Extinction of ethanol-induced conditioned place preference and conditioned place aversion: effects of naloxone |
| |
| Authors: | Christopher L Cunningham Carly M Henderson Nancy M Bormann |
| |
| Institution: | (1) Department of Behavioral Neuroscience and Portland Alcohol Research Center, The Oregon Health Sciences University, 3181 SW Sam Jackson Park Road, Portland, OR 97201-3098, USA, US |
| |
| Abstract: | Four experiments examined the effect of naloxone pretreatment on the expression and extinction of ethanol-induced conditioned
place preference (experiments 1, 2, 4) or conditioned place aversion (experiments 1, 3). DBA/2 J mice received four pairings
of a distinctive tactile (floor) stimulus (CS) with injection of ethanol (2 g/kg) given either immediately before or after
5-min exposure to the CS. A different stimulus was paired with injection of saline. Pre-CS injection of ethanol produced conditioned
place preference, whereas post-CS injection of ethanol produced conditioned place aversion. Both behaviors extinguished partially
during repeated choice testing after vehicle injection. Naloxone (10 mg/kg) had little effect on the initial expression of
conditioned place preference, but facilitated its extinction. Moreover, repeated naloxone testing resulted in the expression
of a weak conditioned place aversion to the CS that initially elicited a place preference. In contrast, naloxone (1.5 or 10
mg/kg) enhanced expression of conditioned place aversion, thereby increasing its resistance to extinction. A control experiment
(experiment 4) indicated that repeated testing with a different aversive drug, lithium chloride, did not affect rate of extinction
or produce an aversion to the CS previously paired with ethanol. These findings do not support the suggestion that naloxone
facilitates the general processes that underlie extinction of associative learning. Also, these data are not readily explained
by the conditioning of place aversion at the time of testing. Rather, naloxone’s effects appear to reflect a selective influence
on maintenance of ethanol’s conditioned rewarding effect, an effect that may be mediated by release of endogenous opioids.
Overall, these findings encourage further consideration of the use of opiate antagonists in the treatment of alcoholism.
Received: 4 December 1997 / Final version: 16 February 1998 |
| |
| Keywords: | Ethanol Naloxone Lithium chloride Reward Reinforcement Aversion Conditioned place preference Conditioned place aversion Extinction Opioid system Locomotor activity Inbred mice |
| 本文献已被 SpringerLink 等数据库收录! |
|
