent cause of discontinuation in the TSC trial (5%)
Insomnia / sleep disorder11% / 5% vs 4% placeboParadoxically more common at lower dose in trials; clinical significance uncertain
Infections (all types)41% / 40% vs 31% placeboIncludes viral infections (7–11%), pneumonia (5–8%), and other infections; pneumonia rate higher with concomitant clobazam
1–10% Common
Adverse EffectIncidence (20 mg/kg/day LGS/DS)Clinical Note
Lethargy8% vs 2% placeboPart of somnolence/sedation cluster; more common with clobazam
Sedation6% vs 1% placeboAdditive with other CNS depressants and alcohol
Aggression, anger5% vs <1% placeboBehavioral adverse effect; monitor in pediatric patients
Irritability, agitation5% vs 2% placeboMay be dose-related or related to underlying epilepsy syndrome
Weight decreased5% vs 1% placebo31% of TSC patients had ≥5% weight loss at 25 mg/kg/day
Pneumonia5% vs 1% placeboRisk substantially higher with concomitant clobazam (10–17%); monitor respiratory function
Drooling / salivary hypersecretion4% vs <1% placeboMore common in younger children
Gastroenteritis4% vs 1% placeboGI effects cluster; may relate to sesame oil formulation
Vomiting17% vs 9% placebo (TSC data; not listed in LGS/DS table)Primarily a TSC finding at 25 mg/kg/day; not reported above placebo threshold in LGS/DS trials
Serious Serious Adverse Effects (Regardless of Frequency)
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Hepatocellular Injury (ALT >3x ULN)13% (LGS/DS) / 12% (TSC) vs 1% placebo; ALT >20x ULN in <1%Typically first 2 months; cases reported up to 18 monthsMandatory LFT monitoring at baseline, 1, 3, 6 months; discontinue if ALT >3x ULN with bilirubin >2x ULN, or ALT >5x ULN sustained; consider VPA/clobazam dose reduction. Postmarketing cholestatic/mixed liver injury also reported
Suicidal Behavior and IdeationAED class effect (RR 1.8 vs placebo)As early as 1 week after initiationMonitor for depression, mood changes, suicidal ideation; counsel patients and caregivers
Hypersensitivity ReactionsRare (pruritus, erythema, angioedema reported in clinical trials)VariableDiscontinue and do not restart; contains sesame seed oil (allergen). Treated with corticosteroids and antihistamines in trials
Pneumonia (with clobazam)10–17% with clobazam vs 0–4% without clobazamDuring treatmentMonitor respiratory status in patients on concomitant clobazam; consider clobazam dose reduction if sedation impairs airway protection
Hematologic Abnormalities (Anemia)New-onset anemia in 30% (LGS/DS) and 38% (TSC) vs 13–15% placeboDuring treatment courseMean Hb decrease –0.37 to –0.42 g/dL; monitor CBC; no effect on RBC indices; clinical significance unclear
Discontinuation Discontinuation Rates
LGS/DS — 10 mg/kg/day
2.7% vs 1.3% placebo
Top reason: Transaminase elevation (1.3%)
LGS/DS — 20 mg/kg/day
11.8% vs 1.3% placebo
Top reasons: Transaminase elevation (5.9%), somnolence/sedation/lethargy (3%)
TSC — 25 mg/kg/day
11% vs 3% placebo
Top reason: Rash (5%)
Managing Hepatotoxicity: The Cardinal Safety Concern

Transaminase elevation is the single most important safety issue with cannabidiol. The risk is dramatically amplified by concomitant valproate: ALT >3x ULN occurred in 30% of patients taking both valproate and clobazam, 21% with valproate alone, versus only 3% without either drug. Higher cannabidiol doses and elevated baseline transaminases further compound the risk. In approximately two-thirds of cases, transaminase elevations resolve with dose reduction of cannabidiol and/or valproate, while in one-third they resolve spontaneously without dose changes. A structured LFT monitoring schedule (baseline, 1, 3, 6 months, then periodically) is mandatory, not optional.

