Selective mu and delta, but not kappa, opiate receptor antagonists inhibit
the habituation of novelty-induced hypoalgesia in the rat
by
Spreekmeester E, Rochford J
Douglas Hospital Research Center,
Department of Psychiatry,
McGill
University,
Verdun, Quebec, Canada.
Psychopharmacology (Berl) 2000 Jan; 148(1):99-105
ABSTRACT
RATIONALE: There is now extensive evidence demonstrating that exposure to
novel stimuli induces hypoalgesia and that this effect habituates over repeated
exposure to the stimuli. Moreover, it has been shown that administration of the
nonselective opiate receptor antagonist naloxone can attenuate the rate of
habituation of novelty-induced hypoalgesia. OBJECTIVES: The present experiments
were conducted to determine the relative influence of different opiate receptor
subtypes in the attenuation of the habituation of novelty-induced hypoalgesia.
METHODS: In experiments 1-3, different groups of male, Wistar rats (275-300 g)
were administered vehicle, 0. 5, 1.0 or 2.0-nmol doses of the mu-selective
antagonist Cys(2)-Tyr(3)-Orn(5)-Pen(7)-amide (CTOP), the delta-receptor
selective antagonist naltrindole, or the kappa-selective antagonist
nor-binaltorphimine (nor-BNI). In experiment 4, animals were administered
vehicle, 5, 25 or 75-nmol doses of nor-BNI. All injections were delivered to the
right lateral ventricle 30 min prior to exposure to a novel hot-plate apparatus
(48.5 degrees C), once a day for eight consecutive days. RESULTS: Paw-lick
latencies in vehicle-treated animals were long during the initial exposures and
declined over repeated tests, suggesting the habituation of novelty-induced
hypoalgesia. The rate of habituation was significantly attenuated by
administration of 1.0-nmol and 2.0-nmol doses of CTOP, by a 2.0-nmol dose of
naltrindole, but was unaffected by all doses of nor-BNI. CONCLUSIONS: These
results support the involvement of the mu and delta, but not the kappa, opiate
receptor subtypes in the habituation of novelty-induced hypoalgesia.
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