Literature DB >> 19443130

Route of administration influences substitution patterns in rats trained to discriminate methadone vs. vehicle.

Robert E Vann1, Laura E Wise, Stephen A Varvel, Scott D Philibin, D Matthew Walentiny, Joseph H Porter.   

Abstract

Replacement therapy with the synthetic mu-opioid agonist methadone is an efficacious treatment for opioid abuse. While much is known about methadone's pharmacology, its discriminative stimulus properties remain largely unexplored. The present study sought to establish methadone discrimination in rats. Moreover, some research suggests that route of administration alters the discriminative stimulus of methadone. Thus, the present study also compared intraperitoneal (i.p.) and subcutaneous (s.c.) routes of administration. Male Sprague-Dawley rats were trained to discriminate 3.0mg/kg methadone (i.p.) from vehicle in a two-lever discrimination procedure. Generalization tests were conducted with a variety of compounds administered i.p. and s.c. Methadone fully substituted for itself, yielding ED(50)s of 1.5mg/kg (i.p.) and 0.2mg/kg (s.c.). Naltrexone (i.p.), an opioid antagonist produced a dose-dependent reduction in methadone-appropriate responding. The methadone stereoisomers fully substituted for methadone when given s.c.; however, when administered i.p., (+) and (-) methadone produced partial and no substitution, respectively. Heroin fully generalized to methadone regardless of administration route, while morphine fully substituted when given s.c., but not i.p. The kappa-agonist U50-488 failed to generalize to methadone with either route of administration. These results demonstrated that methadone's discriminative stimulus is mediated through mu-opioid receptor activity and is similar to that of commonly abused opioids (heroin, morphine). Additionally, route of administration produced differential results for many of the drugs tested, suggesting decreased drug bioavailability following i.p. administration due to hepatic first pass metabolism. Taken together, these results suggest that methadone's shared subjective effects with abused opioids, as well as its unique metabolic properties contribute to its efficacy in opioid maintenance therapy.

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Year:  2009        PMID: 19443130      PMCID: PMC3386854          DOI: 10.1016/j.drugalcdep.2009.02.015

Source DB:  PubMed          Journal:  Drug Alcohol Depend        ISSN: 0376-8716            Impact factor:   4.492


  28 in total

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Journal:  Drug Alcohol Depend       Date:  2000-12-22       Impact factor: 4.492

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  1 in total

1.  Characterization of methadone as a β-arrestin-biased μ-opioid receptor agonist.

Authors:  Seira Doi; Tomohisa Mori; Naoki Uzawa; Takamichi Arima; Tomoyuki Takahashi; Masashi Uchida; Ayaka Yawata; Michiko Narita; Yasuhito Uezono; Tsutomu Suzuki; Minoru Narita
Journal:  Mol Pain       Date:  2016-06-17       Impact factor: 3.395

  1 in total

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