Int

Drug Interactions

Cannabidiol has a broad interaction profile driven by CYP2C19 inhibition, intestinal P-gp inhibition, UGT1A9/UGT2B7 inhibition, and weak CYP1A2 inhibition. CBD itself is a substrate of CYP2C19 and CYP3A4. Of note, cannabidiol does not significantly affect midazolam (CYP3A4 substrate) exposure, suggesting its CYP3A4 inhibitory potential is limited in vivo.

Major Clobazam (N-desmethylclobazam)
MechanismCBD inhibits CYP2C19, increasing N-desmethylclobazam (active metabolite) ~3-fold; no change to parent clobazam
EffectIncreased somnolence (46% vs 16%), sedation, pneumonia risk; contributes to hepatotoxicity risk
ManagementReduce clobazam dose if adverse effects occur; monitor sedation and respiratory function closely
FDA PI
Major Valproate
MechanismSynergistic hepatotoxicity (mechanism not fully elucidated); CBD decreases valproate hepatotoxic metabolite 4-ene-VPA by ~28–33%
EffectALT >3x ULN in 21–30% with concomitant VPA vs 3% without; elevated ammonia also reported
ManagementIntensified LFT monitoring; reduce VPA and/or CBD dose if transaminases rise; check ammonia if transaminases elevated
FDA PI
Major Everolimus (oral P-gp/CYP3A4 substrate)
MechanismCBD inhibits intestinal P-gp efflux of everolimus
EffectEverolimus Cmax and AUC increased ~2.5-fold
ManagementLower starting dose of everolimus; mandatory therapeutic drug monitoring; relevant in TSC patients already on mTOR inhibitors
FDA PI
Moderate Stiripentol
MechanismMechanism not fully determined
EffectStiripentol AUC increased 30–55% and Cmax 17–28%
ManagementMonitor for stiripentol-related adverse effects; dose adjustment may be needed; particularly relevant in Dravet syndrome patients
FDA PI
Moderate Caffeine (CYP1A2 substrate)
MechanismCBD weakly inhibits CYP1A2
EffectCaffeine AUC increased 95%, Cmax increased 15%
ManagementConsider dose reduction of sensitive CYP1A2 substrates (theophylline, tizanidine) if adverse effects occur
FDA PI
Moderate Rifampin (strong CYP3A4/2C19 inducer)
MechanismCYP3A4 and CYP2C19 induction increases CBD metabolism
EffectCBD AUC decreased ~32%; 7-OH-CBD AUC decreased ~63%
ManagementConsider up to 2-fold increase in CBD dose based on clinical response; applies to all strong CYP3A4/2C19 inducers
FDA PI
Moderate CYP2C19 Substrates (e.g., diazepam)
MechanismCBD inhibits CYP2C19
EffectIncreased plasma concentrations of CYP2C19 substrates
ManagementConsider dose reduction of sensitive CYP2C19 substrates; monitor for adverse effects
FDA PI
Minor Other Oral P-gp Substrates (sirolimus, tacrolimus, digoxin)
MechanismCBD inhibits intestinal P-gp (in vivo)
EffectPotentially increased oral bioavailability of P-gp substrates
ManagementTherapeutic drug monitoring and dose reduction of P-gp substrates should be considered
FDA PI
Clinical Pearl: Drugs NOT Significantly Affected

Despite in vitro CYP3A4 substrate status, cannabidiol does not significantly alter midazolam concentrations in vivo. Additionally, itraconazole (potent CYP3A4 inhibitor) and fluconazole (potent CYP2C19 inhibitor) produce only minor, non-clinically meaningful changes in cannabidiol exposure. Valproate exposure is also not significantly changed by cannabidiol, though the hepatotoxicity interaction is pharmacodynamic, not pharmacokinetic.

