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Perphenazine
drug data and news
Perphenazine drug data, resources, and news articles (when available). Onconews.org provides news on cancer research. This section, which includes profiles on medicines that may or not be cancer-related is in beta form. If things run smoothly we will be releasing a new format late in the summer of 2006.
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| Generic name | Perphenazine | ||
| Brand Names/Synonyms | Apo-Perphenazine; Chlorperphenazine; Decentan; Emesinal; Etaperazin; Etaperazine; Ethaperazine; Etrafon-A; Etrafon-Forte; F-Mon; Fentazin; Fluphenazine; PZC; Perfenazina; Perfenazine; Perphenan; Perphenazin; Perphenazine; Perphenazine and Amitriptyline Hcl; Pms Perphenazine; Sch 3940; Thilatazin; Tranquisan; Trifaron; Trilafon; Trilafon Concentrate; Trilifan; Triphenot | ||
| Indication | For the treatment of schizophrenia, nusea, vomiting | ||
| Sponsored links | Description | Not Available | |
| Pharmacology | Perphenazine is a piperazinyl phenothiazine indicated for the treatment of patients with moderate to severe anxiety and/or agitation and depressed mood; patients with depression in whom anxiety and/or agitation are moderate or severe; patients with anxiety and depression associated with chronic physical disease; patients in whom depression and anxiety cannot be clearly differentiated. Perphenazine is also used to treat schizophrenia and symptoms such as hallucinations, delusions, and hostility. It can also be used to treat nausea and vomiting. Perphenazine acts on the central nervous system, and has a greater behavioral potency than other phenothiazine derivatives whose side chains do not contain a piperazine moiety. It is a member of a class of drugs called phenthiazines, which are dopamine D1/D2 receptor antagonists. | ||
| Mechanism Of Action | Binds to the dopamine D1 and dopamine D2 receptors and inhibits their activity. The mechanism of the anti-emetic effect is due predominantly to blockage of the dopamine D2 neurotransmitter receptors in the chemoreceptor trigger zone and vomiting centre. Perphenazine also binds the alpha andrenergic receptor. This receptor's action is mediated by association with G proteins that activate a phosphatidylinositol-calcium second messenger system. | ||
| Perphenazine News (When available) |
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| Dosage Forms | LIQUID; SOLUTION; SYRUP; TABLET | ||
| Drug_Category | Antipsychotics; Phenothiazines; Dopamine Antagonists; ATC:N05AB03 | ||
| Absorption | Not Available | ||
| Interactions |
Interactions for Perphenazine: Metabolism of a number of medications, including antipsychotics, antidepressants, b- blockers, and antiarrhythmics, occurs through the cytochrome P450 2D6 isoenzyme (debrisoquine hydroxylase). Approximately 10% of the Caucasian population has reduced activity of this enzyme, so-called poorî metabolizers. Among other populations the prevalence is not known. Poor metabolizers demonstrate higher plasma concentrations of antipsychotic drugs at usual doses, which may correlate with emergence of side effects. In one study of 45 elderly patients suffering from dementia treated with perphenazine, the 5 patients who were prospectively identified as poor P450 2D6 metabolizers had reported significantly greater side effects during the first 10 days of treatment than the 40 extensive metabolizers, following which the groups tended to converge. Prospective phenotyping of elderly patients prior to antipsychotic treatment may identify those at risk for adverse events. The concomitant administration of other drugs that inhibit the activity of P450 2D6 may acutely increase plasma concentrations of antipsychotics. Among these are tricyclic antidepressants and selective serotonin reuptake inhibitors, e.g.fluoxetine, sertraline and paroxetine. When prescribing these drugs to patients already receiving antipsychotic therapy, close monitoring is essential and dose reduction may become necessary to avoid toxicity. Lower doses than usually prescribed for either the antipsychotic or the other drug may be required. | ||
| Toxicity | Oral LD50:318 mg/kg (rat); IPR LD50:64 mg/kg (mouse) | ||
| Organisms Affected | Humans and other mammals | ||
| Chemical IUPAC Name | 2-[4-[3-(2-chloro-10H-phenothiazin-10-yl)propyl]piperazin-1-yl]ethanol | ||
| Chemical Formula | C21H26ClN3OS | ||
| Molecular Weight | 403.969 g/mol | ||
| Smiles String | C1CN(CCN1CCCN2C3=CC=CC=C3SC4=C2C=C(C=C4)Cl)CCO | ||
| Melting Point | 97 °C | ||
| Water Solubility | 28.3 mg/L | ||
| State | Solid | ||
| LogP/Hphobicity | 4.176 | ||
| Isoelectric Point | 7.94 | ||
| Biotransformation | Not Available | ||
| Half Life | Not Available | ||
| Protein Binding [%] | Not Available | ||
| RxList Link | RXlist | ||
| Sponsored links | |||
| Drug Reference |
http://www.pdrhealth.com/drug_info/rxdrugprofiles/drugs/tri1616.shtml http://www.drugs.com/cons/Perphenazine.html http://www.rxlist.com/cgi/generic2/etrafon.htm | ||
| Drug Type | Approved Drug | ||
| Accession No | APRD00429 | ||
| CAS Registry Number | 58-39-9 | ||
| KEGG Compound ID | C07427 | ||
| PubChem ID | SID:148869 | ||
| PharmGKB ID | PA450882 | ||
| SwissProt ID | Not Available | ||
| GenBank ID | Not Available | ||
| Drug ID Number [DIN] | 726184 |
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