Peringatan Keamanan

Acute oral toxicity (LD50): 71 mg/kg in rats MSDS.

Haloperidol

DB00502

small molecule approved

Deskripsi

Haloperidol is a high potency first-generation (typical) antipsychotic and one of the most frequently used antipsychotic medications used worldwide.^A180616 While haloperidol has demonstrated pharmacologic activity at a number of receptors in the brain,^A27477 it exerts its antipsychotic effect through its strong antagonism of the dopamine receptor (mainly D2), particularly within the mesolimbic and mesocortical systems of the brain. Haloperidol is indicated for the treatment of the manifestations of several psychotic disorders including schizophrenia, acute psychosis, Tourette syndrome, and other severe behavioural states.^F4645 It is also used off-label for the management of chorea associated with Huntington's disease and for the treatment of intractable hiccups as it is a potent antiemetic. Dopamine-antagonizing medications such as haloperidol are though to improve psychotic symptoms and states that are caused by an over-production of dopamine, such as schizophrenia, which is theorized to be caused by a hyperdopaminergic state within the limbic system of the brain.^A34360

Use of the first-generation antipsychotics (including haloperidol) is considered highly effective for the management of the "positive" symptoms of schizophrenia including hallucinations, hearing voices, aggression/hostility, disorganized speech, and psychomotor agitation. However, this class of drugs is also limited by the development of movement disorders induced by dopamine-blockade such as drug-induced parkinsonism, akathisia, dystonia, tardive dyskinesia, as well as other side effects including sedation, weight gain, and prolactin changes. While there are limited high-quality studies comparing haloperidol to lower-potency first-generation antipsychotics such as DB00477, DB01624, DB00623, and DB01403, haloperidol typically demonstrates the least amount of side effects within this class, but demonstrates a stronger disposition for causing extrapyramidal symptoms (EPS).A180613, A180616, A180625 These other low?potency antipsychotics are limited by their lower affinity for dopamine receptors, which requires a higher dose to effectively treat symptoms of schizophrenia. In addition, they block many receptors other than the primary target (dopamine receptors), such as cholinergic or histaminergic receptors, resulting in a higher incidence of side effects such as sedation, weight gain, and hypotension.

Interestingly, in vivo pharmacogenetic studies have demonstrated that the metabolism of haloperidol may be modulated by genetically determined polymorphic CYP2D6 activity. However, these findings contradict the findings from studies in vitro with human liver microsomes and from drug interaction studies in vivo. Inter-ethnic and pharmacogenetic differences in haloperidol metabolism may possibly explain these observations.^A32346

First-generation antipsychotic drugs have largely been replaced with second- and third-generation (atypical) antipsychotics such as DB00734, DB00334, DB00363, DB01224, DB01238, and DB00246. However, haloperidol use remains widespread and is considered the benchmark for comparison in trials of the newer generation antipsychotics.^A180625

The efficacy of haloperidol was first established in controlled trials in the 1960s.^A180610

Struktur Molekul 2D

Berat 375.864

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 oral administration, the half-life was found to be 14.5-36.7 hours. Following intramuscular injection, mean half-life was found to be 20.7 hours.[A32346]

Volume Distribusi The apparent volume of distribution was found to range from 9.5-21.7 L/kg.[A32346] This high volume of distribution is in accordance with its lipophilicity, which also suggests free movement through various tissues including the blood-brain barrier.

Klirens (Clearance) Following intravenous administration, the plasma or serum clearance (CL) was found to be 0.39-0.708 L/h/kg (6.5 to 11.8 ml/min/kg). Following oral administration, clearance was found to be 141.65 L/h (range 41.34 to 335.80 L/h).[A32346] Haloperidol clearance after extravascular administration ranges from 0.9-1.5 l/h/kg, however this rate is reduced in poor metabolizers of C_YP2D6_ enzyme. Reduced CYP2D6 enzyme activity may result in increased concentrations of haloperidol. The inter-subject variability (coefficient of variation, %) in haloperidol clearance was estimated to be 44% in a population pharmacokinetic analysis in patients with schizophrenia [L2028]. Genetic polymorphism of CYP2D6 has been demonstrated to be an important source of inter-patient variability in the pharmacokinetics of haloperidol and may affect therapeutic response and incidence of adverse effects.[A32346]