Mon

Monitoring

  • Hepatic Function (ALT, AST, Bilirubin) Baseline, 1 mo, 3 mo, 6 mo, then periodically; within 1 mo of dose changes
    Routine     Most critical monitoring parameter. More frequent monitoring for patients on concomitant valproate or with elevated baseline LFTs. Discontinue if ALT >3x ULN with bilirubin >2x ULN or if ALT >5x ULN is sustained. Also monitor within 1 month of adding/changing hepatotoxic co-medications. Postmarketing: cholestatic and mixed liver injury patterns reported.
  • Weight and Growth Every visit, ongoing
    Routine     Decreased appetite and weight loss are dose-related (16–31% had ≥5% weight loss in trials). Particularly important in pediatric patients where growth monitoring is essential.
  • Complete Blood Count Baseline, then periodically
    Routine     New-onset anemia in 30–38% of treated patients vs 13–15% placebo. Mean hemoglobin decrease of 0.37–0.42 g/dL. No effect on RBC indices. In TSC: thrombocytopenia (5%) and eosinophilia (5%) also observed.
  • Serum Creatinine Baseline, then early in treatment
    Routine     CBD causes ~10% increase in serum creatinine within 2 weeks of initiation (mechanism unknown, not necessarily reflecting true GFR decline). Reversible in healthy adults.
  • Mood and Suicidality Every visit, ongoing
    Routine     AED class warning. Screen for depression, anxiety, behavioral changes, suicidal ideation at each visit.
  • Everolimus Levels When initiating CBD in patients on everolimus or vice versa
    Trigger-based     CBD increases everolimus AUC ~2.5-fold via P-gp inhibition. Mandatory TDM; critical in TSC patients already receiving mTOR inhibitor therapy.
  • Ammonia If transaminases elevated, especially with concomitant VPA
    Trigger-based     Elevated ammonia reported in patients with concurrent transaminase elevations, mostly on VPA/clobazam. Consider VPA/clobazam dose adjustment if ammonia elevated.
CI

Contraindications & Cautions

Absolute Contraindications

  • Hypersensitivity to cannabidiol or any ingredient in Epidiolex, including sesame seed oil (vehicle), dehydrated alcohol, strawberry flavor, or sucralose

Relative Contraindications (Specialist Input Recommended)

  • Significant baseline liver injury (ALT >3x ULN with bilirubin >2x ULN) — the PI recommends considering not initiating Epidiolex in these patients
  • Severe hepatic impairment (Child-Pugh C) — substantially reduced doses required (one-fifth of normal); AUC up to 5.2-fold higher; proceed only if anticipated benefit clearly outweighs risk
  • Pregnancy — animal data demonstrate embryofetal mortality (rats), decreased fetal weight (rabbits), and neurobehavioral/reproductive impairment in offspring at clinically relevant exposures. Enroll in the EPIDIOLEX Pregnancy Surveillance Program (1-855-272-7158) and NAAED Pregnancy Registry (1-888-233-2334)

Use with Caution

  • Concomitant valproate therapy — dramatically increases hepatotoxicity risk (ALT >3x ULN in up to 30%); intensified LFT schedule required
  • Concomitant clobazam therapy — 3-fold increase in active metabolite; increased somnolence (46%), sedation, and pneumonia risk; consider clobazam dose reduction
  • Moderate hepatic impairment (Child-Pugh B) — halve all doses; AUC 2.5-fold higher
  • Patients on oral P-gp substrates — especially everolimus (2.5-fold AUC increase), sirolimus, tacrolimus, digoxin; TDM required
  • Patients with depression or suicidal history — AED class warning applies
  • Alcohol use — increases cannabidiol exposure (Cmax +93%, AUC +63%) and potentiates CNS depression
  • Sesame allergy — Epidiolex contains sesame seed oil; assess for sesame allergy before prescribing
FDA Class-Wide Regulatory Warning Suicidal Behavior and Ideation — All Antiepileptic Drugs

Antiepileptic drugs, including Epidiolex, increase the risk of suicidal thoughts or behavior. Pooled analysis of 199 placebo-controlled trials of 11 AEDs showed approximately twice the risk (adjusted RR 1.8; 95% CI: 1.2–2.7) in AED-treated patients compared to placebo. Monitor all patients for emergence or worsening of depression, suicidal thoughts, or unusual changes in behavior.

Pt

Patient Counselling

Purpose of Therapy

Epidiolex is a prescription cannabidiol oral solution used to reduce the frequency of seizures associated with Lennox-Gastaut syndrome, Dravet syndrome, or tuberous sclerosis complex. It is the only FDA-approved prescription cannabidiol product and is manufactured to pharmaceutical standards, unlike unregulated over-the-counter CBD products. It will not produce a "high" because it contains no THC.

