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Vol. 302, Issue 1, 101-110, July 2002
Department of Psychology, Wayne State University, Detroit, Michigan
High doses of insurmountable antagonists or frequent administration of
high doses of agonists are required to alter the potency of opioid
agonists to produce discriminative stimuli. In the present study,
insurmountable antagonism and repeated agonist treatment were combined
to remove or disable a large enough proportion of µ-opioid receptors
to alter the potency or maximal effect for four agonists in male
Sprague-Dawley rats trained to discriminate 3.2 mg/kg morphine from
saline under a fixed-ratio 15 schedule of food reinforcement. All
agonists produced 88 to 100% morphine responding and were
differentially sensitive to clocinnamox antagonism (fentanyl < morphine
buprenorphine = nalbuphine). Repeated treatment with 20 mg/kg per day morphine for 6 days decreased by 2- to 3-fold the
potency of fentanyl, morphine, and buprenorphine to produce morphine
responding. After morphine treatment, 3.2 mg/kg clocinnamox produced a
7-fold further decrease in morphine potency. Clocinnamox (10 mg/kg)
produced a 7- and 12-fold further decrease in morphine and fentanyl
potency, respectively, a reduction in the slope of the morphine
dose-response curve, and a suppression of the maximal morphine
responding for buprenorphine. Repeated treatment with 10 mg/kg per day
morphine for 6 days failed to alter the potency of nalbuphine to
produce morphine responding. In these morphine-treated rats, doses of
3.2 or 10 mg/kg clocinnamox suppressed the maximal morphine responding.
Taken together, these data indicate that combined insurmountable
antagonist and repeated agonist treatment produce additive effects at
µ-opioid receptors to diminish discriminative stimulus effects in a
manner predicted by the relative efficacy of opioid agonists.
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