Absorpsi

Haloperidol is a highly lipophilic compound and is extensively metabolized in humans, which may cause a large interindividual variability in its pharmacokinetics.^A32346 Studies have found a wide variance in pharmacokinetic values for orally administered haloperidol with 1.7-6.1 hours reported for time to peak plasma concentration (tmax), 14.5-36.7 hours reported for half-life (t1?2), and 43.73 ?g/L•h range 14.89-120.96 ?g/L•h reported for AUC.^A32346 Haloperidol is well-absorbed from the gastrointestinal tract when ingested orally, however, the first-pass hepatic metabolism decreases its oral bioavailability to 40 - 75%. After intramuscular administration, the time to peak plasma concentration (tmax) is 20 minutes in healthy individuals or 33.8 minutes in patients with schizophrenia, with a mean half-life of 20.7 hours.^A32346 Bioavailability following intramuscular administration is higher than that for oral administration. Administration of haloperidol decanoate (the depot form of haloperidol for long-term treatment) in sesame oil results in slow release of the drug for long-term effects. The plasma concentrations of haloperidol gradually rise, reaching its peak concentration at about 6 days after the injection, with an apparent half-life of about 21 days. Steady-state plasma concentrations are achieved after the third or fourth dose.^F4645

Metabolisme

Haloperidol is extensively metabolised in the liver with only about 1% of the administered dose excreted unchanged in urine.^A32346 In humans, haloperidol is biotransformed to various metabolites, including p-fluorobenzoylpropionic acid, 4-(4-chlorophenyl)-4-hydroxypiperidine, reduced haloperidol, pyridinium metabolites, and haloperidol glucuronide. In psychiatric patients treated regularly with haloperidol, the concentration of haloperidol glucuronide in plasma is the highest among the metabolites, followed, in rank order, by unchanged haloperidol, reduced haloperidol and reduced haloperidol glucuronide. The drug is thought to be metabolized primarily by oxidative N-dealkylation of the piperidine nitrogen to form fluorophenylcarbonic acids and piperidine metabolites (which appear to be inactive), and by reduction of the butyrophenone carbonyl to the carbinol, forming hydroxyhaloperidol. The enzymes involved in the biotransformation of haloperidol include cytochrome P450 (CYP) including CYP3A4 and CYP2D6, carbonyl reductase and uridine di-phosphoglucose glucuronosyltransferase enzymes. The greatest proportion of the intrinsic hepatic clearance of haloperidol is performed by glucuronidation and followed by the reduction of haloperidol to reduced haloperidol and by CYP-mediated oxidation. In studies of cytochrome-mediated disposition in vitro, CYP3A4 appears to be the major isoform of the enzyme responsible for the metabolism of haloperidol in humans. The intrinsic clearance of the back-oxidation of reduced haloperidol to the parent compound, oxidative N-dealkylation and pyridinium formation are of the same order of magnitude. This suggests that the same enzyme system is responsible for the above three metabolic reactions. In vivo human studies on haloperidol metabolism have shown that the glucuronidation of haloperidol accounts for 50 to 60% of haloperidol biotransformation and that approximately 23% of the biotransformation was accounted for by the reduction pathway. The remaining 20 to 30% ofthe biotransformation of haloperidol would be via N-dealkylation and pyridinium formation.^A32346

Rute Eliminasi

In radiolabeling studies, approximately 30% of the radioactivity is excreted in the urine following a single oral administration of 14C-labelled haloperidol, while 18% is excreted in the urine as haloperidol glucuronide, demonstrating that haloperidol glucuronide is a major metabolite in the urine as well as in plasma in humans.^A32346

