Carbamazepine Flashcards
Dr. Lugo Exam 2
Therapeutic range of carbamazepine
4-12 mg/L
preferred 4-8 mg/L to avoid CNS side effects
Toxicities
11-15 mg/L: somnolence, nystagmus, ataxia
15-25 mg/L: combativeness, hallucination, chorea
> 25 mg/L: seizures and coma
Which organs are affected by side effects of carbamazepine?
Blood: dyscrasias: aplastic anemia, anemia, thrombocytopenia, leukopenia, agranulocytosis, pancytopenia
liver: hepatoxic monitor liver, LFT before use
GI: N/V, anorexia, anticholinergic: xerostomia
heart: bradycardia in the elderly, pt over 50 should have an ECG before use
Dermatologic side effects
-antiepileptic drug (AED) hypersensitivity syndrome (skin) -> contraindicated with other aromatic anticonvulsants causing this reaction
-CBZ-induced SJS syndrome and toxic epidermal necrolysis (TENS): risk is 10x higher in asians
CBZ-induced SIADH
-Syndrome of inappropriate antidiuretic hormone
-signs: thirst, N/V, depression, confusion, lethargy, seizures
(-pt with acute depression or seizures should check their sodium levels)
What is the metabolite of CBZ?
-Carbamezaine 10,11 epoxide (CBZE)
-antiepileptic but also neurotoxic
-50% protein bound
What is the ratio between CBZ and CBZE
-in patients not receiving any other CYP450 inducing drugs: CBZE to CBZ = 0.1 - 0.25
-in patients receiving CYP450 inducers:
CBZE to CBZ = 0.25 - 0.5
numbers are higher in those with CYP inducers -> bc more CBZE is produced (nominator)
-pt with CBZ toxicity may have normal CBZ levels -> CHECK CBZE levels
eg: CBZE: 3 mg/L and CBZ: 10 mg/L; 3/10 = 0.3
CBZ is therapeutic but CBZE is not
What is the bioavailability of carbamazepine?
F = 0.8
Extended-release tablet: 0.71
(Vd = 1.4 L/kg - intermediate water-solubility )
eg: Gentamicin is very water-soluble and not very well distributed: Vd = 0.3L/kg
Propofol: >10L/kg -> very well distributed, fat-soluble
How much of CBZ is protein-bound?
-70-80%
-caution: when administered with a highly protein-bound drug it may kick off CBZ from albumin and the free serum concentration increases -> TOXICITY
What is the half-life of CBZ
-long: 25-30h
What is a unique pharmacokinetic characteristic of CBZ?
-Auto-induced metabolism
-half-life goes from 25-30h to 6-8h
-only in a naive patient (patients on other CYP inducer will not have auto-induced metabolism
-the metabolism increases with time -> increase the dose over a month
-start slow and low
How is CBZ metabolized
by CYP3A4 -> CBZ to CBZE (Carbamezapine 10,11 epoxide)
-CYP450 inhibitor will increase CBZ concentration
-CYP3A4 inducer will decrease CBZ concentration
What is the clearance of CBZ?
Monotherapy: 0.064 L/kg/hr
(polytherapy: 0.1 L/kg/hr) with other drugs: like phenytoin, phenobarbital (CYP inducers)
CYP3A4 inhibitors
-Macrolides: erythromycin, clarithromycin, troleandomycin
-Antiarrythmics: Amiodarone, Dronedarone
-Non-DHP-CCB: Diltiazem, Verapamil
-Azoles: Flucanozole, Ketocanozole, Itracanozole, Voriconazole
-Grape juice
CYP3A4 inducers
Universal (3A4, 1A2, 2C9, 2C19)
-Carbamezepine
-Phenytoin
-Phenobarbital
-Primidone
-Rifampin/Rifabutin
-St. John’s wort
Specific inducers (3A4)
-Dexamethasone (corticosteroid)
-Nerivapine (NNRTI for HIV)
