Enadoline, a selective kappa opioid agonist: comparison with butorphanol and hydromorphone in humans

Adult Male Analysis of Variance Cross-Over Studies Pyrrolidines Dose-Response Relationship, Drug Heroin Dependence Receptors, Opioid, kappa Pilot Projects Middle Aged 3. Good health Analgesics, Opioid 03 medical and health sciences Neuroprotective Agents 0302 clinical medicine Butorphanol Double-Blind Method Humans Hydromorphone Female Benzofurans
DOI: 10.1007/s002130100788 Publication Date: 2003-03-05T19:14:55Z
ABSTRACT
The availability of the highly selective and specific kappa opioid agonist enadoline provides an opportunity to explore the function of kappa receptors in humans and their potential utility as a target for substance abuse pharmacotherapy development.The purpose of this study was to characterize the pharmacodynamic effects of enadoline, a selective kappa agonist, and to compare it with butorphanol, a mixed mu/kappa agonist, and hydromorphone, a mu agonist, in humans.Pilot evaluation (n=3) served to establish intramuscular doses of enadoline (20, 40, 80, and 160 microg/70 kg), butorphanol (1.5, 3, 6, and 12 mg/70 kg), and hydromorphone (1.5, 3, and 6 mg/70 kg) of comparable activity. These acute doses were examined under double-blind, placebo-controlled and constrained randomized conditions with a minimum of 72 h between tests in volunteers with polysubstance abuse histories (n=6). Physiological and subject- and observer-rated measures were collected 30 min before and for 4 h after administration.Enadoline significantly increased measures of sedation, confusion and dizziness, produced visual distortions and feelings of depersonalization, and increased urinary output. The highest dose (160 microg/70 kg) was not tolerated and led to psychotomimetic effects. Hydromorphone produced prototypic mu opioid effects including respiratory depression, miosis, and euphoria. Butorphanol was most similar to hydromorphone and shared few effects with enadoline.These results are discussed with respect to the potential use and safety of kappa agonists for clinical indications.
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