Interaksi Makanan

1 Data

1. Avoid alcohol. Alcohol may potential hypotension and CNS adverse effects.

Interaksi Obat

2291 Data

Deferasirox	The serum concentration of Haloperidol can be increased when it is combined with Deferasirox.
Leflunomide	The serum concentration of Haloperidol can be decreased when it is combined with Leflunomide.
Teriflunomide	The serum concentration of Haloperidol can be decreased when it is combined with Teriflunomide.
Buprenorphine	Haloperidol 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 Haloperidol.
Hydrocodone	Haloperidol may increase the central nervous system depressant (CNS depressant) activities of Hydrocodone.
Magnesium sulfate	The therapeutic efficacy of Haloperidol can be increased when used in combination with Magnesium sulfate.
Metyrosine	Haloperidol may increase the sedative activities of Metyrosine.
Minocycline	Minocycline may increase the central nervous system depressant (CNS depressant) activities of Haloperidol.
Suvorexant	Haloperidol 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 Haloperidol.
Thalidomide	Haloperidol may increase the central nervous system depressant (CNS depressant) activities of Thalidomide.
Zolpidem	Haloperidol may increase the central nervous system depressant (CNS depressant) activities of Zolpidem.
Brexpiprazole	The metabolism of Brexpiprazole can be decreased when combined with Haloperidol.
Eliglustat	The metabolism of Eliglustat can be decreased when combined with Haloperidol.
Everolimus	The metabolism of Everolimus can be decreased when combined with Haloperidol.
Flibanserin	The metabolism of Flibanserin can be decreased when combined with Haloperidol.
Ibrutinib	The metabolism of Ibrutinib can be decreased when combined with Haloperidol.
Ivabradine	The metabolism of Ivabradine can be decreased when combined with Haloperidol.
Ivacaftor	The metabolism of Ivacaftor can be decreased when combined with Haloperidol.
Lurasidone	The metabolism of Lurasidone can be decreased when combined with Haloperidol.
Naloxegol	The metabolism of Naloxegol can be decreased when combined with Haloperidol.
Olaparib	The metabolism of Olaparib can be decreased when combined with Haloperidol.
Ranolazine	The metabolism of Ranolazine can be decreased when combined with Haloperidol.
Sonidegib	The metabolism of Sonidegib can be decreased when combined with Haloperidol.
Avanafil	The metabolism of Avanafil can be decreased when combined with Haloperidol.
Eplerenone	The metabolism of Eplerenone can be decreased when combined with Haloperidol.
Cilostazol	The metabolism of Cilostazol can be decreased when combined with Haloperidol.
Colchicine	The metabolism of Colchicine can be decreased when combined with Haloperidol.
Fentanyl	The risk or severity of CNS depression can be increased when Haloperidol is combined with Fentanyl.
Iloperidone	The metabolism of Iloperidone can be decreased when combined with Haloperidol.
Retapamulin	The metabolism of Retapamulin can be decreased when combined with Haloperidol.
Tofacitinib	The metabolism of Tofacitinib can be decreased when combined with Haloperidol.
Vardenafil	The metabolism of Vardenafil can be decreased when combined with Haloperidol.
Lovastatin	The metabolism of Lovastatin can be decreased when combined with Haloperidol.
Amisulpride	Haloperidol may increase the antipsychotic activities of Amisulpride.
Methylphenidate	The risk or severity of adverse effects can be increased when Haloperidol is combined with Methylphenidate.
Metoclopramide	The risk or severity of adverse effects can be increased when Metoclopramide is combined with Haloperidol.
Sulpiride	Haloperidol may increase the antipsychotic activities of Sulpiride.
Icosapent	The therapeutic efficacy of Haloperidol can be increased when used in combination with Icosapent.
Mesalazine	Mesalazine may decrease the excretion rate of Haloperidol which could result in a higher serum level.
Indomethacin	The therapeutic efficacy of Haloperidol can be increased when used in combination with Indomethacin.
Nabumetone	The therapeutic efficacy of Haloperidol can be increased when used in combination with Nabumetone.
Ketorolac	The therapeutic efficacy of Haloperidol can be increased when used in combination with Ketorolac.
Tenoxicam	The therapeutic efficacy of Haloperidol can be increased when used in combination with Tenoxicam.
Tolmetin	The therapeutic efficacy of Haloperidol can be increased when used in combination with Tolmetin.
Piroxicam	The therapeutic efficacy of Haloperidol can be increased when used in combination with Piroxicam.
Fenoprofen	The therapeutic efficacy of Haloperidol can be increased when used in combination with Fenoprofen.
Sulindac	The therapeutic efficacy of Haloperidol can be increased when used in combination with Sulindac.
Flurbiprofen	The therapeutic efficacy of Haloperidol can be increased when used in combination with Flurbiprofen.
Etodolac	The therapeutic efficacy of Haloperidol can be increased when used in combination with Etodolac.
Mefenamic acid	The therapeutic efficacy of Haloperidol can be increased when used in combination with Mefenamic acid.
Naproxen	The therapeutic efficacy of Haloperidol can be increased when used in combination with Naproxen.
