| Structure/Class |
- SSRIs – examples are fluoxetine, citalopram and escitalopram
|
| Pharmacodynamics |
- Mainly bind to SERT.
- Minimal histaminergic, adrenergic or muscarinic blockade.
|
| Absorption/administration |
- PO
|
| Distribution |
- Very lipophilic drug
- Strongly protein bound and large Vd: 20-45L/kg à non-dialysable toxin.
|
| Metabolism |
- Hepatic mainly
- Note that fluoxetine is metabolized to norfluoxetine, its active metabolite. Norfluoxetine’s T ½ is 3x that of fluoxetine and therefore fluoxetine has the longest half-life of all SSRIs.
- This is important because fluoxetine must be stopped at least 4 weeks before commencing a MAO-I.
- Fluoxetine, paroxetine and fluvoxamine are all strong inhibitors of CYP systems.
- Citalopram, escitalopram and sertraline are more modest.
|
| Excretion |
- Urinary
|
| Indications |
- Depressive disorders
- Anxiety disorders, including OCD.
|
| Contraindications |
- Concurrent use of MAO-I is an absolute contraindication
|
| Special precautions |
|
| Interactions |
- MAO-I
- TCA and Calcium channel blockers have increased activity due to enzyme inhibition by fluoxetine.
|
| Adverse events |
- Due to too much serotonin in the CNS
- Nausea/vomiting/diarrhea
- Reduced libido
- Headache and insomnia
- Weight gain
- Discontinuation syndrome (dizziness, paraesthesia)
|
| Dosing/administration |
|
| Toxicology |
- Use activated charcoal
- BZD may be useful for seizures
|
| Withdrawal syndrome |
|
| Special notes |
|
