同: Cerebyx

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出典(authority):フリー百科事典『ウィキペディア（Wikipedia）』「2014/01/29 09:54:29」(JST)

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Fosphenytoin (fosphenytoin sodium injection, previously Cerebyx, Parke-Davis; Prodilantin, Pfizer Holding France^[1]) is a water-soluble phenytoin prodrug that is administered intravenously to deliver phenytoin, potentially more safely than intravenous phenytoin. It is most commonly used in the acute treatment convulsive status epilepticus.

On 18 November 2004, Sicor (a subsidiary of Teva) received a tentative approval letter from the United States Food and Drug Administration for a generic version of fosphenytoin.^[2]

Uses[edit]

Approved[edit]

Fosphenytoin is approved in the United States for the short term (five days or fewer) treatment of epilepsy when more widely used means of phenytoin administration are not possible or are ill-advised,^[3] such as endotracheal intubation, status epilepticus or some other type of repeated seizures; vomiting, and/or the patient is unalert or not awake or both.^[4]

Unapproved/off-label/investigational[edit]

In April 2003, Applebaum and colleagues at the Ben-Gurion University of the Negev in Beersheba reported that even though anticonvulsants are often very effective in mania, and acute mania requires rapid treatment, fosphenytoin had no antimanic effect even 60 minutes after administration of doses used in status epilepticus.^[5]

Fosphenytoin was more successfully used to relieve pain refractory to opiates in a 37-year-old woman with neuroma, according to Dr. Gary J. McCleane of the Rampark Pain Center in Lurgan, Northern Ireland.^[6] She was given 1,500 phenytoin equivalent units of fosphenytoin over a 24 hour period, producing pain relief that last three to fourteen weeks after each infusion, allowing her to use less opiates.^[6]

Metabolism[edit]

One millimole of phenytoin is produced for every millimole of fosphenytoin administered; the hydrolysis of fosphenytoin also yields phosphate and formaldehyde, the latter of which is subsequently metabolized to formate, which is in turn metabolized by a folate dependent mechanism.^[3]

Side effects[edit]

Side effects are similar to intravenous phenytoin and include hypotension, cardiac arrhythmias, CNS adverse events (nystagmus, dizziness, sedation/somnolence, ataxia and stupor), and local dermatological reactions. Purple glove syndrome probably occurs with fosphenytoin but possibly at lower frequency than with intravenous phenytoin. Fosphenytoin can cause hyperphosphatemia in end-stage renal failure patients.^[7]

History[edit]

Phenytoin, in both its acidic and sodium salt forms, is erratically bioavailable whether it is injected or taken orally due to its high melting point, weak acidity, and its being only sparingly soluble in water.^[8] Simply putting patients on other drugs is not always an option; this was especially true before 1993, when the number of anticonvulsants available was much more limited.^[9] One solution was to develop a prodrug that did not have these drawbacks.

Fosphenytoin was approved by the Food and Drug Administration (FDA) on August 5, 1996 for use in epilepsy.^[10]

References[edit]

^ "PRODILANTIN 75 mg/ml sol inj IM et p perf IV". VIDAL, l'information de référence sur les produits de santé. Retrieved 23 October 2005.
^ "Fosphenytoin Sodium Approval History". Retrieved 20 October 2005.
^ ^a ^b Parke-Davis (2001). "Cerebyx: Fosphenytoin Sodium Injection - Labeling Revision" (PDF). Cerebyx Approval History. Warner-Lambert Company. Retrieved 20 October 2005. ^{[dead link]}
^ Johnson J, Wrenn K (2001). "Inappropriate fosphenytoin use in the ED". American Journal of Emergency Medicine 19 (4): 293–4. doi:10.1053/ajem.2001.24471. PMID 11447516. Fulltext options List of Library Holdings Worldwide
^ Applebaum J, Levine J, Belmaker RH (2003). "Intravenous fosphenytoin in acute mania" (PDF). Journal Clinical Psychiatry 64 (4): 408–9. doi:10.4088/JCP.v64n0408. PMID 12716241.
^ ^a ^b McCleane GJ (2002). "Intravenous infusion of fosphenytoin produces prolonged pain relief: a case report". The Journal of Pain 3 (2): 156–8. doi:10.1054/jpai.2002.123004. PMID 14622802. List of Library Holdings Worldwide
^ McBryde KD, Wilcox J, Kher KK (2005). "Hyperphosphatemia due to fosphenytoin in a pediatric ESRD patient". Pediatric Nephrology (Berlin, Germany) (PDF|format= requires |url= (help)) 20 (8): 1182–5. doi:10.1007/s00467-005-1947-0. PMID 15965770.
^ Yamaoka Y, Roberts RD, Stella VJ (April 1983). "Low-melting phenytoin prodrugs as alternative oral delivery modes for phenytoin: a model for other high-melting sparingly water-soluble drugs". J Pharm Sci 72 (4): 400–5. doi:10.1002/jps.2600720420. PMID 6864479.
^ Anticonvulsants before 1993 Neuroland
^ "Cerebyx Approval History". Retrieved 20 October 2005.

UpToDate Contents

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1. 小児における痙攣を伴うてんかん重積状態のマネージメント management of convulsive status epilepticus in children
2. 成人における痙攣性のてんかん重積状態：治療および予後 convulsive status epilepticus in adults treatment and prognosis
3. 神経疾患を有する手術患者の周術期ケア perioperative care of the surgical patient with neurologic disease
4. フェニトイン中毒 phenytoin poisoning
5. 抗てんかん剤：作用機序、薬理学、および有害事象 antiepileptic drugs mechanism of action pharmacology and adverse effects

English Journal

Levetiracetam versus lorazepam in status epilepticus: a randomized, open labeled pilot study.

