Assessment of abuse potential of carfentanil

Author:

Wei Jiayun123,Lai Miaojun4,Li Feng12,Chen Yuanyuan12,Li Xiangyu25,Qiu Yi6,Shen Haowei7,Xu Peng125,Di Bin12

Affiliation:

1. School of Pharmacy China Pharmaceutical University Nanjing China

2. Office of China National Narcotics Control Commission China Pharmaceutical University Joint Laboratory on Key Technologies of Narcotics Control Beijing China

3. Zhejiang Xiaoshan Hospital Hangzhou China

4. Laboratory of Behavioral Neuroscience, Key Laboratory of Addiction Research of Zhejiang Province Ningbo Kangning Hospital Ningbo China

5. Key Laboratory of Drug Monitoring and Control, Drug Intelligence and Forensic Center Ministry of Public Security Beijing China

6. National Institute on Drug Dependence Peking University Beijing China

7. Faculty of Physiology and Pharmacology, School of Medicine Ningbo University Ningbo China

Abstract

AbstractCarfentanil, as a fentanyl analogue, is a potent synthetic opioid. It has been controlled in many countries, and its emergence has been highlighted by many recent reports. However, although discriminative stimulus effects of carfentanil in rats had been reported, its abuse potential has not been fully evaluated. In this study, we evaluated the abuse potential of carfentanil via the tests of conditioned place preference (CPP), drug self‐administration and naloxone‐precipitated opioid withdrawal assay, compared with fentanyl and heroin. Carfentanil exhibited significant place preference at a minimum dose of 1 μg/kg in mice, whereas fentanyl and heroin induced significant place preference at the minimum doses of 100 μg/kg and 1000 μg/kg, respectively. In the drug‐substitution test in heroin self‐administered rats (50 μg/kg/infusion), carfentanil and fentanyl acquired significant self‐administrations above saline levels from 0.05–0.1 and 0.1–10.0 μg/kg/infusion, respectively. Carfentanil induced the maximum number of infusions at 0.1 μg/kg, whereas fentanyl and heroin at 1 and 25 μg/kg, respectively. In short, carfentanil showed the highest potency to induce CPP and self‐administration. Furthermore, repeated treatment with escalating doses of carfentanil, fentanyl or heroin induced typical withdrawal symptoms in mice, including a greater number of jumping and weight loss than saline group. This indicated that carfentanil could produce physical dependence similar to fentanyl and heroin. Taken together, the present study demonstrated the higher abuse potential of carfentanil compared with fentanyl and heroin. The rank order of abuse potential for these compounds is carfentanil > fentanyl > heroin.

Publisher

Wiley

Subject

Psychiatry and Mental health,Pharmacology,Medicine (miscellaneous)

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