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Vol. 298, Issue 1, 156-164, July 2001
Department of Pharmacology, Emory University School of Medicine,
Atlanta, Georgia
Pretreatment with morphine-like agonists potentiates the behavioral
effects of opioid antagonists, possibly reflecting a state of acute
physical dependence. Several studies have used operant behavior to
quantify these effects. However, little research has been done using
unconditioned behavior. One objective of this study was to determine
whether opioid agonist pretreatment (e.g., morphine, fentanyl, and
meperidine) potentiated naltrexone-induced suppression of water
consumption following deprivation. Another objective was to determine
whether the agonist pretreatment interval was functionally related to
efficacy for the manifestation of acute dependence. Finally, we
compared temporally the effects of the three agonists. Adult male
Sprague-Dawley rats were water deprived for 18, 20, or 22 h and
given an injection (s.c.) of an agonist or saline. After 1.75, 3.75, or
5.75 h, animals received a single dose (s.c.) of naltrexone
(0.01-30 mg/kg) or saline. Fifteen minutes later, subjects had access
to water for 30 min. A time course of antinociception was constructed
after agonist administration, using the tail-flick procedure. All three
agonists dose dependently potentiated naltrexone-induced drinking
suppression, decreasing the ED50 of naltrexone by as much
as 150-fold. There was no clear relationship between agonist efficacy
and pretreatment interval. Sensitization to naltrexone was seen up to
6 h after agonist administration, occurring in the apparent
absence of an antinociceptive effect. These data extend the range of
behavioral effects of opioid antagonists potentiated by opioid agonist
pretreatment to suppression of drinking and show that such potentiation
can occur in the absence of a prototypical agonist effect.
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