Psychopharmacopeia: Online Searchable Psychopharmacology Drug Database for Clinicians

oxcarbazepine TRILEPTAL

Class: AED/Mood Stabilizer
FDA Indications: Partial Seizures
Off-Label Use: Neuropathic Pain, Bipolar Disorder, Restless Leg Syndrome

Prescribing

Forms: 150, 300, 600mg tablet; 300 mg/5 mL po soln
Dose Range: 600-2400 mg/day
Starting: 300 mg bid; usual daily dose is 1200 mg/day in 2 divided doses; dosage ↑'s are made Q3 days in increments of 150 mg or 300 mg depending on weight and tolerability
Stopping: Taper. Abrupt discontinuation can elicit seizures and increase the risk of relapse in bipolar patients
Monitoring: Serum Na⁺ for 1^st 3 mos b/c of possibility of hyponatremia

NAMI drug fact sheet

Precautions

Serious Side Effects: Hyponatremia (2.5%)
Side Effects: dizziness (20-49%), drowsiness (12-36%), headache, ataxia, fatigue, tremor, vomiting, nausea, diplopia, visual changes, nystagmus

Pharmacodynamics

1° MOA: Binds to a site located within the open channel conformation of the VSSC α subunit, which decreases repetitive firing and spread of electrical activity

Pharmacokinetics

t½: 7-20° T_MAX: 4.5°
Substrate of: AKR (oxcarbazepine→MHD), UGT (MHD→inactive metabolites→renal elimination)
Inhibits: 2C19; Induces: 3A4, UGT1A4
Active Metabolites: MHD

DDIs

- ↑'s levels of phenytoin
- ↓'s levels of lamotrigine & topiramate
- ↓'s levels of ethinylestradiol & levonorgestrel

Misc

- oxcarbazepine is a prodrug that is virtually entirely converted into MHD (by cytosolic AKR), which is responsible for the pharmacological effect of the drug
- unlike carbamazepine, MHD does not cause autoinduction of its own metabolism
- t½ of parent drug is 1-5°; t½ of MHD is 7-20°
- low potential for drug interactions
- compared to carbamazepine, less sedating, has less bone-marrow toxicity, and has fewer CYP3A4 interactions

Special Populations

Category C—Limited Human Data–Animal Data Suggest Risk: is embryo and fetal toxic and teratogenic in some animal species

Limited Human Data–Probably Compatible

No adjustments required

No dosage adjustment required in mild-moderate impairment, but should be initiated at ½ the usual starting dose in severe impairment (CrCl <30 mg/min)

No dose adjustment is needed for hepatically impaired subjects

References

Stahl's Essential Psychopharmacology 4th Ed
Applied Clinical Pharmacokinetics And Pharmacodynamics Of Psychopharmacological Agents
Foye's Principles Of Medicinal Chemistry
Drugs In Pregnancy And Lactation 11th Ed

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Last updated August 15 2022 20:48:12. Disclaimer: This website does not provide medical advice, nor is it a substitute for clinical judgment.

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