How to Take

Epidiolex is taken twice daily as a liquid measured with the provided oral syringes. It should be taken consistently either with food or without food at every dose, since food dramatically affects how much of the drug is absorbed. An opened bottle must be discarded after 12 weeks. Patients receiving Epidiolex via nasogastric or gastrostomy tube should follow specific flushing instructions provided in the product labeling. Epidiolex contains dehydrated alcohol (7.9% w/v) and sesame seed oil.

Liver Safety
Tell patient Epidiolex can cause liver problems, especially when taken with valproate (Depakote). Regular blood tests are required before starting and at 1, 3, and 6 months during treatment. These tests are essential and must not be skipped.
Call prescriber Immediately if you or your child develop unexplained nausea, vomiting, right upper abdominal pain, fatigue, loss of appetite, yellowing of the skin or eyes, or dark urine.
Drowsiness and Sedation
Tell patient Feeling sleepy is common, especially if also taking clobazam (Onfi). This effect usually improves over time. Avoid driving or operating machinery until you know how Epidiolex affects you. Alcohol can make drowsiness worse and also increases the amount of cannabidiol in the blood.
Call prescriber If sleepiness is severe, persists beyond a few weeks, or interferes with daily activities or breathing, especially in young children.
Appetite and Weight Loss
Tell patient Decreased appetite and weight loss are common, particularly at higher doses. In children, this may affect growth. Weigh your child regularly and report significant weight changes to your doctor.
Call prescriber If significant weight loss occurs (more than 5% of body weight), if the child is refusing to eat, or if growth appears to be slowing.
Drug Testing
Tell patient Epidiolex may cause a positive result on cannabis drug screening tests. If you are required to undergo drug testing, inform the person administering the test that you take prescription cannabidiol.
Call prescriber If a positive drug test result creates problems with employment, legal, or other situations, your prescriber can provide documentation confirming your prescription.
Do Not Stop Suddenly
Tell patient Never stop Epidiolex abruptly. Sudden discontinuation can trigger increased seizure frequency or status epilepticus. If treatment needs to end, your doctor will gradually reduce the dose.
Call prescriber If you cannot take Epidiolex for any reason (illness, supply issues) or if seizures worsen during dose changes.
Allergic Reactions
Tell patient Epidiolex contains sesame seed oil. Tell your doctor before starting if you have a sesame allergy. Allergic reactions including itching, redness, and swelling have occurred in clinical trials.
Call prescriber Immediately if you develop a skin rash, itching, swelling (especially of the face, lips, or throat), or difficulty breathing after taking Epidiolex.
Ref