Sulfasalazine	The therapeutic efficacy of Haloperidol can be increased when used in combination with Sulfasalazine.
Phenylbutazone	The therapeutic efficacy of Haloperidol can be increased when used in combination with Phenylbutazone.
Carprofen	The therapeutic efficacy of Haloperidol can be increased when used in combination with Carprofen.
Diflunisal	The therapeutic efficacy of Haloperidol can be increased when used in combination with Diflunisal.
Salicylic acid	The therapeutic efficacy of Haloperidol can be increased when used in combination with Salicylic acid.
Meclofenamic acid	The therapeutic efficacy of Haloperidol can be increased when used in combination with Meclofenamic acid.
Acetylsalicylic acid	The therapeutic efficacy of Haloperidol can be increased when used in combination with Acetylsalicylic acid.
Oxaprozin	The therapeutic efficacy of Haloperidol can be increased when used in combination with Oxaprozin.
Ketoprofen	The therapeutic efficacy of Haloperidol can be increased when used in combination with Ketoprofen.
Balsalazide	The therapeutic efficacy of Haloperidol can be increased when used in combination with Balsalazide.
Olsalazine	Olsalazine may decrease the excretion rate of Haloperidol which could result in a higher serum level.
Lumiracoxib	The therapeutic efficacy of Haloperidol can be increased when used in combination with Lumiracoxib.
Magnesium salicylate	The therapeutic efficacy of Haloperidol can be increased when used in combination with Magnesium salicylate.
Salsalate	The therapeutic efficacy of Haloperidol can be increased when used in combination with Salsalate.
Choline magnesium trisalicylate	The therapeutic efficacy of Haloperidol can be increased when used in combination with Choline magnesium trisalicylate.
Antrafenine	The therapeutic efficacy of Haloperidol can be increased when used in combination with Antrafenine.
Tiaprofenic acid	The therapeutic efficacy of Haloperidol can be increased when used in combination with Tiaprofenic acid.
Taxifolin	The therapeutic efficacy of Haloperidol can be increased when used in combination with Taxifolin.
Oxyphenbutazone	The therapeutic efficacy of Haloperidol can be increased when used in combination with Oxyphenbutazone.
Licofelone	The therapeutic efficacy of Haloperidol can be increased when used in combination with Licofelone.
Benoxaprofen	The therapeutic efficacy of Haloperidol can be increased when used in combination with Benoxaprofen.
Metamizole	Metamizole may decrease the excretion rate of Haloperidol which could result in a higher serum level.
Cimicoxib	The therapeutic efficacy of Haloperidol can be increased when used in combination with Cimicoxib.
Lornoxicam	The therapeutic efficacy of Haloperidol can be increased when used in combination with Lornoxicam.
Aceclofenac	The therapeutic efficacy of Haloperidol can be increased when used in combination with Aceclofenac.
Zaltoprofen	The therapeutic efficacy of Haloperidol can be increased when used in combination with Zaltoprofen.
Azapropazone	The therapeutic efficacy of Haloperidol can be increased when used in combination with Azapropazone.
Salicylamide	The therapeutic efficacy of Haloperidol can be increased when used in combination with Salicylamide.
Kebuzone	The therapeutic efficacy of Haloperidol can be increased when used in combination with Kebuzone.
Isoxicam	The therapeutic efficacy of Haloperidol can be increased when used in combination with Isoxicam.
Indoprofen	The therapeutic efficacy of Haloperidol can be increased when used in combination with Indoprofen.
Ibuproxam	The therapeutic efficacy of Haloperidol can be increased when used in combination with Ibuproxam.
Floctafenine	The therapeutic efficacy of Haloperidol can be increased when used in combination with Floctafenine.
Fenbufen	The therapeutic efficacy of Haloperidol can be increased when used in combination with Fenbufen.
Etofenamate	The therapeutic efficacy of Haloperidol can be increased when used in combination with Etofenamate.
Epirizole	The therapeutic efficacy of Haloperidol can be increased when used in combination with Epirizole.
Benzydamine	The therapeutic efficacy of Haloperidol can be increased when used in combination with Benzydamine.
Dexibuprofen	The therapeutic efficacy of Haloperidol can be increased when used in combination with Dexibuprofen.
Dexketoprofen	The therapeutic efficacy of Haloperidol can be increased when used in combination with Dexketoprofen.
Droxicam	The therapeutic efficacy of Haloperidol can be increased when used in combination with Droxicam.
Firocoxib	The therapeutic efficacy of Haloperidol can be increased when used in combination with Firocoxib.
Clonixin	The therapeutic efficacy of Haloperidol can be increased when used in combination with Clonixin.
Morniflumate	The therapeutic efficacy of Haloperidol can be increased when used in combination with Morniflumate.
Talniflumate	The therapeutic efficacy of Haloperidol can be increased when used in combination with Talniflumate.
Robenacoxib	The therapeutic efficacy of Haloperidol can be increased when used in combination with Robenacoxib.
Tepoxalin	The therapeutic efficacy of Haloperidol can be increased when used in combination with Tepoxalin.
Flunixin	The therapeutic efficacy of Haloperidol can be increased when used in combination with Flunixin.

