| Structure/Class |
- Similar to TCA/Imipramine
|
| Pharmacodynamics |
- Similar to phenytoin
- Na+ channel blockade. Inhibits repetitive high frequency neuronal firing.
- Also may potentiate K+ channel, causing hyperpolarization.
|
| Absorption/administration |
- PO
- Peak levels occur at 6 hours
|
| Distribution |
- Distributes slowly.
- Vd = 1L/kg,
- It is 70% bound to plasma proteins but there is no displacement of other drugs.
|
| Metabolism |
- Completely metabolized hepatically to carbamazepine 10,11 epoxide (it has anti-convulsant activity)
- Strong inducer of hepatic enzymes. May induce its own metabolism and may require frequent dose changes in the first few weeks of treatment.
|
| Excretion |
- Renal
|
| Indications |
- GTCS
- Trigeminal neuralgia
- Mania
|
| Contraindications |
|
| Special precautions |
|
| Interactions |
- Strong enzyme inducer and may also induce its own metabolism.
- Other inducers, e.g. phenytoin/phenobarbital may decrease its level.
- Other inhibitors (e.g. valproate) may increase its levels.
|
| Adverse events |
- Side effects as follows:
- CNS (most common) – diplopia and ataxia. Mild drowsiness.
- GIT upset
- Idiosyncratic à blood dyscrasias and aplastic anaemia.
- Rash
|
| Dosing/administration |
|
| Toxicology |
|
| Withdrawal syndrome |
|
| Special notes |
|
