A Blocker of N- and T-type Voltage-Gated Calcium Channels Attenuates Ethanol-Induced Intoxication, Place Preference, Self-Administration, and Reinstatement

Authors
Newton, Philip M.Zeng, LilyWang, VictoriaConnolly, JacklynWallace, Melisa J.Kim, ChankiShin, Hee-SupBelardetti, FrancescoSnutch, Terrance P.Messing, Robert O.
Issue Date
2008-11-05
Publisher
SOC NEUROSCIENCE
Citation
JOURNAL OF NEUROSCIENCE, v.28, no.45, pp.11712 - 11719
Abstract
There is a clear need for new therapeutics to treat alcoholism. Here, we test our hypothesis that selective inhibitors of neuronal calcium channels will reduce ethanol consumption and intoxication, based on our previous studies using knock-out mice and cell culture systems. We demonstrate that pretreatment with the novel mixed N-type and T-type calcium channel antagonist 1-(6,6-bis(4-fluorophenyl) hexyl)-4-(3,4,5-trimethoxybenzyl) piperazine (NP078585) reduced ethanol intoxication. NP078585 also attenuated the reinforcing and rewarding properties of ethanol, measured by operant self-administration and the expression of an ethanol conditioned place preference, and abolished stress-induced reinstatement of ethanol seeking. NP078585 did not affect alcohol responses in mice lacking N-type calcium channels. These results suggest that selective calcium channel inhibitors may be useful in reducing acute ethanol intoxication and alcohol consumption by human alcoholics.
Keywords
ALCOHOL DEPENDENCE TREATMENT; OMEGA-CONOTOXIN; GABA RELEASE; SEEKING BEHAVIOR; CONDITIONED CUES; RATS DRINKING; CA2+ CHANNELS; C57BL/6 MICE; DBA/2J MICE; NALTREXONE; ALCOHOL DEPENDENCE TREATMENT; OMEGA-CONOTOXIN; GABA RELEASE; SEEKING BEHAVIOR; CONDITIONED CUES; RATS DRINKING; CA2+ CHANNELS; C57BL/6 MICE; DBA/2J MICE; NALTREXONE; alcoholism; calcium channel; N type; T type; conotoxin; addiction; relapse
ISSN
0270-6474
URI
https://pubs.kist.re.kr/handle/201004/132982
DOI
10.1523/JNEUROSCI.3621-08.2008
Appears in Collections:
KIST Article > 2008
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