Misra UK, Kalita J, Maurya PK.SourceDepartment of Neurology, Sanjay Gandhi Postgraduate Institute of Medical Sciences, Raebareily Road, Lucknow, 226014, India, drukmisra@rediffmail.com.
Journal of neurology.J Neurol.2011 Sep 6. [Epub ahead of print]
For the management of status epilepticus (SE), lorazepam (LOR) is recommended as the first and phenytoin or fosphenytoin as the second choice. Both these drugs have significant toxicity. Intravenous levetiracetam (LEV) has become available, but its efficacy and safety has not been reported in compar
PMID 21898137

Cost-utility analysis of levetiracetam and phenytoin for posttraumatic seizure prophylaxis.

Cotton BA, Kao LS, Kozar R, Holcomb JB.SourceDepartment of Surgery and The Center for Translational Injury Research, The University of Texas Health Science Center, Houston, Texas 77030, USA. bryan.a.cotton@uth.tmc.edu
The Journal of trauma.J Trauma.2011 Aug;71(2):375-9.
BACKGROUND: The standard for early posttraumatic brain injury (TBI) seizure prophylaxis is phenytoin. Despite its effectiveness, some argue for the use of newer antiepileptics (e.g., levetiracetam) because phenytoin requires close monitoring to maintain its therapeutic window and is associated with
PMID 21825941

Japanese Journal

けいれん(てんかん)重積の薬物治療ストラテジー (特集熱性けいれんと急性脳症の最新情報) -- (熱性けいれん--病態とマネジメント)

林北見
小児科診療 74(6), 903-908, 2011-06
NAID 40018848776

A comparison of central brain (cerebrospinal and extracellular fluids) and peripheral blood kinetics of phenytoin after intravenous phenytoin and fosphenytoin

WANG X
Seizure 12, 330-336, 2003
NAID 30015079804

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リンク元	「ホスフェニトイン」

「ホスフェニトイン」

Fosphenytoin
Systematic (IUPAC) name
	(2,5-dioxo-4,4-diphenyl-imidazolidin-1-yl)methoxyphosphonic acid
Clinical data
Trade names	Cerebyx
AHFS/Drugs.com	monograph
MedlinePlus	a604036
Pregnancy cat.	D (US)
Legal status	℞ Prescription only
Routes	Intravenous, intramuscular
Pharmacokinetic data
Bioavailability	100% (IM)
Protein binding	95 to 99%
Metabolism	Hepatic
Half-life	15 minutes to convert to phenytoin
Excretion	Renal (as phenytoin)
Identifiers
CAS number	93390-81-9
ATC code	N03AB05
PubChem	CID 56339
DrugBank	DB00252
ChemSpider	50839
UNII	B4SF212641
KEGG	D07993
ChEMBL	CHEMBL919
Chemical data
Formula	C16H15N2O6P
Mol. mass	362.274 g/mol
	SMILES O=C3N(C(=O)C(c1ccccc1)(c2ccccc2)N3)COP(=O)(O)O;
	InChI InChI=1S/C16H15N2O6P/c19-14-16(12-7-3-1-4-8-12,13-9-5-2-6-10-13)17-15(20)18(14)11-24-25(21,22)23/h1-10H,11H2,(H,17,20)(H2,21,22,23) ; Key:XWLUWCNOOVRFPX-UHFFFAOYSA-N ;
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英: fosphenytoin
同: フォスフェニトイン
関: 抗てんかん剤

フェニトインのプロドラッグ。水溶性が高く経静脈的に投与される。

[French_trade_name-1] "PRODILANTIN 75 mg/ml sol inj IM et p perf IV". VIDAL, l'information de référence sur les produits de santé. Retrieved 23 October 2005.

[generic-2] "Fosphenytoin Sodium Approval History". Retrieved 20 October 2005.

[approved_use-3] Parke-Davis (2001). "Cerebyx: Fosphenytoin Sodium Injection - Labeling Revision" (PDF). Cerebyx Approval History. Warner-Lambert Company. Retrieved 20 October 2005. ^{[dead link]}

[when_to_use_fosphenytoin-4] Johnson J, Wrenn K (2001). "Inappropriate fosphenytoin use in the ED". American Journal of Emergency Medicine 19 (4): 293–4. doi:10.1053/ajem.2001.24471. PMID 11447516. Fulltext options List of Library Holdings Worldwide

[not_an_antimanic-5] Applebaum J, Levine J, Belmaker RH (2003). "Intravenous fosphenytoin in acute mania" (PDF). Journal Clinical Psychiatry 64 (4): 408–9. doi:10.4088/JCP.v64n0408. PMID 12716241.

[neuropathic_pain-6] McCleane GJ (2002). "Intravenous infusion of fosphenytoin produces prolonged pain relief: a case report". The Journal of Pain 3 (2): 156–8. doi:10.1054/jpai.2002.123004. PMID 14622802. List of Library Holdings Worldwide

[not_in_kidney_failure-7] McBryde KD, Wilcox J, Kher KK (2005). "Hyperphosphatemia due to fosphenytoin in a pediatric ESRD patient". Pediatric Nephrology (Berlin, Germany) (PDF|format= requires |url= (help)) 20 (8): 1182–5. doi:10.1007/s00467-005-1947-0. PMID 15965770.

[erratic-8] Yamaoka Y, Roberts RD, Stella VJ (April 1983). "Low-melting phenytoin prodrugs as alternative oral delivery modes for phenytoin: a model for other high-melting sparingly water-soluble drugs". J Pharm Sci 72 (4): 400–5. doi:10.1002/jps.2600720420. PMID 6864479.

[pre-1993-9] Anticonvulsants before 1993 Neuroland

[approval-10] "Cerebyx Approval History". Retrieved 20 October 2005.

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fosphenytoin