| Structure/class |
- Typical anti-psychotic of the Butyrophenone class.
|
| Pharmacodynamics |
- D2 receptor antagonist.
- Also has α-blockade, serotonergic blockade, histaminergic blockade and muscarinic blockade (see previous page for side effect details)
- Haloperidol has the highest chance of causing extra-pyramidal SES.
|
| Administration |
- PO, IM, IV
|
| Distribution |
- Readily (but incompletely) absorbed
- Highly lipid soluble, strong protein binding and large Vd – means that it has a longer clinical duration of action than can be predicted from T ½
|
| Metabolism |
- Hepatic. Note that haloperidol has the least first-pass metabolism with bioavailability 65%.
|
| Excretion |
- Urine
|
| Indications |
- Psychosis
- Mania
- Agitation/Tourette
- Droperidol (a butyrophenone) is used together with fentanyl as neurolepanaesthesia.
|
| Contraindications |
|
| Special precautions |
- Elderly – oversedation
- Liver disease
- CVS disease
|
| Interactions |
- Haloperidol may potentiate the effects of other CNS depressants, especially if used in conjunction with benzodiazepines
- Reduced effect of Levodopa
- Worsens Parkinson’s disease
|
| Adverse events |
- As with previous page
|
| Dosing/administration |
|
| Toxicology |
|
| Withdrawal syndrome |
|
| Special notes |
|
