Discriminative stimulus and locomotor effects of para-substituted and benzofuran analogs of amphetamine

Dolan, Sean B.; Forster, Michael J.; Gatch, Michael B.

doi:10.1016/j.drugalcdep.2017.07.041

Cited by 21 publications

(16 citation statements)

References 31 publications

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“…Other compounds with psychostimulant-like effects also decrease locomotor activity, although most of them (MDMA, flephedrone, MDAI, and DMAA) produce rebound stimulant effects later in the time course (Dolan and Gatch, 2015;Gatch et al, 2013;2016). 4-Fluoroamphetamine (4-FA) did produce depressant effects with little or no rebound stimulant effects (Dolan et al, 2017) similar to those produced by TH-PVP in the present study. None of these compounds are selectively dopaminergic, as MDMA and MDAI produce both serotonergically and dopaminergically mediated effects and DMAA produces its effects primarily through adrenergic receptors (Monte et al, 1993;Iversen et al, 2013).…”

Section: Discussionsupporting

confidence: 58%

Locomotor activity and discriminative stimulus effects of five novel synthetic cathinone analogs in mice and rats

Gatch

Dolan

Forster

2019

Drug and Alcohol Dependence

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Background: The development of novel synthetic psychoactive substances continues to accelerate. There are little or no data on the pharmacological mechanisms, behavioral effects, or abuse liability of many of the newer compounds, despite increasing reports of severe adverse effects in recreational users. Methods: The current study investigated the discriminative stimulus and locomotor stimulant effects of a group of synthetic cathinone analogs: N-ethylpentylone, dimethylone, dibutylone, clephedrone, 3',4'-tetramethylene-α-pyrrolidinovalerophenone (TH-PVP). Locomotor activity was assessed in an open-field assay using Swiss-Webster mice. Discriminative stimulus effects were assessed in Sprague-Dawley rats trained to discriminate either cocaine, methamphetamine or MDMA from vehicle. Results: N-ethylpentylone, dimethylone, dibutylone and clephedrone increased locomotor activity. Maximal effects were similar among the test compounds. Relative potencies were: methamphetamine>N-ethylpentylone>clephedrone> dimethylone>MDMA> cocaine>dibutylone. TH-PVP dose-dependently depressed locomotor activity. N-ethylpentylone, dimethylone, dibutylone and clephedrone substituted fully for the discriminative stimulus effects of methamphetamine. N-ethylpentylone, dibutylone and clephedrone fully substituted for cocaine, whereas dimethylone produced a maximum of 67% drug-appropriate responding. Dimethylone, dibutylone and clephedrone fully substituted for MDMA, whereas N-ethylpentylone produced only 50% drug-appropriate responding. TH-PVP produced a maximum of 38% methamphetamine-appropriate responding, 50% cocaine-appropriate responding, and less than 1% MDMA-appropriate responding.

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Section: Discussionsupporting

confidence: 58%

Locomotor activity and discriminative stimulus effects of five novel synthetic cathinone analogs in mice and rats

Gatch

Dolan

Forster

2019

Drug and Alcohol Dependence

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“…However, given that response rate was similarly reduced in the discrimination studies as the locomotor studies, it seems feasible that comparable processes are occurring in both rats and mice. In addition, there are strong correlations between ED50s in the locomotor activity assay and the drug discrimination assay across psychostimulants (Carroll et al, 2009; Gatch et al, 2013; 2015; Katz et al, 2001) and other compounds with psychostimulant-like discriminative stimulus effects, such as the supplement dimethylamylamine (Dolan and Gatch, 2015), 4-fluoroamphetamine (Dolan et al, 2017), and MDAI (Gatch et al, 2016) also decrease locomotor activity.…”

Section: Discussionmentioning

confidence: 99%

Impure but not inactive: Behavioral pharmacology of dibenzylpiperazine, a common by-product of benzylpiperazine synthesis

et al. 2018

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“…A recent study regarding the effects of the benzofurans 5‐APB and 6‐APDB on discriminative stimulus and behavior of rodents concluded that these drugs increase locomotor activity and fully substitute for MDMA, indicating that they might share an abuse pattern with this classic club drug (Dolan, Forster, & Gatch, ). Another recent work on the dependence liability of 5‐APB in rodents concluded that this benzofuran elicited increases in conditioned place preference but did not facilitate self‐administration, suggesting that 5‐APB has rewarding effects, rather than reinforcing effects (Cha et al, ).…”

Section: Subjective Effects In Humans and Other Biological Effectsmentioning

confidence: 99%

“…Both benzofurans elicited a time‐ and dose‐dependent stimulation of horizontal activity in the animals, with an increase in the duration of stimulation accompanying the dose increase from 1 mg/kg up to 10 mg/kg. A dose of 25 mg/kg caused the depression of activity and delayed the stimulant effect (Dolan et al, ). Therefore, it is possible to expect a significant influence over other pharmacodynamic effects.…”

Section: Influential Factors On Toxicodynamic Effectsmentioning

confidence: 99%

Benzo fury: A new trend in the drug misuse scene

Bravo

Carmo

Carvalho

et al. 2019

J of Applied Toxicology

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Benzofurans, also known by users as benzo fury or benzofury, are synthetic phenethylamines and constitute the third most prominent group of new psychoactive substances (NPS). As the use of these substances has been spread as an alternative to the classic illicit psychostimulants, such as amphetamines, their legal status was reviewed, resulting in an utter prohibition of these NPS in many countries worldwide.Herein, the prevalence of abuse, chemistry, biological effects, metabolism, and the potential harms and risky behaviors associated with the abuse of benzofurans are reviewed. The congeners of this group are mainly consumed recreationally at electronic dance music parties, in polydrug abuse settings. Benzofurans preferentially act by disturbing the functioning of serotonergic circuits, which induces their entactogenic and stimulant effects and is the reason behind the considerable number of recent benzo fury-related deaths. The slight interaction of these drugs with the dopaminergic system justifies the rewarding effects of these drugs. To date, published evidence on the mechanisms of toxicity of benzo fury is very limited but a body of research is now beginning to emerge revealing an alarming public health threat regarding the abuse of these NPS.

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Discriminative stimulus and locomotor effects of para-substituted and benzofuran analogs of amphetamine

Cited by 21 publications

References 31 publications

Locomotor activity and discriminative stimulus effects of five novel synthetic cathinone analogs in mice and rats

Locomotor activity and discriminative stimulus effects of five novel synthetic cathinone analogs in mice and rats

Impure but not inactive: Behavioral pharmacology of dibenzylpiperazine, a common by-product of benzylpiperazine synthesis

Benzo fury: A new trend in the drug misuse scene

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