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Vol. 283, Issue 1, 200-206, 1997
Laboratory of Behavioral Neuroscience, Department of Psychology,
Boston University, Boston, Massachusetts
Previous studies suggest that magnesium chloride may have
discriminative stimulus effects that partially overlap with those of
noncompetitive N-methyl-D-aspartate antagonists as well as certain monoamine uptake inhibitors. In our study, rats were trained to
discriminate 100 mg/kg magnesium chloride from saline and its discriminative stimulus effects were characterized with respect to
N-methyl-D-aspartate receptor and monoamine transporter
functions in substitution tests. The discriminative stimulus effects of magnesium chloride were acquired within a moderate number of training sessions and showed dose-related substitution after either subcutaneous (3-300 mg/kg) or intracerebroventricular (0.3-300 µg)
administration. The intracerebroventricular administration of magnesium
chloride was over 4000 times more potent than its s.c. administration. The monoamine uptake inhibitors cocaine, GBR 12909, talsupram and
citalopram fully substituted (
90% magnesium-appropriate responses) for magnesium chloride in the majority of subjects tested and the group
averages reached a maximum of 72 to 82% responses on the
magnesium-appropriate lever. Based on relative potency analysis, the
rank order of potency of these four drugs for producing
magnesium-appropriate responses was talsupram = cocaine > citalopram = GBR 12909. The N-methyl-D-aspartate
receptor antagonists dizocilpine, phencyclidine and NPC 17742 engendered maximum group averages of 49 to 65% responses on the
magnesium-appropriate lever. The results suggest that the centrally
mediated discriminative stimulus effects of magnesium chloride may be
more directly related to interactions with monoamine neurotransmitter
functions than to N-methyl-D-aspartate receptor blockade.
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