Phenytoin

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Phenytoin
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Systematic (IUPAC) name
5,5-diphenylimidazolidine-2,4-dione
Clinical data
Pregnancy
category
  • D
Routes of
administration
Oral, parenteral
Legal status
Legal status
  • ℞ (Prescription only)
Pharmacokinetic data
Bioavailability 70-100% oral, 24.4% for rectal and intravenous administration
Protein binding 90%
Metabolism hepatic
Biological half-life 6-24 hours
Excretion Primarily through the bile, urinary
Identifiers
CAS Number 57-41-0
ATC code N03AB02 (WHO) N03AB04, N03AB05
PubChem CID 1775
DrugBank DB00252
ChemSpider 1710
Chemical data
Formula C15H12N2O2
Molar mass 252.268 g/mol[[Script error: No such module "String".]]
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Phenytoin sodium is a commonly used antiepileptic. Phenytoin (fen-i-TOE-in) acts to suppress the abnormal brain activity seen in seizure by reducing electrical conductance among brain cells by stabilizing the inactive state of voltage-gated sodium channels. Aside from seizures, it is an option in the treatment of trigeminal neuralgia in the event that carbamazepine is deemed inappropriate.

It is sometimes considered a class 1b antiarrhythmic.[1]

Trade names

Phenytoin sodium has been marketed as Phenytek by Mylan Laboratories, previously Bertek Pharmaceuticals, and Dilantin; Australia also Dilantin Kapseals and Dilantin Infatabs in the USA, Eptoin by Abbott Group in India and as Epanutin in the UK and Israel, by Parke-Davis, now part of Pfizer. In the USSR and post-USSR countries, it was/is marketed as Дифенин (Diphenin, Dipheninum),.

History

Phenytoin (diphenylhydantoin) was first synthesized by German chemist Heinrich Biltz in 1908[2]. Biltz sold his discovery to Parke-Davis, which did not find an immediate use for it. In 1938, outside scientists including H. Houston Merritt and Tracy Putnam discovered phenytoin's usefulness for controlling seizures, without the sedative effects associated with phenobarbital.

According to Goodman and Gilman's Pharmacological Basis of Therapeutics,

In contrast to the earlier accidental discovery of the antiseizure properties of bromide and phenobarbital, phenytoin was the product of a search among nonsedative structural relatives of phenobarbital for agents capable of suppressing electroshock convulsions in laboratory animals.[3]

There are some indications that phenytoin has other effects, including anxiety control and mood stabilization, although it has never been approved for those purposes by the FDA. Jack Dreyfus, founder of the Dreyfus Fund, became a major proponent of phenytoin as a means to control nervousness and depression when he received a prescription for Dilantin in 1966. He is believed to have supplied large amounts of the drug to Richard Nixon throughout the late 1960s and early 1970s. Dreyfus' experience with phenytoin is outlined in his book, A Remarkable Medicine Has Been Overlooked,[4]. Despite more than $70 million in personal financing, his push to see phenytoin evaluated for alternative uses has had little lasting effect on the medical community. This was partially because Parke-Davis was reluctant to invest in a drug nearing the end of its patent life, and partially due to mixed results from various studies. It was approved by the USA Food and Drug Administration in 1953 for use in seizures.

Dilantin made an appearance in the 1962 novel One Flew Over the Cuckoo's Nest by Ken Kesey, both as an anticonvulsant and as a mechanism to control inmate behavior.

In 2008, the drug was put on the FDA's Potential Signals of Serious Risks List to be further evaluated for approval. The list means that the FDA has identified a potential safety issue, but does not mean that FDA has identified a causal relationship between the drug and the listed risk.

According to the FDA's New Safety Information Identified by the Adverse Event Reporting System (AERS) Phenytoin Injection (Dilantin) has been associated with the risk of Purple Glove Syndrome.

Side-effects

Neurologic

At therapeutic doses, phenytoin produces horizontal gaze nystagmus, which is harmless but occasionally tested for by police as a marker for alcohol intoxication (which can also produce nystagmus). At toxic doses, patients experience sedation, cerebellar ataxia, and ophthalmoparesis, as well as seizures. Idiosyncratic side-effects of phenytoin, as with other anticonvulsants, include rash and severe allergic reactions.

Phenytoin may accumulate in the cerebral cortex over long periods of time, as well as causing atrophy of the cerebellum when administered at chronically high levels. Despite this, the drug has a long history of safe use, making it one of the more popular anti-convulsants prescribed by doctors, and a common "first line of defense" in seizure cases.

Hematologic

It has been suggested that phenytoin causes a reduction in folic acid levels, predisposing patients to megaloblastic anemia. Folic acid is presented in foods as polyglutamate, which is then converted into monoglutamates by intestinal conjugase. Phenytoin acts by inhibiting this enzyme, thereby causing folate deficiency.[5] Other side effects may include: agranulocytosis, aplastic anemia, leukopenia, thrombocytopenia.

