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Vol. 295, Issue 1, 114-124, October 2000
Behavioral Pharmacology Research Unit, Department of Psychiatry and
Behavioral Sciences, The Johns Hopkins University School of Medicine,
Baltimore, Maryland
The purpose of this study was to examine the discrimination of
agonist-antagonist opioids in humans trained in a two-choice hydromorphone/not hydromorphone discrimination. Eight adult male volunteers with histories of opioid abuse who were not currently physically dependent were trained to discriminate the mu receptor agonist hydromorphone (3 mg/70 kg, i.m.) ("Drug A") from a "Not Drug A" training condition (saline placebo). Volunteers received financial reinforcement for correct responses. After training, generalization dose-effect curves for hydromorphone, butorphanol, pentazocine, nalbuphine, and buprenorphine were determined. Other subjective, behavioral, and physiological measures were concurrently collected in all sessions. In generalization testing hydromorphone and
buprenorphine produced dose-related increases in
hydromorphone-appropriate responses. Pentazocine produced an inverted
U-shaped dose-response curve with complete substitution at 32 mg/70 kg
but not at 64 mg/70 kg. Butorphanol and nalbuphine did not completely
substitute for hydromorphone at any dose tested. These results differ
from an earlier two-choice, Drug A versus Drug B (hydromorphone/saline) discrimination study. After Drug/Not Drug instructions the behavioral discriminations of agonist-antagonist opioids were more consistent with
their putative agonist activities at the mu opioid receptor and with
their subjective effects profiles than was the case after Drug A versus
Drug B instructions. These results suggest that instructions are an
important factor in the outcome of human drug discrimination studies.
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