Glenn W. Stevenson scite author profile

Agonists at ␦, , and opioid receptors produce interacting effects in rodents and nonhuman primates. To further evaluate the determinants of these interactions, this study examined the effects of mixtures of ␦ ϩ and ␦ ϩ agonists in rhesus monkeys (n ϭ 4 -5) using two behavioral procedures, an assay of schedulecontrolled responding for food reinforcement and an assay of thermal nociception. Results were analyzed using dose-addition analysis. In the assay of schedule-controlled responding, the; the agonists methadone, fentanyl, morphine, and nalbuphine; and the agonists (5␣,7␣,8␤)-(Ϫ)-N-methyl-N-(7-(1-pyrrolidinyl)-1-oxaspiro(4,5)dec-8-yl) benzeneacetamide (U69,593) and bremazocine all dose dependently decreased rates of food-maintained responding when administered alone. Fixed ratio mixtures of SNC80 ϩ agonists produced additive or subadditive effects, whereas SNC80 ϩ agonist mixtures produced only additive effects. In the assay of thermal nociception, SNC80 produced no measurable effects when administered alone, whereas and agonists produced dose-dependent antinociception. SNC80 ϩ agonist mixtures produced superadditive effects manifested as leftward shifts in agonist dose-effect curves. This synergism was antagonized by the ␦-selective antagonist naltrindole, suggesting that SNC80-induced enhancement of agonist antinociception was ␦ receptor-mediated. SNC80 did not enhance the antinociceptive effects of the highly selective agonist U69,593, and it produced only a marginal enhancement of antinociception produced by the less selective agonist bremazocine. These results suggest that ␦ agonists may selectively enhance the antinociceptive effects of agonists in rhesus monkeys. These results also confirm that opioid agonist interactions may depend on the receptor selectivity and relative doses of the agonists and on the experimental endpoint.Biochemical and behavioral evidence indicates the existence of three opioid receptor types, the ␦, , and receptors (Martin et al., 1976;Lord et al., 1977;Evans et al., 1992;Thompson et al., 1993;Yasuda et al., 1993). Agonists selective for ␦, , and receptors produce distinct profiles of physiological and behavioral effects (Gutstein, 2001). In addition, selective ␦, , and agonists may also produce interacting effects. Studies of opioid receptor interactions have been conducted primarily with ␦ and agonists in rodents using assays of antinociception, and results from these studies suggest that the nature of the interaction depends on such variables as the particular agonists used, the relative doses tested, and the behavioral endpoint (Heyman et al., 1989;Jiang et al., 1990;Adams et al., 1993). For example, the peptidic ␦ agonists [D-Pen 2 ,D-Pen 5 ]-enkephalin (DPDPE) and deltorphin II enhanced the effects of some intermediate-efficacy agonists (morphine, normorphine, and codeine), but not of higher efficacy -agonists (PL017, fentanyl, or sufentanil), in an assay of thermal nociception in mice (Heyman et al., 1989;Jiang et al., 1990). In a subsequent study, DPDPE enhanced ...

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Targeting Pain-Suppressed Behaviors in Preclinical Assays of Pain and Analgesia: Effects of Morphine on Acetic Acid-Suppressed Feeding in C57BL/6J Mice

Stevenson¹,

Bilsky²,

Negus³

2006

The Journal of Pain

101

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Mu/kappa opioid interactions in rhesus monkeys: Implications for analgesia and abuse liability.

