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Alcohol and Alcoholism Advance Access originally published online on September 8, 2009
Alcohol and Alcoholism 2009 44(6):535-546; doi:10.1093/alcalc/agp047
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© The Author 2009. Published by Oxford University Press [on behalf of the Medical Council on Alcohol]. All rights reserved

The Influence of Chronic Nicotine Administration on Behavioural and Neurochemical Parameters in Male and Female Rats after Repeated Binge Drinking Exposure

Frédéric Lallemand, Roberta J. Ward and Philippe De Witte*

Université Catholique de Louvain, Laboratoire de Biologie du Comportement, 1 Place Croix du Sud, 1348 Louvain-la-Neuve, Belgium

* Corresponding author: Biologie du Comportement, Université catholique de Louvain, 1 Place Croix du Sud, 1348 Louvain-la-Neuve, Belgium. Tel: +32-10-474384; Fax: +32-10-474094; E-mail: dewitte{at}uclouvain.be

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   Abstract

Aims: The possible interaction between nicotine and ‘binge drinking’ in eliciting changes in behavioural patterns of ‘binge drinking’ rats as well as nucleus accumbens (NAc) glutamate levels has been investigated in these present studies. Methods: Adult or adolescent male and female rats received ethanol, 2 g/kg or 3 g/kg, by gavage in a ‘binge drinking’ regimen (3 times/day over a 6 h period, for 2 days followed by 5 days of abstinence) combined with or without nicotine, 0.3 g/kg, for either a 5-week (adult) or a 4-week (adolescent) period. Motor activity was then assessed for a period of 60 min after three further doses of ethanol or water. In addition, the NAc glutamate level was assayed in each group for 1 h after the first gavage regimen with ethanol, 2 g/kg or 3 g/kg, or water. Results: Adult female rats showed greater sensitivity to each ethanol dose (2 g/kg and 3 g/kg) than the adult male rats, their motor activity decreasing during the first and third ‘binge’. In contrast, in male adult rats, the sedative effects of ethanol were reduced, particularly after the third binge when no significant changes in the locomotor activity were apparent between the ethanol-administered male rats and controls. Adolescent rats did differ in their response to ethanol in comparison with adult rats. It was noteworthy that in young female adolescent rats, given 2 g/kg ethanol, motor activity was enhanced, thereby indicating that adolescent female rats are less sensitive to the sedative effects of ethanol at specific doses. In addition, male and female adolescent rats showed little change in locomotor activity in comparison with controls during the third ‘binge administration’ possibly indicating that tolerance to such alcohol doses was occurring. Nicotine administration did prevent the decrease in locomotor activity after ethanol administration during the first binge regimen in both male and female adolescents as well as adult female rats. However, after the third binge, such alcohol-induced changes in motor activity were not so well defined in the female adult rats that now showed significant decreases in motor activity. In contrast, adolescent male and female rats still showed similar motor activity to that of the controls. No clear association between the NAc glutamate extracellular content and locomotor activity was discernible in either adult or adolescent rats in these present studies. However, chronic nicotine administration markedly reduced the elevated basal glutamate content in the ‘binge drinking female’ adult rats. Conclusions: These studies have shown clear and distinct differences, with respect to both sensitivity and tolerance, in adult and adolescent male and female rats, which could be modified by supplementation with nicotine.


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