Peringatan Keamanan

LD₅₀ and Overdose

Oral LD₅₀ in rats is 750 mg/kg. Intraperitoneal and subcutaneous LD₅₀ in mice are 191 mg/kg and 320 mg/kg, respectively.MSDS In placebo-controlled trials, there were increased incidences of mortality in elderly patients with dementia-related psychosis receiving antipsychotic medications. The risk of death in drug-treated patients was about 1.6 to 1.7 times that of placebo-treated patients. Deaths were largely resulting from cardiovascular, such as heart failure and sudden death, or infectious, such as pneumonia, conditions.label Due to its antagonist action on dopamine receptors, prochlorperazine is associated with a risk for developing extrapyramidal symptoms such as tardive dyskinesia, which is a syndrome consisting of potentially irreversible, involuntary, dyskinetic movements. This risk is also conferred on other antipsychotic agents that block dopamine receptors. It is proposed that increased duration of the drug treatment is likely thus increased total cumulative dose of antipsychotic drugs administered to the patient leads to increased risk for developing the syndrome and the likelihood that it will become irreversible. As with other antipsychotic agents, prochlorperazine is associated with a risk for causing neuroleptic malignant syndrome (NMS), which is a potentially fatal symptom complex, which is manifested as hyperpyrexia, muscle rigidity, altered mental status and evidence of autonomic instability.

There is no known antidote for prochlorperazine thus overdose treatment should be supportive and symptomatic. Overdose of prochlorperazine may produce dystonic reactions that involve extrapyramidal mechanism. To reduce these symptoms, antiparkinsonism drugs, barbiturates, or diphenhydramine may be used. Symptoms of central nervous system depression, such as somnolence or coma, may also be observed. Amphetamine, destroamphetamine, or caffeine and sodium benzoate may be used to induce stimulatory effects. In contrast, agitation and restlessness may also be seen in case of overdose. Other possible manifestations include convulsions, EKG changes and cardiac arrhythmias, fever, and autonomic reactions such as hypotension, dry mouth and ileus. Hypotension can be responded with the standard measures for managing circulatory shock.label

Nonclinical Toxicology

In a rat developmental or reproductive toxicity study, abnormalities in both the reproductive measures and neurobehavioral testing were observed following administration of 25 mg/kg of prochlorperazine.^L6649

Use in specific populations

As the use of antipsychotic agents during the third trimester of pregnancy is associated with a risk for extrapyramidal and/or withdrawal symptoms following delivery, the use of prochlorperazine in pregnant patients is generally not recommended and it should be limited after careful consideration of the potential benefit of drug therapy justifying the potential risk to the fetus. Caution should be exercised when prochlorperazine is administered to a nursing mother. While lower doses of prochlorperazine is reported to be safe for elderly patients, caution is still advised, especially those with higher susceptibility to hypotension and neuromuscular reactions.label

Prochlorperazine

DB00433

small molecule approved vet_approved

Deskripsi

Prochlorperazine, also known as compazine, is a piperazine phenothiazine and first-generation antipsychotic drug that is used for the treatment of severe nausea and vomiting, as well as short-term management of psychotic disorders such as generalized non-psychotic anxiety and schizophrenia.label It mainly works by depressing the chemoreceptor trigger zone and blocking D2 dopamine receptors in the brain. It was shown to also block histaminergic, cholinergic and noradrenergic receptors.^L6637 Prochlorperazine was first developed in the 1950s ^L6643 and was first approved by the FDA in 1956. Although newer antiemetic agents such as 5-HT3 antagonists are more heavily promoted, prochlorperazine is still widely used in nausea and vomiting.^L6640

Struktur Molekul 2D

Berat 373.943

Wujud solid

Peta Jejaring Molekuler

Obat Target Gen Interaksi Enzim Transporter Carrier

Legenda: Obat • Target • Gen • Enzim • (Panah → menunjukkan arah efek / relasi) • Transporter • Carrier

1. Pendahuluan & Konsep

Fitur visualisasi ini dikembangkan menggunakan pendekatan Graph Theory untuk memetakan hubungan polifarmasi dan molekuler. Entitas (Obat, Target, Gen) direpresentasikan sebagai Simpul (Nodes), sedangkan hubungan biologisnya sebagai Sisi (Edges).