Negus¹,

Schrode²,

Stevenson³

2008

Experimental and Clinical Psychopharmacology

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Mu opioid receptor agonists are clinically valuable as analgesics; however, their use is limited by high abuse liability. Kappa opioid agonists also produce antinociception, but they do not produce mu agonist-like abuse-related effects, suggesting that they may enhance the antinociceptive effects and/or attenuate the abuse-related effects of mu agonists. To evaluate this hypothesis, the present study examined interactions between the mu agonist fentanyl and the kappa agonist U69,593 in three behavioral assays in rhesus monkeys. In an assay of schedule-controlled responding, monkeys responded under a fixed-ratio 30 (FR 30) schedule of food presentation. Fentanyl and U69,593 each produced rate-decreasing effects when administered alone, and mixtures of 0.22:1, 0.65:1 and 1.96:1 U69,593/fentanyl usually produced subadditive effects. In an assay of thermal nociception, tail withdrawal latencies were measured from water heated to 50°C. Fentanyl and U69,593 each produced dose-dependent antinociception, and effects were additive for all mixtures. In an assay of drug selfadministration, rhesus monkeys responded for i.v. drug injection, and both dose and FR values were manipulated. Fentanyl maintained self-administration, whereas U69,593 did not. Addition of U69,593 to fentanyl produced a proportion-dependent decrease in both rates of fentanyl selfadministration and behavioral economic measures of the reinforcing efficacy of fentanyl. Taken together, these results suggest that simultaneous activation of mu and kappa receptors, either with a mixture of selective drugs or with a single drug that targets both receptors, may reduce abuse liability without reducing analgesic effects relative to selective mu agonists administered alone.

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Interactions between δ and μ Opioid Agonists in Assays of Schedule-Controlled Responding, Thermal Nociception, Drug Self-Administration, and Drug versus Food Choice in Rhesus Monkeys: Studies with SNC80 [(+)-4-[(αR)-α-((2S,5R)-4-Allyl-2,5-dimethyl-1-piperazinyl)-3-methoxybenzyl]-N,N-diethylbenzamide] and Heroin

Stevenson

Folk²,

Rice³

et al. 2005

J Pharmacol Exp Ther

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Interactions between ␦ and opioid agonists in rhesus monkeys vary as a function of the behavioral endpoint. The present study compared interactions between the ␦ agonist SNC80 [(ϩ)-4-[(␣R)-␣-((2S,5R)-4-allyl-2,5-dimethyl-1-piperazinyl)-3-methoxybenzyl]-N,N-diethylbenzamide] and the agonist heroin in assays of schedule-controlled responding, thermal nociception, and drug self-administration. Both SNC80 (ED 50 ϭ 0.43 mg/kg) and heroin (ED 50 ϭ 0.088 mg/kg) produced a dose-dependent and complete suppression of response rates in the assay of schedule-controlled responding. Heroin also produced thermal antinociception (ED 5°C ϭ 0.18 mg/kg) and maintained drug self-administration under both a fixed ratio schedule [dose-effect curve peak at 0.0032 mg/kg/injection (inj)] and under a food versus heroin concurrent-choice schedule (ED 50 ϭ 0.013 mg/kg/inj), whereas SNC80 did not produce thermal antinociception or maintain self-administration. Fixed ratio mixtures of SNC80 and heroin (1.6:1, 4.7:1, and 14:1 SNC80/heroin) produced additive effects in the assay of schedule-controlled responding and superadditive effects in the assay of thermal nociception. Also, SNC80 did not enhance the reinforcing effects of heroin, indicating that mixtures of SNC80 and heroin produced additive or infra-additive reinforcing effects. These results provide additional evidence to suggest that ␦/ interactions depend on the experimental endpoint and further suggest that ␦ agonists may selectively enhance the antinociceptive effects of agonists while either not affecting or decreasing the sedative and reinforcing effects of agonists.Biochemical and behavioral evidence indicates the existence of three opioid receptor types, the ␦, , and receptors (Martin et al., 1976;Lord et al., 1977;Evans et al., 1992). Agonists selective for ␦, , and receptors produce distinct profiles of physiological and behavioral effects (Gutstein, 2001). In addition, selective ␦, , and agonists may also produce interacting effects. Studies of opioid receptor interactions in rodents and nonhuman primates have been conducted primarily with ␦ and agonists using assays of nociception, and results from these studies suggest that ␦ agonists enhance the antinociceptive effects of agonists and that this interaction depends on such variables as the species studied, the particular agonists used, the relative doses tested, and the behavioral endpoint (Heyman et al., 1989;Adams et al., 1993;Dykstra et al., 2002;Stevenson et al., 2003).Interactions between ␦ and agonists have also been reported for other behavioral endpoints, such as bladder motility, convulsions, Straub tail, respiratory depression, and sedation (Sheldon et al., 1989;O'Neill et al., 1997;Su et al.,

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