Indication |
For the treatment or relief of nausea and vomiting. |
Pharmacodynamics |
Thiethylperazine, an atypical antipsychotic agent, is used to
treat both negative and positive symptoms of schizophrenia, acute mania
with bipolar disorder, agitation, and psychotic symptoms in dementia.
Future uses may include the treatment of obsessive-compulsive disorder
and severe behavioral disorders in autism. Structurally and
pharmacologically similar to clozapine, Thiethylperazine binds to
alpha(1), dopamine, histamine H1, muscarinic, and serotonin type 2
(5-HT2) receptors. |
Mechanism of action |
Thiethylperazine is an antagonist at types 1, 2, and 4 dopamine
receptors, 5-HT receptor types 2A and 2C, muscarinic receptors 1 through
5, alpha(1)-receptors, and histamine H1-receptors. Thiethylperazine's
antipsychotic effect is due to antagonism at dopamine and serotonin type
2 receptors, with greater activity at serotonin 5-HT2 receptors than at
dopamine type-2 receptors. This may explain the lack of extrapyramidal
effects. Thiethylperazine does not appear to block dopamine within the
tubero-infundibular tract, explaining the lower incidence of
hyperprolactinemia than with typical antipsychotic agents or
risperidone. Antagonism at muscarinic receptors, H1-receptors, and
alpha(1)-receptors also occurs with thiethylperazine. |
Absorption |
Not Available |
Volume of distribution |
Not Available |
Protein binding |
60% |
Metabolism |
Not Available |
Route of elimination |
Thiethylperazine is eliminated in the urine. |
Half life |
Not Available |
Clearance |
Not Available |
Toxicity |
Manifestations of acute overdosage of TORECAN (thiethylperazine)
can be expected to reflect the CNS effects of the drug and include
extrapyramidal symptoms (E.P.S), confusion and convulsions with reduced
or absent reflexes, respiratory depression and hypotension. |
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