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Bedside Snapshot
  • Workhorse ASM: Broad-spectrum antiseizure medication for new-onset seizures, status epilepticus adjunct, and post-neurosurgery/ICH/TBI prophylaxis
  • IV/PO Equivalence: IV and PO have essentially 1:1 equivalence; easy to transition from IV → PO when enteral route available
  • Common ICU Dosing: Loading 60 mg/kg IV (max 4,500 mg) for status epilepticus (many centers 40–60 mg/kg), then 1,000–1,500 mg IV/PO q12h for maintenance
  • Renal Clearance: Renally cleared → dose-reduce in CKD; minimal hepatic metabolism and very few drug–drug interactions compared with older agents
  • Major Downside: Behavioral/psychiatric effects (agitation, irritability, mood change, psychosis) and somnolence; watch closely in delirious or brain-injured patients
  • Key Advantage: Generally hemodynamically stable, non-sedating at typical doses, and safe in hepatic dysfunction, which is why neuro/ICU teams love it
Brand & Generic Names
  • Generic Name: Levetiracetam
  • Brand Names: Keppra, Keppra XR, generics
Medication Class

Antiseizure medication (ASM); pyrrolidone derivative; SV2A modulator

Pharmacology

Mechanism of Action:

  • Binds to synaptic vesicle protein 2A (SV2A), a presynaptic protein involved in neurotransmitter release; modulation of SV2A is thought to reduce neuronal excitability and seizure propagation
  • Also may inhibit N-type calcium channels and modulate GABA and glycine–gated currents in some models, but the exact antiseizure mechanism is not fully defined
  • Does not act via classic sodium channel blockade like phenytoin/carbamazepine, which may contribute to its more favorable interaction profile

Pharmacokinetics:

  • Bioavailability: Oral ≈ 100%; IV and PO are interchangeable 1:1 on a mg-per-mg basis
  • Onset: Peak concentration ~1 hour after PO; IV administration achieves peak at end of infusion (commonly 15 minutes)
  • Distribution: Low protein binding (<10%); volume of distribution ~0.5–0.7 L/kg; good CNS penetration
  • Metabolism: Minimal hepatic metabolism (non–CYP mediated hydrolysis)
  • Elimination: ~66% excreted unchanged in urine; elimination half-life ~6–8 hours in normal renal function, prolonged in CKD
  • Special Considerations: Dose adjustment is required in reduced creatinine clearance; not significantly affected by hepatic impairment alone
Indications
  • Acute treatment of status epilepticus (after benzodiazepine) as part of first- or second-line ASM therapy
  • New-onset focal or generalized seizures in ED/ICU when long-term ASM is likely
  • Seizure prophylaxis in selected patients: TBI, subarachnoid hemorrhage, intracerebral hemorrhage, post–brain tumor resection (per neurosurgery/neurocritical care protocols)
  • Conversion from older ASMs (e.g., phenytoin) in critically ill patients when interaction or toxicity concerns arise
Dosing & Administration

Available Forms:

  • IV solution: 100 mg/mL (e.g., 500 mg/5 mL, 1,000 mg/10 mL, etc.) for dilution in compatible fluids
  • Immediate-release tablets: 250 mg, 500 mg, 750 mg, 1,000 mg
  • Oral solution: 100 mg/mL (varies by manufacturer)
  • Extended-release (XR) tablets: typically once-daily dosing, more outpatient than ICU

Adult Dosing (IV/PO):

Indication / Scenario Dose Route / Frequency Notes
Status epilepticus loading (common ICU) 60 mg/kg (max 4,500 mg) IV once over 10–15 min Some protocols 40–60 mg/kg; avoid underdosing
Alternative loading dose 20–40 mg/kg (max 3,000 mg) IV once Used where lower loading is standard or renal concerns
Maintenance – typical starting dose 500–1,000 mg IV/PO q12h Often increased quickly to 1,000–1,500 mg q12h in ICU
High-end maintenance (select patients) 1,500 mg IV/PO q12h (3,000 mg/day) Doses up to 4,000–6,000 mg/day used off-label in refractory cases
CrCl 50–80 mL/min 500–1,000 mg q12h Usually no major change, but avoid very high doses
CrCl 30–50 mL/min 250–750 mg q12h Reduce dose; consider lower loading in severe CKD
CrCl <30 mL/min (non-dialysis) 250–500 mg q12h Consider 50% loading dose reduction; consult pharmacy/neuro
Intermittent hemodialysis 500–1,000 mg q24h + 250–500 mg post-HD IV/PO Follow unit-specific dialysis dosing protocols
Contraindications

Contraindications:

  • Known hypersensitivity to levetiracetam or other pyrrolidone derivatives
  • History of serious hypersensitivity reaction (e.g., anaphylaxis, angioedema) to the drug

Major Precautions:

  • Behavioral and psychiatric effects: irritability, agitation, mood lability, depression, and psychosis can occur—monitor closely, especially in patients with prior psychiatric disease or delirium
  • Somnolence and fatigue: generally less sedating than many ASMs, but can still contribute to decreased alertness, especially at high doses or with other CNS depressants
  • Renal impairment: accumulation increases risk of adverse effects; adjust dose based on creatinine clearance
  • Gradual taper is recommended when discontinuing chronic therapy to avoid increased seizure risk
  • Use caution in pregnancy; levetiracetam is often preferred over older agents but still requires risk–benefit discussion and folate supplementation
Behavioral Effects: Severe agitation, aggression, psychosis, and suicidal ideation can occur. Monitor closely after initiation or dose escalation, especially in patients with prior psychiatric disease or delirium.
Renal Dosing Required: Must adjust dose based on creatinine clearance. Accumulation in CKD increases risk of adverse effects.
Adverse Effects

Common:

  • Somnolence, fatigue
  • Dizziness, incoordination
  • Headache
  • Nausea, vomiting, decreased appetite
  • Irritability, agitation, anxiety

Serious:

  • Behavioral disturbances: severe agitation, aggression, psychosis, suicidal ideation
  • Serious hypersensitivity reactions including Stevens–Johnson syndrome (rare)
  • Blood dyscrasias (e.g., neutropenia, pancytopenia) – rare but reported
  • Increased seizure frequency with abrupt withdrawal or nonadherence
Special Populations

Elderly Patients:

  • Often have reduced renal function; adjust dose accordingly
  • Start at lower end of dosing range
  • Monitor for somnolence and falls risk

Renal Impairment:

  • Dose adjustment essential based on CrCl (see dosing table)
  • Consider 50% loading dose reduction in severe CKD
  • Post-dialysis supplemental doses required

Hepatic Impairment:

  • No dose adjustment required for hepatic impairment alone
  • Advantage over older ASMs with hepatic metabolism

Pregnancy:

  • Often preferred over older ASMs (less teratogenic)
  • Still requires risk-benefit discussion
  • Folate supplementation recommended
  • Levels may decrease in pregnancy; monitor clinical response

Lactation:

  • Excreted in breast milk
  • Monitor infant for sedation, poor feeding
Monitoring

Clinical Monitoring:

  • Clinical seizure control: frequency, duration, and electrographic seizures if on continuous EEG
  • Mental status and behavior for signs of agitation, mood change, or psychosis—especially after initiation or dose escalation
  • Renal function (SCr, CrCl) regularly in critically ill patients to guide dosing
  • CBC periodically with prolonged use, particularly if infection, bruising, or fatigue occurs
  • Adherence and timing of doses when transitioning IV → PO and at ICU-to-floor or floor-to-home handoffs
Clinical Pearls
Don't Underdose the Load: In status epilepticus, 60 mg/kg (max 4.5 g) is now common and well tolerated hemodynamically.
Easy IV to PO Transition: Because IV and PO are 1:1, you can safely transition as soon as enteral access is reliable—helpful for step-down and discharge planning.
Minimal Interactions: Compared with phenytoin/fosphenytoin, levetiracetam has minimal interactions (no CYP induction), making it ideal in polypharmacy ICU patients.
Behavioral Issues: If behavior becomes an issue (new severe agitation, psychosis), consider dose reduction, slower titration, or alternative ASM in coordination with neurology/psychiatry.
Renal Failure Check: In renal failure, check that high maintenance doses have been reduced—iatrogenic overshoot is common when patients crash into AKI.
First-Line in Many Centers: Increasingly preferred as first-line ASM due to favorable side effect profile, lack of drug interactions, and hemodynamic stability compared to older agents.
References
  • 1. Lexicomp. (2024). Levetiracetam: Drug information. Wolters Kluwer.
  • 2. Glauser, T., Shinnar, S., Gloss, D., et al. (2016). Evidence-based guideline: Treatment of convulsive status epilepticus in children and adults. Epilepsy Currents, 16(1), 48–61. https://doi.org/10.5698/1535-7597-16.1.48
  • 3. Brophy, G. M., Bell, R., Claassen, J., et al. (2012). Guidelines for the evaluation and management of status epilepticus. Neurocritical Care, 17(1), 3–23. https://doi.org/10.1007/s12028-012-9695-z
  • 4. Patsalos, P. N. (2000). Pharmacokinetic profile of levetiracetam: Toward ideal characteristics. Pharmacology & Therapeutics, 85(2), 77–85. https://doi.org/10.1016/S0163-7258(99)00052-2
  • 5. Kapur, J., Elm, J., Chamberlain, J. M., et al. (2019). Randomized trial of three anticonvulsant medications for status epilepticus. New England Journal of Medicine, 381(22), 2103–2113. https://doi.org/10.1056/NEJMoa1905795
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