Alcohol
Volume 21, Issue 2 , Pages 107-115, June 2000

Neonatal nicotine administration influences ethanol-induced behaviors

  • Anders Fredriksson

      Affiliations

    • Department of Neuroscience and Psychiatry, Ulleråker, Uppsala, University, S-750 17 Uppsala, Sweden
  • ,
  • Per Eriksson

      Affiliations

    • Department of Environmental Toxicology, Uppsala University, S-752 38 Uppsala, Sweden
  • ,
  • Emma Ankarberg

      Affiliations

    • Department of Environmental Toxicology, Uppsala University, S-752 38 Uppsala, Sweden
  • ,
  • Tomás Palomo

      Affiliations

    • Servicio de Psiquiatria, Hospital Universitario, 12 de Octubre, Avenida de Córdoba s/n, 28041 Madrid, Spain
  • ,
  • Trevor Archer

      Affiliations

    • Department of Psychology, University of Göteborg, Box 500, SE-405 30 Gothenborg, Sweden
    • Corresponding Author InformationCorresponding author

Received 31 March 1999; received in revised form 5 October 1999; accepted 17 November 1999.

Abstract 

Neonatal mice were administered nicotine (66 μg (−)-nicotine base/kg body weight (bw) s.c. twice daily at 0800 and 1700 h on postnatal days 10 and 14) and control mice received saline (10 ml 0.9% NaCl/kg bw s.c.) on the same occasions. Behavioral testing was initiated 3 months after birth. In Experiment 1, neonatal nicotine administration did not affect spontaneous motor activity but altered the peak dose stimulatory effect of ethanol upon locomotion and rearing activity from 3.0 mg/kg, in the control mice, to 1.5 mg/kg. Administration of the nicotine antagonist, mecamylamine (MEC, 2.0 mg/kg), had no effect upon the peak dose stimulatory effect (i.e., 1.5 mg/kg) evidenced in the nicotine-treated mice, but attenuated the stimulatory effect of the 3.0 mg/kg dose of ethanol in the control mice. In Experiment 2, the effects of neonatal nicotine administration upon ethanol intake and preference were assessed. In the single fluid access (one-bottle) test, nicotine-treated mice consumed both more ethanol (2%, 4%, or 6% concentrations) and more tap water than control mice. In the two-bottle ethanol preference test, nicotine-treated mice consumed more ethanol and tap water. Further analysis of the high-preferring (HP) ethanol mice indicated higher ethanol intake and preference in the nicotine-treated mice but no differences in tap water or total fluid intake. The present findings are considered together with prevailing notions of nicotine receptor alterations and possible cross-sensitization effects modulating substance abuse.

Keywords:  Nicotine, Ethanol, Neonatal, Motor behavior, Mecamylamine, Peak effect, Ethanol intake, Ethanol preference, Mice

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PII: S0741-8329(00)00085-9

Alcohol
Volume 21, Issue 2 , Pages 107-115, June 2000