Target Protein

5-hydroxytryptamine receptor 2C HTR2C

D(2) dopamine receptor DRD2

5-hydroxytryptamine receptor 2A HTR2A

D(3) dopamine receptor DRD3

Melanin-concentrating hormone receptor 1 MCHR1

Synaptic vesicular amine transporter SLC18A2

Sigma non-opioid intracellular receptor 1 SIGMAR1

Histamine H1 receptor HRH1

Muscarinic acetylcholine receptor M3 CHRM3

Alpha-1A adrenergic receptor ADRA1A

Alpha-2A adrenergic receptor ADRA2A

Alpha-2B adrenergic receptor ADRA2B

Alpha-2C adrenergic receptor ADRA2C

5-hydroxytryptamine receptor 1A HTR1A

5-hydroxytryptamine receptor 6 HTR6

5-hydroxytryptamine receptor 7 HTR7

Glutamate receptor ionotropic, NMDA 2B GRIN2B

D(1A) dopamine receptor DRD1

Referensi & Sumber

Artikel (PubMed)

PMID: 14331
Niemegeers CJ, Laduron PM: Pharmacology and biochemistry of haloperidol. Proc R Soc Med. 1976;69 suppl 1:3-8.
PMID: 3559159
Gelders YG: Pharmacology, pharmacokinetics and clinical development of haloperidol decanoate. Int Clin Psychopharmacol. 1986 Jul;1 Suppl 1:1-11.
PMID: 10628896
Kudo S, Ishizaki T: Pharmacokinetics of haloperidol: an update. Clin Pharmacokinet. 1999 Dec;37(6):435-56. doi: 10.2165/00003088-199937060-00001.
PMID: 11873706
Seeman P: Atypical antipsychotics: mechanism of action. Can J Psychiatry. 2002 Feb;47(1):27-38.
PMID: 2033640
Mumtaz MM, Farooqui MY, Ghanayem BI, Rajaraman S, Frankenberg L, Ahmed AE: Studies on the mechanism of urotoxic effects of N,N'-dimethylaminopropionitrile in rats and mice. 1. Biochemical and morphologic characterization of the injury and its relationship to metabolism. J Toxicol Environ Health. 1991 May;33(1):1-17. doi: 10.1080/15287399109531501.
PMID: 25007358
Tardy M, Huhn M, Kissling W, Engel RR, Leucht S: Haloperidol versus low-potency first-generation antipsychotic drugs for schizophrenia. Cochrane Database Syst Rev. 2014 Jul 9;(7):CD009268. doi: 10.1002/14651858.CD009268.pub2.
PMID: 25592299
Dold M, Samara MT, Li C, Tardy M, Leucht S: Haloperidol versus first-generation antipsychotics for the treatment of schizophrenia and other psychotic disorders. Cochrane Database Syst Rev. 2015 Jan 16;1:CD009831. doi: 10.1002/14651858.CD009831.pub2.
PMID: 24242360
Adams CE, Bergman H, Irving CB, Lawrie S: Haloperidol versus placebo for schizophrenia. Cochrane Database Syst Rev. 2013 Nov 15;(11):CD003082. doi: 10.1002/14651858.CD003082.pub3.

Menampilkan 8 dari 10 artikel.

Link

Attachment

Contoh Produk & Brand

Produk: 401 • International brands: 13

Produk

Apo Haloperidol Tab 0.5mg

Tablet • .5 mg • Oral • Canada • Generic • Approved
Apo Haloperidol Tab 1mg

Tablet • 1 mg • Oral • Canada • Generic • Approved
Apo-haloperidol LA Injectable

Liquid • 50 mg / mL • Intramuscular • Canada • Generic • Approved
Apo-haloperidol LA Injectable

Liquid • 100 mg / mL • Intramuscular • Canada • Generic • Approved
Apo-haloperidol Liq 2mg/ml

Solution • 2 mg / mL • Oral • Canada • Generic • Approved
Apo-haloperidol Tab 10mg

Tablet • 10 mg • Oral • Canada • Generic • Approved
Apo-haloperidol Tab 2mg

Tablet • 2 mg • Oral • Canada • Generic • Approved
Apo-haloperidol Tab 5mg

Tablet • 5 mg • Oral • Canada • Generic • Approved

Menampilkan 8 dari 401 produk.

International Brands

Aloperidin — Janssen-Cilag
Bioperidolo — Firma
Brotopon — Pfizer
Dozic — Rosemont
Duraperidol
Einalon S
Eukystol — Merckle
Halosten — Shionogi Seiyaku
Keselan — Sumitomo
Linton — Tanabe Mitsubishi Pharma

Sekuens Gen/Protein (FASTA)

Sekuens dimuat saat dibutuhkan agar halaman tetap ringan.