Praziquantel

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Praziquantel
File:Praziquantel.svg
File:Praziquantel.gif
Systematic (IUPAC) name
(RS)-2-(Cyclohexylcarbonyl) -1,2,3,6,7,11b-hexahydro-4H-pyrazino (2,1-alpha) isoquinolin-4-one
Clinical data
Pregnancy
category
  • Only when clearly needed (lack of sufficient data in humans)
Routes of
administration
oral
Legal status
Legal status
  • U.S.: Rx-only (human use), over-the-counter (veterinary use)[1]
Pharmacokinetic data
Bioavailability relatively small
Metabolism hepatic
Biological half-life 0.8 to 1.5 hours (Main Metabolites 4 to 5 hours)
Excretion mainly in urine
Identifiers
CAS Number 55268-74-1
ATC code P02BA01 (WHO) QP52AA01
PubChem CID 4891
DrugBank EXPT02728
Chemical data
Formula C19H24N2O2
Molar mass 312.411[[Script error: No such module "String".]]
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Praziquantel (Biltricide) is an anthelmintic effective against flatworms.

Praziquantel is not licensed for use in humans in the UK; it is, however, available as a veterinary anthelmintic, and is available for use in humans on a named-patient basis.

Uses

Flukes/trematodes

It is used against Schistosoma.[1] As of 2005, praziquantel is the primary treatment for human schistosomiasis, for which it is usually effective in a single dose.[2]

It is used to treat liver flukes (such as Clonorchis sinensis)[3] except for fascioliasis.[citation needed]

It is also used to treat paragonimiasis.

Tapeworms/cestodes

It is also used to treat:

History

Praziquantel was developed in the laboratories for parasitological research of Bayer AG and Merck KGaA in Germany (Elberfeld and Darmstadt) in the mid 1970s. The World Health Organization includes it on its Model List of Essential Medicines.

Pharmacokinetics

Praziquantel is well (approximately 80%) absorbed from the gastrointestinal tract. Due to extensive first-pass metabolism only relatively small amounts enter systemic circulation. Praziquantel has a serum half-life of 0.8 to 1.5 hours (metabolites 4 to 5 hours) in adults with normal renal and liver function. In patients with significantly impaired liver function (Child Pugh classes B ll///d C) the serum half-life is increased to 3 to 8 hours. Praziquantel and its metabolites are mainly excreted renally; within 24 hours after a single oral dose, 70 to 80% are found in urine, but less than 0.1% as the unchanged drug. Praziquantel is metabolized through the cytochrome P450 pathway 3A4. Agents that induce or inhibit CYP3A4 (i.e., phenytoin, rifampin, azole antifungals) will affect the metabolism of praziquantel.

Praziquantel has a particularly dramatic effect on patients with schistosomiasis. Studies of those treated have shown that within six months of receiving a dose of praziquantel, up to 90% of the damage done to internal organs due to schistosomiasis infection can be reversed.[2]

Mode of action

Although the mode of action is not exactly known at present, there is experimental evidence that Praziquantel increases the permeability of the membranes of parasite cells (certain schistosomes) for calcium ions. The drug thereby induces contraction of the parasites resulting in paralysis in the contracted state. The dying parasites are dislodged from their site of action in the host organism and may enter systemic circulation or may be destroyed by host immune reaction (phagocytosis). Additional mechanisms — focal disintegrations and disturbances of oviposition (laying of eggs) — are seen in other types of sensitive parasites.

Another hypothesis on the mechanism of action of praziquantel has been recently reported. The drug seems to interfere with adenosine uptake in cultured worms. This effect may have therapeutical relevance given that the schistosome, as the taenia and the echinococcus (other praziquantel sensitive parasites), is unable to synthesize purines de novo.