Sources

Regulatory (PI / SmPC)
  1. EPIDIOLEX (cannabidiol) oral solution. Full Prescribing Information. Jazz Pharmaceuticals, Inc. Revised 03/2024. FDA Label Primary regulatory source for all dosing, pharmacokinetic, safety, and interaction data in this monograph.
  2. Epidiolex (cannabidiol) Summary of Product Characteristics. GW Pharma (International) B.V. EMA Approved. EMA EPAR European regulatory source for adjunctive indication in LGS and DS; marketed as Epidyolex in the EU.
Key Clinical Trials
  1. Thiele EA, Marsh ED, French JA, et al. Cannabidiol in patients with seizures associated with Lennox-Gastaut syndrome (GWPCARE4): a randomised, double-blind, placebo-controlled phase 3 trial. Lancet. 2018;391(10125):1085–1096. doi:10.1016/S0140-6736(18)30136-3 Study 1 (GWPCARE4): pivotal phase 3 LGS RCT demonstrating 44% median reduction in drop seizures at 20 mg/kg/day vs 22% placebo.
  2. Devinsky O, Patel AD, Cross JH, et al. Effect of cannabidiol on drop seizures in the Lennox-Gastaut syndrome. N Engl J Med. 2018;378(20):1888–1897. doi:10.1056/NEJMoa1714631 Study 2 (GWPCARE3): LGS RCT comparing 10 and 20 mg/kg/day with placebo; established efficacy of both dose levels.
  3. Devinsky O, Cross JH, Laux L, et al. Trial of cannabidiol for drug-resistant seizures in the Dravet syndrome. N Engl J Med. 2017;376(21):2011–2020. doi:10.1056/NEJMoa1611618 Study 3: pivotal DS RCT showing 39% median reduction in convulsive seizures at 20 mg/kg/day vs 13% placebo.
  4. Thiele EA, Bebin EM, Bhathal H, et al. Add-on cannabidiol treatment for drug-resistant seizures in tuberous sclerosis complex: a placebo-controlled randomized clinical trial. JAMA Neurol. 2021;78(3):285–292. doi:10.1001/jamaneurol.2020.4607 Study 4 (GWPCARE6): pivotal TSC RCT demonstrating 48% estimated mean seizure reduction at 25 mg/kg/day vs 24% placebo.
Guidelines
  1. Wirrell EC, Laux L, Donner E, et al. Optimizing the diagnosis and management of Dravet syndrome: recommendations from a North American consensus panel. Pediatr Neurol. 2017;68:18–34.e3. doi:10.1016/j.pediatrneurol.2017.01.025 North American consensus recommendations for Dravet syndrome management including role of cannabidiol in treatment algorithms.
  2. Cross JH, Auvin S, Falip M, et al. Expert opinion on the management of Lennox-Gastaut syndrome: treatment algorithms and practical considerations. Front Neurol. 2017;8:505. doi:10.3389/fneur.2017.00505 Expert consensus on LGS treatment algorithms providing context for where cannabidiol fits among therapeutic options.
Mechanistic / Basic Science
  1. Devinsky O, Cilio MR, Cross H, et al. Cannabidiol: pharmacology and potential therapeutic role in epilepsy and other neuropsychiatric disorders. Epilepsia. 2014;55(6):791–802. doi:10.1111/epi.12631 Seminal review of cannabidiol pharmacology covering non-CB receptor targets including TRPV1, GPR55, adenosine reuptake, and intracellular calcium modulation.
  2. Perucca E, Bialer M, White HS. New GABA-targeting therapies for the treatment of seizures and epilepsy: I. role of GABA as a modulator of seizure activity and recently approved medications acting on the GABA system. CNS Drugs. 2023;37(9):755–779. doi:10.1007/s40263-023-01025-4 Review of recently approved ASMs including cannabidiol, placing its mechanism in context of GABAergic and non-GABAergic pathways.
Pharmacokinetics / Special Populations
  1. Wheless JW, Dlugos D, Miller I, et al. Pharmacokinetics and tolerability of multiple doses of pharmaceutical-grade synthetic cannabidiol in pediatric patients with treatment-resistant epilepsy. CNS Drugs. 2019;33(6):593–604. doi:10.1007/s40263-019-00624-4 Pediatric pharmacokinetic data supporting weight-based dosing in treatment-resistant epilepsy populations.
  2. Lattanzi S, Brigo F, Trinka E, et al. Efficacy and safety of cannabidiol in epilepsy: a systematic review and meta-analysis. Drugs. 2018;78(17):1791–1804. doi:10.1007/s40265-018-0992-5 Systematic review and meta-analysis of cannabidiol efficacy across pivotal trials, quantifying responder rates and adverse event profiles.
  3. Gaston TE, Bebin EM, Cutter GR, Liu Y, Szaflarski JP. Interactions between cannabidiol and commonly used antiepileptic drugs. Epilepsia. 2017;58(9):1586–1592. doi:10.1111/epi.13852 Key study characterizing the clobazam interaction and N-desmethylclobazam level changes with cannabidiol co-administration.
  4. Devinsky O, Marsh E, Friedman D, et al. Cannabidiol in patients with treatment-resistant epilepsy: an open-label interventional trial. Lancet Neurol. 2016;15(3):270–278. doi:10.1016/S1474-4422(15)00379-8 Early open-label efficacy and safety data from 162 patients with treatment-resistant epilepsy that informed the design of subsequent pivotal trials.