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Vol. 291, Issue 1, 390-398, October 1999
Department of Pharmacology and Toxicology, Medical College of
Virginia of Virginia Commonwealth University, Richmond, Virginia
Metanicotine
[N-methyl-4-(3-pyridinyl)-3-butene-1-amine], a novel
neuronal nicotinic agonist, was found to bind with high affinity
(Ki = 24 nM) to rat brain
[3H]nicotine binding sites and it generalized to nicotine
in a dose-dependent manner in the drug discrimination procedure.
Metanicotine produced significant antinociceptive effects in mice and
rats subjected to either acute thermal (tail-flick), mechanical
(paw-pressure), chemical (para-phenylquinone),
persistent (Formalin), and chronic (arthritis) pain stimuli.
Metanicotine was about 5-fold less potent than nicotine in the
tail-flick test after s.c administration, but slightly more potent
after central administration. Its duration of action was longer than
that of nicotine. Nicotinic antagonists, mecamylamine and
dihydro-
-erythroidine, blocked metanicotine-induced antinociception
in the different pain models. However, the antinociceptive effect was
not affected by pretreatment with either naloxone or by atropine,
confirming that metanicotine exerts its antinociceptive effect via
nicotinic rather than either opioid or muscarinic mechanisms. In
contrast to nicotine, antinociceptive effects of metanicotine were
observed at doses that had virtually no effect on spontaneous activity
and body temperature in mice. These data indicate that metanicotine is
a centrally acting neuronal nicotinic agonist with preferential
antinociceptive effects in animals. Thus, metanicotine and related
nicotinic agonists may have great potential for development as a new
class of analgesics.
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