2. Sumber Data (Validasi)

Data Obat: Diekstraksi dari elemen drugbank-id dan name pada skema XML DrugBank.
Target Protein: Diambil dari elemen targets/target yang memuat polipeptida sasaran.
Genetik: Disinkronisasi dari sub-elemen gene-name dan varian snp-effects.
Genetik: Jumlah titik node dibatasi pada maksimal 10 (Slice=10) interaksi untuk menghindari tumpukan data.

3. Algoritma Visualisasi

Tata letak grafik menggunakan algoritma Force-Directed Graph (Barnes-Hut). Model fisika ini menerapkan gaya tolak-menolak antar simpul (Gravitasi: -3000) agar tidak tumpang tindih, serta gaya pegas (Spring: 0.04) pada garis penghubung untuk fleksibilitas interaksi.

4. Legenda Visual

Obat Utama (Pusat Analisis)

Target Protein (Mekanisme)

Gen (Faktor Genetik)

Metode ini mendukung analisis Precision Medicine dan evaluasi risiko Drug-Drug Interaction (DDI).

Profil Farmakokinetik

Waktu Paruh (Half-Life) Following intravenous and single oral dose administration, the terminal elimination half live were 9 and 8 hours, respectively.[A179173]

Volume Distribusi In a preliminary pharmacokinetic study involving healthy volunteers, the mean apparent volume of distribution following intravenous administration of 6.25 mg and 12.5 mg prochlorperazine were approximately 1401 L and 1548 L, respectively.[A179185] Prochlorperazine is reported to be distributed to most body tissues with high concentrations being distributed into liver and spleen.[L6646] There is evidence that phenothiazines are excreted in the breast milk of nursing mothers.[label]

Klirens (Clearance) The mean plasma clearance (CL) of prochlorperazine following intravenous administration in healthy volunteers was approximately 0.98L/h x kg. The mean renal clearance was about 23.6 mL/h.[A179173]

Absorpsi

Following oral administration, prochlorperazine is reported to be well absorbed from the gastrointestinal tract. The onset of pharmacological action is about 30 to 40 minutes following oral administration and 10 to 20 minutes following intramuscular administration. The duration of action for all routes is about 3 to 4 hours.^L6646 Following oral administration in healthy volunteers, the mean oral bioavailability was about 12.5%. In these patients, the time to reach the peak plasma concentrations was about 5 hours. Repeated oral dosing resulted in an accumulation of prochlorperazine and its metabolite. Following multiple twice daily dosing, the steady state of prochlorperazine was reached by 7 days.^A179173

Metabolisme

Prochlorperazine undergoes hepatic metabolism involving oxidation, hydroxylation, demethylation, sulfoxide formation and conjugation with glucuronic acid.^L6649 The oxidation reaction is mediated by CYP2D6.^A179179 N-desmethyl prochlorperazine was detected in the plasma^A179173, as well as prochlorperazine sulfoxide, prochlorperazine 7-hydroxide and prochlorperazine sulfoxide 4'-N-oxide, following oral and buccal administration.^A179188 Prochlorperazine may enter the enterohepatic circulation.^L6646

Rute Eliminasi

Prochlorperazine is reported to be mainly excreted via the feces and bile.^L6646 Low quantities of unchanged prochlorperazine and its metabolite were detectable in the urine.^A179173