Bayer's Animal Health Division[2] website states, "Praziquantel is active against cestodes (tapeworms). Praziquantel is absorbed, metabolized in the liver and excreted in the bile. Upon entering the digestive tract from the bile, cestocidal activity is exhibited.1 Following exposure to praziquantel, the tapeworm loses its ability to resist digestion by the mammalian host. Because of this, whole tapeworms, including the scolices, are very rarely passed after administration of praziquantel. In many instances only disintegrated and partially digested pieces of tapeworms will be seen in the stool. The majority of tapeworms are digested and are not found in the feces."

Side effects

The majority of side-effects develop due to the release of the contents of the parasites as they are killed and the consequent host immune reaction. The heavier the parasite burden, the heavier and more frequent the side effects normally are.

  • Central nervous system: Frequently occurring side effects are dizziness, headache, and malaise. Drowsiness, somnolence, fatigue, and vertigo have also been seen. Almost all patients with cerebral cysticercosis experience CNS side effects related to the cell-death of the parasites (headache, worsening of preexisting neurological problems, seizures, arachnoiditis, and meningism). These side effects may be life-threatening and can be reduced by coadministration of corticosteroids. It is strongly recommended that all patients with cerebral cysticercosis are hospitalized during treatment.
  • GI Tract: Approximately 90% of all patients have abdominal pain or cramps with or without nausea and vomiting. Diarrhea may develop and may be severe with colic. Sweating, fever, and sometimes bloody stools may occur together with diarrhea.
  • Liver: Asymptomatic and transient increases of liver enzymes (AST and ALT) are noted frequently (up to 27%). No case of symptomatic liver damage has ever been seen so far.
  • Sensitivity reactions: Urticaria, rash, pruritus and eosinophilia in White Blood Counts.
  • Other locations/Body as a whole: Lower back pain, myalgia, arthralgia, fever, sweating, various cardiac arrhythmias, and hypotension.

Drug interactions

Antibiotics

A study found that the antibiotic rifampicin decreases plasmatic concentrations of praziquantel.[5]

Antiepileptics

Carbamazepine and phenytoin are reported to reduce the bioavailability of praziquantel.[6]

Antimalarials

Chloroquine reduces the bioavailability of praziquantel.[7]

Antacids / histamine H2-antagonists

At least 2 studies indicate the drug cimetidine heightens praziquantel bioavailability.[8][9]

Dosage

For schistosomiasis, the dose is 20 milligrams/kilogram by mouth every 4-6 hours for one day.

For tapeworms, the dose is 5-25 mg/kg by mouth once.

For liver fluke, the dose is 25 mg/kg by mouth every 4-6 hours for one day.

These dosages are for patients over 4 years old, and are to be taken with food.

Brand names

  • Biltricide (Bayer) 600 mg Tablets (for human use)
  • Cesol (Merck) Tablets
  • Kaicide (Taiwan)
  • Cysticide (Merck) Tablets
  • Zentozide (Berich (Thailand) Co)
  • Profender (combination with emodepside) (Bayer) for veterinary use
  • Droncit (Bayer) for veterinary use
  • Drontal (combination with pyrantel pamoate) (Bayer) for veterinary use
  • D-Worm (Farnum) for veterinary use; note that D-Worm also makes roundworm medicine containing piperidine which is not effective against tapeworms.
  • Tape Worm Tabs (Trade Winds) for veterinary use
  • Cestoved (Vedco) both tablets and injectable for veterinary use
  • PraziPro (Hikari) for aquarium use

References

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de:Praziquantel

es:Praziquantel fr:Praziquantel ko:프라지콴텔 it:Praziquantel arz:برازيكوانتيل nl:Praziquantel ja:プラジカンテル pl:Prazykwantel pt:Praziquantel

ru:Празиквантел
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  2. 2.0 2.1 The Carter Center. ""Schistosomiasis Control Program"". Retrieved 2008-07-17. 
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  4. Matthaiou DK, Panos G, Adamidi ES, Falagas ME (2008). "Albendazole versus Praziquantel in the Treatment of Neurocysticercosis: A Meta-analysis of Comparative Trials". PLoS Negl Trop Dis. 2 (3): e194. doi:10.1371/journal.pntd.0000194. PMC 2265431Freely accessible. PMID 18335068. 
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