4.4 Article Proceedings Paper

The discriminative stimulus properties of self-administered ethanol are mediated by GABAA and NMDA receptors in rats

Journal

PSYCHOPHARMACOLOGY
Volume 154, Issue 1, Pages 13-22

Publisher

SPRINGER-VERLAG
DOI: 10.1007/s002130000619

Keywords

ethanol; GABA(A); NMDA; rat; self-administration; drug discrimination; investigator-administered

Funding

  1. NIAAA NIH HHS [AA 09981] Funding Source: Medline

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Rationale: The neurobiological systems that mediate the discriminative stimulus effects of self-administered drugs are largely unknown. The present study examined the discriminative stimulus effects of self-administered ethanol. Methods: Rats were trained to discriminate ethanol (1 g/kg, IF) from saline on a two-lever drug discrimination task with sucrose (10% w/v) reinforcement. Test sessions were conducted with ethanol (0 or 10% v/v) added to the sucrose reinforcement to determine if self-administered ethanol would interact with the discriminative stimulus effects of investigator-administered ethanol, or with the ethanol-like discriminative stimulus effects of the GABA(A)-positive modulator pen tobarbital or the non-competitive NMDA antagonist MK-801. Results. During a saline test session, ethanol (10% v/v) was added to the sucrose reinforcement. Responding by all animals began accurately on the saline-appropriate lever and then switched to the ethanol-appropriate lever after rats self-administered a mean dose of 1.2 +/- 0.14 g/kg ethanol. During cumulative self-administration trials, responding initially occurred on the saline lever and then switched to the ethanol-appropriate lever after ethanol (0.68 +/- 0.13 g/kg) was self-administered. Investigator-administered MK-801 (0.01-1.0 mg/kg, cumulative IF) and pentobarbital (0.3-10.0 mg/kg, cumulative IF) dose-dependently substituted for ethanol. When ethanol (10% v/v) was added to the sucrose reinforcer, MK-801 and pentobarbital dose-response curves were shifted significantly to the left. Conclusions: Self-administered ethanol substituted for and potentiated the stimulus effects of investigator-administered ethanol, suggesting that the discriminative stimulus effects of self-administered ethanol are similar to those produced by investigator-administered ethanol. Self-administered ethanol enhanced the ethanol-like discriminative stimulus effects of MK-801 and pentobarbital, which suggests that the discriminative stimulus effects of self-administered ethanol are mediated by NMDA and GABA(A) receptors.

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