Interaksi Makanan

1 Data

1. Avoid alcohol. The drug may intensify or prolong the action of central nervous system depressants.

Interaksi Obat

1269 Data

Ivabradine	Ivabradine may increase the QTc-prolonging activities of Prochlorperazine.
Buprenorphine	Prochlorperazine may increase the central nervous system depressant (CNS depressant) activities of Buprenorphine.
Doxylamine	Doxylamine may increase the central nervous system depressant (CNS depressant) activities of Prochlorperazine.
Dronabinol	Dronabinol may increase the central nervous system depressant (CNS depressant) activities of Prochlorperazine.
Droperidol	Droperidol may increase the central nervous system depressant (CNS depressant) activities of Prochlorperazine.
Hydrocodone	Prochlorperazine may increase the central nervous system depressant (CNS depressant) activities of Hydrocodone.
Magnesium sulfate	The therapeutic efficacy of Prochlorperazine can be increased when used in combination with Magnesium sulfate.
Methotrimeprazine	Prochlorperazine may increase the central nervous system depressant (CNS depressant) activities of Methotrimeprazine.
Minocycline	Minocycline may increase the central nervous system depressant (CNS depressant) activities of Prochlorperazine.
Mirtazapine	Prochlorperazine may increase the central nervous system depressant (CNS depressant) activities of Mirtazapine.
Nabilone	Nabilone may increase the central nervous system depressant (CNS depressant) activities of Prochlorperazine.
Orphenadrine	Prochlorperazine may increase the central nervous system depressant (CNS depressant) activities of Orphenadrine.
Paraldehyde	Prochlorperazine may increase the central nervous system depressant (CNS depressant) activities of Paraldehyde.
Perampanel	Perampanel may increase the central nervous system depressant (CNS depressant) activities of Prochlorperazine.
Rotigotine	Prochlorperazine may increase the sedative activities of Rotigotine.
Rufinamide	The risk or severity of adverse effects can be increased when Rufinamide is combined with Prochlorperazine.
Sodium oxybate	Prochlorperazine may increase the central nervous system depressant (CNS depressant) activities of Sodium oxybate.
Suvorexant	Prochlorperazine may increase the central nervous system depressant (CNS depressant) activities of Suvorexant.
Tapentadol	Tapentadol may increase the central nervous system depressant (CNS depressant) activities of Prochlorperazine.
Thalidomide	Prochlorperazine may increase the central nervous system depressant (CNS depressant) activities of Thalidomide.
Zolpidem	Prochlorperazine may increase the central nervous system depressant (CNS depressant) activities of Zolpidem.
Dofetilide	Prochlorperazine may decrease the excretion rate of Dofetilide which could result in a higher serum level.
Amisulpride	Prochlorperazine may increase the antipsychotic activities of Amisulpride.
Methylphenidate	The risk or severity of adverse effects can be increased when Prochlorperazine is combined with Methylphenidate.
Dexmethylphenidate	The risk or severity of adverse effects can be increased when Prochlorperazine is combined with Dexmethylphenidate.
Metoclopramide	The risk or severity of adverse effects can be increased when Metoclopramide is combined with Prochlorperazine.
Quinagolide	The therapeutic efficacy of Quinagolide can be decreased when used in combination with Prochlorperazine.
Sulpiride	Prochlorperazine may increase the antipsychotic activities of Sulpiride.
Methadone	The risk or severity of adverse effects can be increased when Methadone is combined with Prochlorperazine.
Lithium citrate	Lithium citrate may increase the neurotoxic activities of Prochlorperazine.
Lithium hydroxide	Lithium hydroxide may increase the neurotoxic activities of Prochlorperazine.
Mequitazine	Prochlorperazine may increase the arrhythmogenic activities of Mequitazine.
Thiopental	The risk or severity of adverse effects can be increased when Prochlorperazine is combined with Thiopental.
Deferoxamine	The risk or severity of adverse effects can be increased when Deferoxamine is combined with Prochlorperazine.
Metyrosine	The risk or severity of extrapyramidal symptoms and CNS depression can be increased when Metyrosine is combined with Prochlorperazine.
Mirabegron	The serum concentration of Prochlorperazine can be increased when it is combined with Mirabegron.
Ethanol	Prochlorperazine may increase the central nervous system depressant (CNS depressant) activities of Ethanol.
Azelastine	Prochlorperazine may increase the central nervous system depressant (CNS depressant) activities of Azelastine.
Brimonidine	Brimonidine may increase the central nervous system depressant (CNS depressant) activities of Prochlorperazine.
Zimelidine	The risk or severity of adverse effects can be increased when Prochlorperazine is combined with Zimelidine.
Dapoxetine	The risk or severity of adverse effects can be increased when Prochlorperazine is combined with Dapoxetine.
Seproxetine	The risk or severity of adverse effects can be increased when Prochlorperazine is combined with Seproxetine.
Sertraline	The risk or severity of adverse effects can be increased when Prochlorperazine is combined with Sertraline.
Sibutramine	The risk or severity of adverse effects can be increased when Prochlorperazine is combined with Sibutramine.
Milnacipran	The risk or severity of adverse effects can be increased when Prochlorperazine is combined with Milnacipran.
Desvenlafaxine	The serum concentration of Prochlorperazine can be increased when it is combined with Desvenlafaxine.
Levomilnacipran	The risk or severity of adverse effects can be increased when Levomilnacipran is combined with Prochlorperazine.
Indalpine	The risk or severity of adverse effects can be increased when Prochlorperazine is combined with Indalpine.
Alaproclate	The risk or severity of adverse effects can be increased when Prochlorperazine is combined with Alaproclate.
