Methamphetamine-like discriminative stimulus effects of bupropion and its two hydroxy metabolites in male rhesus monkeys

Banks, Matthew L.; Smith, D.; Blough, Bruce E.

doi:10.1097/fbp.0000000000000224

Cited by 7 publications

(1 citation statement)

References 47 publications

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“…Based simply on the close genetic homology of NHPs to humans [59], it is reasonable to expect they would be a superior translational model to understand bupropion CNS disposition and ensuing central effects in humans. However, in vitro metabolite kinetics, and 15 in vivo metabolite disposition in NHPs is limited [51,[60][61][62], and reports of stereoselective analysis are absent. We found that the total percentage of hydroxybupropion, threohydrobupropion, erythrohydrobupropion in marmoset monkey liver microsomes (62%, 23%,14%, respectively) is in good agreement with a previously published report (62%,28%,10%) in baboon hepatic microsomes [60].…”

Section: Discussionmentioning

confidence: 99%

Comparison of In Vitro Stereoselective Metabolism of Bupropion in Human, Monkey, Rat, and Mouse Liver Microsomes

Bhattacharya

Kirby

Stipdonk

et al. 2018

Eur J Drug Metab Pharmacokinet

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Section: Discussionmentioning

confidence: 99%

Comparison of In Vitro Stereoselective Metabolism of Bupropion in Human, Monkey, Rat, and Mouse Liver Microsomes

Bhattacharya

Kirby

Stipdonk

et al. 2018

Eur J Drug Metab Pharmacokinet

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Molecular Mechanisms of Amphetamines

Reith

Gnegy

2019

Handbook of Experimental Pharmacology

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Discriminative Stimulus Properties of S(−)-Nicotine: “A Drug for All Seasons”

Rosecrans

Young

2017

Current Topics in Behavioral Neurosciences

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S(-)-Nicotine is the major pharmacologically active substance in tobacco and can function as an effective discriminative stimulus in both experimental animals and humans. In this model, subjects must detect and communicate the nicotine drug state versus the non-drug state. This review describes the usefulness of the procedure to study nicotine, presents a general overview of the model, and provides some relevant methodological details for the establishment of this drug as a stimulus. Once established, the (-)-nicotine stimulus can be characterized for dose response and time course effects. Moreover, tests can be conducted to determine the similarity of effects produced by test drugs to those produced by the training dose of nicotine. Such tests have shown that the stimulus effects of nicotine are stereoselective [S(-)-nicotine >R(+)-nicotine] and that other "natural" tobacco alkaloids and (-)-nicotine metabolites can produce (-)-nicotine-like effects, but these drugs are much less potent than (-)-nicotine. Stimulus antagonism tests with mecamylamine and DHβE (dihydro-β-erythroidine) indicate that the (-)-nicotine stimulus is mediated via α4β2 nicotinic acetylcholine receptors (nAChRs) in brain; dopamine systems also are likely involved. Individuals who try to cease their use of nicotine-based products are often unsuccessful. Bupropion (Zyban) and varenicline (Chantix) may be somewhat effective as anti-smoking medications because they probably produce stimulus effects that serve as suitable substitutes for (-)-nicotine in the individual who is motivated to quit smoking. Finally, it is proposed that future drug discrimination studies should apply the model to the issue of maintenance of abstinence from (-)-nicotine-based products.

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Methamphetamine-like discriminative stimulus effects of bupropion and its two hydroxy metabolites in male rhesus monkeys

Cited by 7 publications

References 47 publications

Comparison of In Vitro Stereoselective Metabolism of Bupropion in Human, Monkey, Rat, and Mouse Liver Microsomes

Comparison of In Vitro Stereoselective Metabolism of Bupropion in Human, Monkey, Rat, and Mouse Liver Microsomes

Molecular Mechanisms of Amphetamines

Discriminative Stimulus Properties of S(−)-Nicotine: “A Drug for All Seasons”

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