Self-administration and behavioral economics of second-generation synthetic cathinones in male rats

Huskinson, Sally L.; Naylor, Jennifer E.; Townsend, E. Andrew; Rowlett, James K.; Blough, Bruce E.; Freeman, Kevin B.

doi:10.1007/s00213-016-4492-6

Cited by 44 publications

(39 citation statements)

References 29 publications

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“…The present study characterized the reinforcing effects of four second-generation cathinones, and found that responding for each of these cathinones was rapidly acquired and not different from previous reports for the first-generation cathinone, MDPV (Gannon et al 2017b). Although self-administration of α-PVP (DEA Schedule I) has previously been described (Aarde et al, 2015a; Gannon et al, 2017c; Huskinson et al, 2017), these studies provide new and important information about the reinforcing effects of MDPBP, MDPPP, and α-PPP, and suggest that they each possess a high potential for abuse. In addition, all four of these synthetic cathinones established high levels of drug intake and/or compulsive-like patterns of responding during post-infusion timeouts in a subset of rats.…”

Section: Discussionmentioning

confidence: 88%

“…In rodents, MDPV, α-PVP, α-PPP, and MDPBP have been shown to increase locomotor activity and produce cocaine-, methamphetamine-, and MDMA-like discriminative stimulus effects (e.g., Collins et al, 2016; Fantegrossi et al, 2013; Gannon et al, 2016; Gatch et al, 2013, 2015, 2017; Naylor et al, 2015). MDPV and α-PVP have also been shown to facilitate intracranial self-stimulation and maintain self-administration in rats, suggesting that they function as reinforcers (e.g., Aarde et al, 2015a; 2015b; Gannon et al, 2017a; 2017b; 2017c; Huskinson et al, 2017; Watterson et al, 2014a, 2014b). Additionally, it has been shown that a subset of rats trained to self-administer MDPV (but not cocaine) develop a persistent “high-responder” phenotype, characterized by high levels of drug intake and increased responding during post-infusion timeouts (Gannon et al, 2017b), an effect that may be related to the selective actions of MDPV at DAT relative to SERT (SERT/DAT ~100-800) (Baumann et al, 2013; Eshleman et al, 2013; Simmler et al, 2013).…”

Section: Introduction1mentioning

confidence: 99%

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Relative reinforcing effects of second-generation synthetic cathinones: Acquisition of self-administration and fixed ratio dose-response curves in rats

et al. 2018

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"Bath salts" preparations contain synthetic cathinones which interact with monoamine transporters and function as either monoamine uptake inhibitors or releasers. 3,4-Methylenedioxypyrovalerone (MDPV), 3,4-methylenedioxymethcathinone (methylone), and 4-methylmethcathinone (mephedrone) were three of the most common cathinones (i.e., "first-generation" cathinones); however, after the US Drug Enforcement Administration placed them under Schedule I regulations, they were replaced with structurally related cathinones that were not subject to regulations (i.e., "second-generation" cathinones). Although the reinforcing effects of some second-generation cathinones have been described (e.g., α-pyrrolidinopentiophenone [α-PVP]), little is known about how structural modifications, particularly those involving the methylenedioxy moiety and α-alkyl side chain, impact the abuse liability of other second-generation cathinones (e.g., α-pyrrolidinopropiophenone [α-PPP], 3,4-methylenedioxy-α-pyrrolidinobutiophenone [MDPBP], and 3,4-methylenedioxy-α-pyrrolidinopropiophenone [MDPPP]). The present study used male Sprague-Dawley rats (n = 12 per drug) to directly compare: (1) the acquisition of responding for α-PVP (0.032 mg/kg/inf), α-PPP (0.32 mg/kg/inf), MDPBP (0.1 mg/kg/inf), and MDPPP (0.32 mg/kg/inf) under a fixed ratio (FR) 1 schedule of reinforcement; and (2) full dose-response curves for each drug to maintain responding under an FR5 schedule of reinforcement. The average number of days (∼4 days) and percentage (100%) of rats that acquired self-administration was similar for each drug. The observed rank order potency to maintain responding under an FR5 schedule of reinforcement (α-PVP ≈ MDPBP>α-PPP > MDPPP) is consistent with their potencies to inhibit dopamine uptake. These are the first studies to report on the reinforcing effects of the unregulated second-generation cathinones MDPBP, MDPPP, and α-PPP and indicate all three compounds are readily self-administered, suggesting each possesses high potential for abuse. This article is part of the Special Issue entitled 'Designer Drugs and Legal Highs.'