Esmolol	The serum concentration of Esmolol can be increased when it is combined with Prochlorperazine.
Betaxolol	The serum concentration of Betaxolol can be increased when it is combined with Prochlorperazine.
Atenolol	The serum concentration of Atenolol can be increased when it is combined with Prochlorperazine.
Timolol	The serum concentration of Timolol can be increased when it is combined with Prochlorperazine.
Propranolol	The serum concentration of Propranolol can be increased when it is combined with Prochlorperazine.
Labetalol	The serum concentration of Labetalol can be increased when it is combined with Prochlorperazine.
Bisoprolol	The serum concentration of Bisoprolol can be increased when it is combined with Prochlorperazine.
Alprenolol	The serum concentration of Alprenolol can be increased when it is combined with Prochlorperazine.
Pindolol	The serum concentration of Pindolol can be increased when it is combined with Prochlorperazine.
Carvedilol	The serum concentration of Carvedilol can be increased when it is combined with Prochlorperazine.
Acebutolol	The serum concentration of Acebutolol can be increased when it is combined with Prochlorperazine.
Nadolol	The serum concentration of Nadolol can be increased when it is combined with Prochlorperazine.
Bevantolol	The serum concentration of Bevantolol can be increased when it is combined with Prochlorperazine.
Practolol	The serum concentration of Practolol can be increased when it is combined with Prochlorperazine.
Penbutolol	The serum concentration of Penbutolol can be increased when it is combined with Prochlorperazine.
Oxprenolol	The serum concentration of Oxprenolol can be increased when it is combined with Prochlorperazine.
Dexpropranolol	The serum concentration of Dexpropranolol can be increased when it is combined with Prochlorperazine.
Celiprolol	The serum concentration of Celiprolol can be increased when it is combined with Prochlorperazine.
Nebivolol	The serum concentration of Nebivolol can be increased when it is combined with Prochlorperazine.
Bufuralol	The serum concentration of Bufuralol can be increased when it is combined with Prochlorperazine.
Bopindolol	The serum concentration of Bopindolol can be increased when it is combined with Prochlorperazine.
Bupranolol	The serum concentration of Bupranolol can be increased when it is combined with Prochlorperazine.
Indenolol	The serum concentration of Indenolol can be increased when it is combined with Prochlorperazine.
Arotinolol	The serum concentration of Arotinolol can be increased when it is combined with Prochlorperazine.
Levobetaxolol	The serum concentration of Levobetaxolol can be increased when it is combined with Prochlorperazine.
Talinolol	The serum concentration of Talinolol can be increased when it is combined with Prochlorperazine.
Anisodamine	The serum concentration of Anisodamine can be increased when it is combined with Prochlorperazine.
Bucindolol	The serum concentration of Bucindolol can be increased when it is combined with Prochlorperazine.
Esatenolol	The serum concentration of Esatenolol can be increased when it is combined with Prochlorperazine.
Cloranolol	The serum concentration of Cloranolol can be increased when it is combined with Prochlorperazine.
Mepindolol	The serum concentration of Mepindolol can be increased when it is combined with Prochlorperazine.
Epanolol	The serum concentration of Epanolol can be increased when it is combined with Prochlorperazine.
Tertatolol	The serum concentration of Tertatolol can be increased when it is combined with Prochlorperazine.
Landiolol	The serum concentration of Landiolol can be increased when it is combined with Prochlorperazine.
Morphine	The risk or severity of hypotension and CNS depression can be increased when Prochlorperazine is combined with Morphine.
Codeine	The risk or severity of hypotension and CNS depression can be increased when Prochlorperazine is combined with Codeine.
Hydromorphone	The risk or severity of hypotension and CNS depression can be increased when Prochlorperazine is combined with Hydromorphone.
Oxycodone	The risk or severity of hypotension and CNS depression can be increased when Prochlorperazine is combined with Oxycodone.
Butorphanol	The risk or severity of hypotension and CNS depression can be increased when Prochlorperazine is combined with Butorphanol.
Dextropropoxyphene	The risk or severity of hypotension and CNS depression can be increased when Prochlorperazine is combined with Dextropropoxyphene.
Pentazocine	The risk or severity of hypotension and CNS depression can be increased when Prochlorperazine is combined with Pentazocine.
Naltrexone	The risk or severity of hypotension and CNS depression can be increased when Prochlorperazine is combined with Naltrexone.
Sufentanil	The risk or severity of hypotension and CNS depression can be increased when Prochlorperazine is combined with Sufentanil.
Nalbuphine	The risk or severity of hypotension and CNS depression can be increased when Prochlorperazine is combined with Nalbuphine.
Levorphanol	The risk or severity of hypotension and CNS depression can be increased when Prochlorperazine is combined with Levorphanol.
Remifentanil	The risk or severity of hypotension and CNS depression can be increased when Prochlorperazine is combined with Remifentanil.
Diphenoxylate	The risk or severity of hypotension and CNS depression can be increased when Prochlorperazine is combined with Diphenoxylate.
Oxymorphone	The risk or severity of hypotension and CNS depression can be increased when Prochlorperazine is combined with Oxymorphone.
Dezocine	The risk or severity of hypotension and CNS depression can be increased when Prochlorperazine is combined with Dezocine.
Methadyl acetate	The risk or severity of hypotension and CNS depression can be increased when Prochlorperazine is combined with Methadyl acetate.
Dihydroetorphine	The risk or severity of hypotension and CNS depression can be increased when Prochlorperazine is combined with Dihydroetorphine.

