| Structure/Class |
- Examples of MAO-I: moclobemide, isocarboxacid
|
| Pharmacodynamics |
- Binds to MAO-A and MAO-B
- This increases the levels of noradrenaline, adrenaline and serotonin at the CNS synapse, by reducing their metabolism.
- It also reduces the metabolism of tyramine (tyramine is important because it acts as a catecholamine releasing agent)
- MAO-Is also resemble amphetamine and therefore may have CNS stimulating effects.
|
| Absorption/administration |
- PO
|
| Distribution |
|
| Metabolism |
- Extensive first pass effect
- Low bioavailability
|
| Excretion |
|
| Indications |
|
| Contraindications |
- Concurrent use of TCA and SSRI are absolute contra-indications.
|
| Special precautions |
|
| Interactions |
- SSRI/TCA
- Life-threatening serotonin syndrome. Note that fluoxetine must be ceased 4 weeks prior to commencing a MAO-I and MAO-I must be ceased 2 weeks prior to commencing SSRI.
- Sympathomimetics
- Overall increased activity, e.g. ephedrine in over the counter cold preparations.
- Foods rich in tyramine
- Cheese, soy products, certain sausages (may get malignant hypertension)
|
| Adverse events |
- Weight gain (serotonergic effect) and orthostatic hypotension
- Amphetamine like effects – activation, insomnia and restlessness
- Discontinuation syndrome may occur – psychosis, excitement
|
| Dosing/administration |
|
| Toxicology |
- MAO-I overdose leads to increased adrenergic and serotonergic activity
- Autonomic instability
- Psychosis
- Confusion, delirium
Treatment is with cardiac monitoring and good supportive care. |
| Withdrawal syndrome |
|
| Special notes |
|
