- Vanoxerine
Drugbox
IUPAC_name = 1- [2- [bis(4-fluorophenyl)methoxy] ethyl] -4-(3-phenylpropyl)piperazine
width = 250
CAS_number= 67469-78-7
ATC_prefix=
ATC_suffix=
ATC_supplemental=
PubChem=3455
DrugBank=
C=28 | H=33 | F=2 | N=2 | O=1
molecular_weight = 450.563 g/mol (freebase); 523.494 g/mol (dihydrochloride)
bioavailability=
metabolism =
elimination_half-life= 6 hours approx
excretion =
pregnancy_category =
legal_status = Investigational New Medicine
routes_of_administration=Vanoxerine, also known as GBR-12909, is a
piperazine derivative which is a potent and selectivedopamine reuptake inhibitor . GBR-12909 binds to the target site on thedopamine reuptake transporter around 500 times more strongly thancocaine , but has only mild stimulant effects, because as well as inhibiting the reuptake of dopamine, GBR-12909 inhibits dopamine release, and so produces only a slight elevation of dopamine levels. [Singh S. Chemistry, Design, and Structure-Activity Relationship of Cocaine Antagonists. "Chemistry Reviews", 2000. 100(3): 925-1024.]Vanoxerine has been researched for use in treating
cocaine dependence both as a substitute for cocaine and to block the rewarding effects. This strategy of using a competingagonist with a longer half-life has been successfully used to treat addiction to opiates such asheroin by substituting withmethadone . It is hoped that vanoxerine will be of similar use in treating cocaine addiction. [Vetulani J. Drug addiction. Part III. Pharmacotherapy of addiction. "Polish Journal of Pharmacology". 2001 Sep-Oct;53(5):415-34.] [Preti A. New developments in the pharmacotherapy of cocaine abuse. "Addiction Biology". 2007 Jun;12(2):133-51.]Research also indicates that vanoxerine may have additional mechanisms of action including antagonist action at
nicotinic acetylcholine receptor s, [Szasz BK, Vizi ES, Kiss JP. Nicotinic acetylcholine receptor antagonistic property of the selective dopamine uptake inhibitor, GBR-12909 in rat hippocampal slices. "Neuroscience". 2007 Mar 2;145(1):344-9.] and it has also been shown to reduce the consumption of alcohol in animal models of alcohol abuse. [Kamdar NK, Miller SA, Syed YM, Bhayana R, Gupta T, Rhodes JS. Acute effects of naltrexone and GBR 12909 on ethanol drinking-in-the-dark in C57BL/6J mice. "Psychopharmacology (Berlin)". 2007 Jun;192(2):207-17.]Vanoxerine has been through human trials up to Phase 2, but has not been developed for clinical use, although it is still being researched. [cite journal |author=Søgaard U, Michalow J, Butler B, "et al" |title=A tolerance study of single and multiple dosing of the selective dopamine uptake inhibitor GBR 12909 in healthy subjects |journal=International clinical psychopharmacology |volume=5 |issue=4 |pages=237–51 |year=1990 |pmid=2150527 |doi=] [Preti A. Vanoxerine National Institute on Drug Abuse. "Current Opinion in Investigational Drugs". 2000 Oct;1(2):241-51.] [Gorelick DA, Gardner EL, Xi ZX. Agents in development for the management of cocaine abuse. "Drugs". 2004;64(14):1547-73.]
A
decanoate ester of vanoxerine, DBL-583, has also been developed, which slowly breaks down in the body and lasts for up to a month after a single injection. [Baumann MH, Ayestas MA, Sharpe LG, Lewis DB, Rice KC, Rothman RB. Persistent antagonism of methamphetamine-induced dopamine release in rats pretreated with GBR12909 decanoate. "Journal of Pharmacology and Experimental Therapeutics". 2002 Jun;301(3):1190-7.] [Baumann MH, Phillips JM, Ayestas MA, Ali SF, Rice KC, Rothman RB. Preclinical evaluation of GBR12909 decanoate as a long-acting medication for methamphetamine dependence. "Annals of the New York Academy of Sciences". 2002 Jun;965:92-108.]References
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