Target Protein

D(2) dopamine receptor DRD2

Histamine H1 receptor HRH1

Alpha-1 adrenergic receptors ADRA1A

Alpha-2 adrenergic receptors ADRA2A

Referensi & Sumber

Artikel (PubMed)

PMID: 1768559
Isah AO, Rawlins MD, Bateman DN: Clinical pharmacology of prochlorperazine in healthy young males. Br J Clin Pharmacol. 1991 Dec;32(6):677-84.
PMID: 1553856
Isah AO, Rawlins MD, Bateman DN: The pharmacokinetics and effects of prochlorperazine in elderly female volunteers. Age Ageing. 1992 Jan;21(1):27-31. doi: 10.1093/ageing/21.1.27.
PMID: 21365391
Perwitasari DA, Gelderblom H, Atthobari J, Mustofa M, Dwiprahasto I, Nortier JW, Guchelaar HJ: Anti-emetic drugs in oncology: pharmacology and individualization by pharmacogenetics. Int J Clin Pharm. 2011 Feb;33(1):33-43. doi: 10.1007/s11096-010-9454-1. Epub 2011 Jan 28.
PMID: 3828192
Taylor WB, Bateman DN: Preliminary studies of the pharmacokinetics and pharmacodynamics of prochlorperazine in healthy volunteers. Br J Clin Pharmacol. 1987 Feb;23(2):137-42. doi: 10.1111/j.1365-2125.1987.tb03021.x.
PMID: 16291713
Finn A, Collins J, Voyksner R, Lindley C: Bioavailability and metabolism of prochlorperazine administered via the buccal and oral delivery route. J Clin Pharmacol. 2005 Dec;45(12):1383-90. doi: 10.1177/0091270005281044.
PMID: 18556493
O'Brien C: Nausea and vomiting. Can Fam Physician. 2008 Jun;54(6):861-3.

Link

Contoh Produk & Brand

Produk: 200 • International brands: 4

Produk

Compazine

Tablet, coated • 5 mg/1 • Oral • US • Approved
Compazine

Suppository • 25 mg/1 • Rectal • US • Approved
Compazine

Suppository • 25 mg/1 • Rectal • US • Generic • Approved
Compazine

Tablet, coated • 5 mg/1 • Oral • US • Approved
Compazine

Tablet, coated • 10 mg/1 • Oral • US • Approved
Compazine

Tablet, film coated • 5 mg/1 • Oral • US • Generic • Approved
Compazine

Tablet, film coated • 10 mg/1 • Oral • US • Generic • Approved
Compazine

Capsule, extended release • 10 mg/1 • Oral • US • Approved

Menampilkan 8 dari 200 produk.

International Brands

Buccastem — Reckitt Benckiser
Emetiral — Zentiva
Stemzine — Sanofi-Aventis
Volimin — Chin Teng

Sekuens Gen/Protein (FASTA)

Sekuens dimuat saat dibutuhkan agar halaman tetap ringan.