TY - JOUR
T1 - Acute and chronic bupropion treatment does not prevent morphine-induced conditioned place preference in mice
AU - McKendrick, Greer
AU - Sharma, Sonakshi
AU - Sun, Dongxiao
AU - Randall, Patrick A.
AU - Graziane, Nicholas M.
N1 - Funding Information:
We thank Dr. Diane McCloskey for edits and comments pertaining to this manuscript. We thank Dr. Jennifer Zampogna for her thoughts on bupropion as a potential treatment for the prevention of opioid drug craving. Also, we thank the Mass Spectrometry and Proteomics Core Facility at Penn State College of Medicine for performing analysis of bupropion concentrations in mouse serum. This project is supported by the NARSAD Young Investigator Award (27364; NG) and by the Pennsylvania Department of Health using Tobacco CURE Funds.
Funding Information:
(−)-morphine sulfate pentahydrate was provided by the National Institute on Drug Abuse (NIDA) Drug Supply Program. Bupropion hydrochloride (B102) and (±)-Bupropion-D9 hydrochloride solution (100 μg/ml methanol) (B-052-1 ml) were purchased from Sigma-Aldrich (St. Louis, MO). JHW 007 hydrochloride (Cat. # 4351) was purchased from Tocris (Minneapolis, MN). Formic acid was purchased from J. T. Baker (New Jersey, USA). Optima LC-MS grade water, acetonitrile, methanol, and other chemicals were purchased from Fisher Scientific (New Jersey, USA).
Publisher Copyright:
© 2020 Elsevier B.V.
PY - 2020/12/15
Y1 - 2020/12/15
N2 - A substantial barrier to the treatment of Opioid Use Disorder (OUD) is the elevated relapse rates in affected patients, and a significant contributor to these events of relapse is exposure to cues and contexts that are intensely associated with prior drug abuse. The neurotransmitter dopamine plays a key role in reward-related behaviors, and previous studies have illustrated that dopamine hypofunction in periods of abstinence serves to prompt drug craving and seeking. We hypothesized that restoration of dopaminergic signaling could attenuate drug-seeking behaviors. Therefore, we investigated whether use of an FDA-approved drug, bupropion, an inhibitor of the dopamine transporter (DAT), or a dopamine uptake inhibitor with high affinity for DAT, JHW 007, was able to decrease preference for a drug-paired context. In these experiments, mice underwent 5 days of non-contingent morphine (10 mg/kg) exposure in a conditioned place preference (CPP) paradigm. We found that systemic injection of bupropion (20 mg/kg, i. p.) or intracranial injection of JHW 007 into the nucleus accumbens shell did not prevent the expression of morphine CPP. We then investigated whether chronic bupropion treatment (via implanted osmotic pumps) would influence morphine CPP. We observed that chronic bupropion treatment for 21 days following morphine conditioning did not attenuate the prolonged preference for morphine-paired contexts. Overall, with our dose and paradigm, neither acute nor chronic bupropion diminishes morphine CPP. Continued studies should address FDA-approved medications and their potential for recovery in OUD patients.
AB - A substantial barrier to the treatment of Opioid Use Disorder (OUD) is the elevated relapse rates in affected patients, and a significant contributor to these events of relapse is exposure to cues and contexts that are intensely associated with prior drug abuse. The neurotransmitter dopamine plays a key role in reward-related behaviors, and previous studies have illustrated that dopamine hypofunction in periods of abstinence serves to prompt drug craving and seeking. We hypothesized that restoration of dopaminergic signaling could attenuate drug-seeking behaviors. Therefore, we investigated whether use of an FDA-approved drug, bupropion, an inhibitor of the dopamine transporter (DAT), or a dopamine uptake inhibitor with high affinity for DAT, JHW 007, was able to decrease preference for a drug-paired context. In these experiments, mice underwent 5 days of non-contingent morphine (10 mg/kg) exposure in a conditioned place preference (CPP) paradigm. We found that systemic injection of bupropion (20 mg/kg, i. p.) or intracranial injection of JHW 007 into the nucleus accumbens shell did not prevent the expression of morphine CPP. We then investigated whether chronic bupropion treatment (via implanted osmotic pumps) would influence morphine CPP. We observed that chronic bupropion treatment for 21 days following morphine conditioning did not attenuate the prolonged preference for morphine-paired contexts. Overall, with our dose and paradigm, neither acute nor chronic bupropion diminishes morphine CPP. Continued studies should address FDA-approved medications and their potential for recovery in OUD patients.
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U2 - 10.1016/j.ejphar.2020.173638
DO - 10.1016/j.ejphar.2020.173638
M3 - Article
C2 - 33039460
AN - SCOPUS:85092235402
SN - 0014-2999
VL - 889
JO - European Journal of Pharmacology
JF - European Journal of Pharmacology
M1 - 173638
ER -