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Section: Discussionmentioning

confidence: 88%

Section: Introduction1mentioning

confidence: 99%

Relative reinforcing effects of second-generation synthetic cathinones: Acquisition of self-administration and fixed ratio dose-response curves in rats

et al. 2018

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“…Intravenous catheters were implanted and maintained as described previously (Huskinson et al 2017). Rats were allowed to recover for 5–7 days following surgery.…”

Section: Methodsmentioning

confidence: 99%

Effects of nalfurafine on the reinforcing, thermal antinociceptive, and respiratory-depressant effects of oxycodone: modeling an abuse-deterrent opioid analgesic in rats

et al. 2017

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Rationale Strategies to reduce the misuse of mu opioid agonists are critically needed. Previous work has shown that kappa opioid agonists can diminish the abuse-related effects and augment the antinociceptive effects of mu agonists. However, use of traditional kappa agonists is limited by their dysphoric side effects. Objectives The current study examined the effects of nalfurafine, a clinically available atypical kappa agonist, on the reinforcing, thermal antinociceptive, and respiratory depressant effects of oxycodone in male rats. Methods To determine oxycodone:nalfurafine mixture proportions to be examined intravenously across procedures, a progressive-ratio (PR) self-administration procedure compared the reinforcing effects of oxycodone (56 μg/kg/inj) available alone or as a mixture with co-administered nalfurafine (0.32, 1, or 3.2 μg/kg/inj), corresponding to oxycodone:nalfurafine proportions of 175:1, 56:1 and 18:1, respectively. Next, PR and thermal antinociception dose-effect functions were each determined for oxycodone, nalfurafine, and the same oxycodone:nalfurafine mixture proportions. Finally, the respiratory depressant effects of equi-antinociceptive doses of oxycodone, nalfurafine, and the mixtures were compared. Results Nalfurafine decreased the reinforcing effects of oxycodone, and the 18:1 mixture did not function as a reinforcer. Oxycodone and nalfurafine each produced dose-dependent antinociception, and the mixtures produced additive antinociception. In addition, antinociceptive doses of the 56:1 and 18:1 mixtures did not produce respiratory depression. Conclusions These results suggest that nalfurafine may augment the thermal antinociceptive effects while reducing the reinforcing and respiratory depressant effects of oxycodone.

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“…Thirty-five Sprague-Dawley rats (18 males, 17 females) were acquired at 10 weeks of age (Envigo Laboratories, Frederick, MD, USA) and surgically implanted with custom-made jugular catheters and vascular access ports (Instech, Plymouth Meeting, PA, USA) as described previously [27]. Rats were singly housed in a temperature-and humidity-controlled vivarium that was maintained on a 12-h light/dark cycle (lights off at 6:00 p.m.).…”

Section: Subjectsmentioning

confidence: 99%

Sex differences in opioid reinforcement under a fentanyl vs. food choice procedure in rats

Townsend

Negus

Caine

et al. 2019

Neuropsychopharmacol.

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Clinical evidence suggest that men are more sensitive than women to the abuse-related effects of mu-opioid agonists. In contrast, preclinical studies suggest the opposite sex difference. The aim of the present study was to clarify this discrepancy using a fentanyl vs. diluted Ensure ® choice procedure to assess sex differences in opioid reinforcement. Sex differences in intravenous (IV) fentanyl self-administration were examined under a fixed-ratio (FR5) schedule, a multi-day progressive-ratio (PR) schedule for behavioral economic analysis, and a concurrent (choice) schedule of fentanyl and diluted Ensure ® reinforcement in Sprague-Dawley male and female rats. The fentanyl dose-effect function under the FR5 schedule was significantly shifted upward in females compared to males. Similarly, the reinforcing effectiveness of both fentanyl (3.2 and 10 µg/kg per injection, IV) and diluted Ensure ® (18 and 56%) were greater in females than in males as assessed using behavioral economic analysis, irrespective of dose or concentration. However, under a fentanyl vs. foodchoice procedure, males chose 3.2 µg/kg per injection fentanyl injections over 18%, but not 56%, diluted Ensure ® at a higher percentage compared to females. Overall, these results suggest that the expression of sex differences in opioid reinforcement depends upon the schedule of reinforcement and that preclinical opioid vs. food choice procedures provide a translationally relevant measure (i.e., behavioral allocation) consistent with the direction of sex differences reported in the clinical literature.

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Self-administration and behavioral economics of second-generation synthetic cathinones in male rats

Cited by 44 publications

References 29 publications

Relative reinforcing effects of second-generation synthetic cathinones: Acquisition of self-administration and fixed ratio dose-response curves in rats

Relative reinforcing effects of second-generation synthetic cathinones: Acquisition of self-administration and fixed ratio dose-response curves in rats

Effects of nalfurafine on the reinforcing, thermal antinociceptive, and respiratory-depressant effects of oxycodone: modeling an abuse-deterrent opioid analgesic in rats

Sex differences in opioid reinforcement under a fentanyl vs. food choice procedure in rats

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