Teratogenicity

Phenytoin is a known teratogen. The syndrome consists of craniofacial anomalies (broad nasal bridge, cleft lip and palate, microcephaly) and a mild form of mental retardation (average IQ=71).[6] This syndrome resembles the well-described Fetal Alcohol Syndrome[7] and has also been called the "fetal hydantoin syndrome".[citation needed] Data now being collected by the Epilepsy and Antiepileptic Drug Pregnancy Registry may one day answer this question definitively.

Some recommend avoiding polytherapy and maintaining the minimal dose possible during pregnancy, but acknowledge that current data do not provide clear answers.[8]

Carcinogenicity

There is no good evidence that phenytoin is a human carcinogen.[9][10]

Gingival

Phenytoin has been associated with drug induced gingival enlargement (hyperplasia) in the oral cavity probably due to above mentioned folate defiency. Plasma concentrations needed to induce gingival lesions has not been clearly defined. Effects consist of the following: bleeding upon probing, increased gingival exudate, pronounced gingival inflammatory response to plaque levels, associated in some instances with bone loss but without tooth detachment.

Suicide risk

Following almost 200 studies of 11 anti-seizure drugs, the FDA has also warned of an increased suicide risk for any patients treated with certain anti-seizure drugs. The study of 44,000 patients found that patients whose epilepsy is treated with drugs face about twice the risk of suicidal thoughts compared to placebo-takers. Although phenytoin was not named in the study, the FDA announced that it expected the risk applied to every epilepsy drug.[11]

Dermatologic

Hypertrichosis, rash, exfoliative dermatitis, pruritis.

In autoimmune disease

Phenytoin has been known to cause drug-induced lupus.[12]

Phenytoin therapy has been linked to the life-threatening skin reactions Stevens-Johnson syndrome (SJS) and toxic epidermal necrolysis (TEN). These conditions are significantly more common in patients with a particular HLA-B allele, HLA-B*1502.[13] This allele occurs almost exclusively in patients with ancestry across broad areas of Asia, including South Asian Indians.

In immunodeficiency disease

Phenytoin is also associated with induction of reversible IgA deficiency.[13]

Interactions

Phenytoin is an inducer of the CYP3A4 and CYP2C19 families of the P450 enzyme responsible for the hepatic elimination and degradation of various drugs.

See also

References

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External links

de:Phenytoin

es:Fenitoína eu:Fenitoina fa:فنی توئین fr:phénytoïne hr:Fenitoin it:Fenitoina ja:フェニトイン no:Fenytoin pl:Fenytoina pt:Fenitoína ru:Фенитоин fi:Fenytoiini

zh:苯妥英钠
  1. Lua error in package.lua at line 80: module 'Module:Citation/CS1/Suggestions' not found.
  2. Biltz, H. Constitution of the Products of the Interaction of Substituted Carbamides on Benzil and Certain New Methods for the Preparation of 5,5-Diphenylhydantoin. 1908, 41, 1379-93.
  3. Goodman and Gilman's Pharmacological Basis of Therapeutics, 10th ed. (New York: McGraw-Hill, 2001).
  4. Dreyfus, Jack (1998). A Remarkable Medicine Has Been Overlooked: Including an Autobiography and the Clinical Section of the Broad Range of Use of Phenytoin. Continuum International Publishing Group. ISBN 0-8264-1069-3. 
  5. Carl GF, Smith ML. (1995). Phenytoin-folate interactions: differing effects of the sodium salt and the free acid of phenytoin. http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=1547769&dopt=Abstract.
  6. Beckmann, Charles R, et al. Obstetrics and Gynecology. 4th Ed. Baltimore: Lippincott Williams & Wilkins, 2002.
  7. CDC. (2004). Fetal Alcohol Syndrome: Guidelines for Referral and Diagnosis. Can be downloaded at http://www.cdc.gov/fas/faspub.htm.
  8. Adab N, Tudur SC, Vinten J, Williamson P, Winterbottom J (2004). "Common antiepileptic drugs in pregnancy in women with epilepsy". Cochrane Database Syst Rev (3): CD004848. doi:10.1002/14651858.CD004848. PMID 15266543. 
  9. Report on Carcinogens, Eleventh Edition (PB2005-104914, 2004) p III-216.
  10. Maeda T, Sano N, Togei K, Shibata M, Izumi K, Otsuka H (1988). "Lack of carcinogenicity of phenytoin in (C57BL/6 x C3H)F1 mice". J Toxicol Environ Health. 24 (1): 111–9. doi:10.1080/15287398809531144. PMID 3373561. 
  11. FDA warns of risks from epilepsy drugs.. http://news.yahoo.com/s/ap/20080201/ap_on_he_me/epilepsy_drugs
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