- 18-Methoxycoronaridine
drugbox
IUPAC_name = (-)-18-methoxycoronaridine
width = 180
CAS_number = 308123-60-6
ATC_prefix =
ATC_suffix =
PubChem = 10248465
C=22 | H=28 | N=2 | O=3
molecular_weight = 368.47 g/mol
smiles =
melting_point =
melting_high =
bioavailability =
protein_bound =
metabolism =
elimination_half-life =
excretion =
pregnancy_AU =
pregnancy_US =
pregnancy_category =
legal_AU =
legal_CA =
legal_UK =
legal_US =
legal_status =
routes_of_administration =(-)-18-Methoxycoronaridine (18-MC) is a derivative of
ibogaine invented in 1996 by the research team around the pharmacologistStanley D. Glick from theAlbany Medical College and the chemistMartin E. Kuehne from theUniversity of Vermont . In animal studies it has proved to be effective at reducing self-administration ofmorphine ,cocaine ,methamphetamine andnicotine . [cite journal | author=S.D. Glick | title=18-Methoxycoronaridine, a non-toxic iboga alkaloid congener:effects on morphine and cocaine self-administration and on mesolimbic dopamine release in rats | journal=Brain Res. | year=1996 | pages=29–35 | volume=719 | issue=1-2 | pmid=8782860 | doi=10.1016/0006-8993(96)00056-X] 18MC is a selective α3β4 nicotinic antagonist and, opposed to ibogaine, has no affinity at the α4β2 subtype nor at NMDA-channels nor at theserotonin transporter . [cite journal | author=I.M. Maisonneuve | title=Anti-addictive actions of an iboga alkaloid congener: a novel mechanism for a novel treatment | journal=Pharmacol. Biochem. Behav. | year=2003 | pages=607–18 | volume=75 | issue=3 | pmid=12895678 | doi=10.1016/S0091-3057(03)00119-9] 18-MC has not yet been tested in humans. In 2002 the research team started trying to raise funds for human trials, but were unable to secure the estimated $5 million needed. [Addiction Treatment Strives for Legitimacy. "Journal of the American Medical Association". 2002; 288: 3096-3101.] Efforts to raise funds for future trials are still ongoing. [http://www.uvm.edu/~chem/?Page=news.html]Its CAS number is [308123-60-6] for the free base and [266686-77-5] for the monohydrochloride.
A number of derivatives of 18-MC have also been developed, with several of them being superior to 18-MC itself, the methoxyethyl congener ME-18-MC being more potent than 18-MC but with similar efficacy, and the methylamino analogue 18-MAC being more effective than 18-MC but with around the same potency. These compounds were also found to act as selective α3β4 nicotinic acetylcholine antagonists, with little or no effect on NMDA receptors. [Kuehne ME, He L, Jokiel PA, Pace CJ, Fleck MW, Maisonneuve IM, Glick SD, Bidlack JM. Synthesis and biological evaluation of 18-methoxycoronaridine congeners. Potential antiaddiction agents. "Journal of Medicinal Chemistry". 2003 Jun 19;46(13):2716-30. PMID 12801235] [Pace CJ, Glick SD, Maisonneuve IM, He LW, Jokiel PA, Kuehne ME, Fleck MW. Novel iboga alkaloid congeners block nicotinic receptors and reduce drug self-administration. "European Journal of Pharmacology". 2004 May 25;492(2-3):159-67. PMID 15178360]
ee also
*
Coronaridine
*Ibogaine
*Noribogaine
*Voacangine References
Further reading
#
Wikimedia Foundation. 2010.
