Higher anhedonia during withdrawal from initial opioid exposure is protective against subsequent opioid self-administration in rats

Yayi Swain; Peter Muelken; Annika Skansberg; Danielle Lanzdorf; Zachary Haave; Mark G. LeSage; Jonathan C. Gewirtz; Andrew C. Harris

doi:10.1007/s00213-020-05532-w

Higher anhedonia during withdrawal from initial opioid exposure is protective against subsequent opioid self-administration in rats

Yayi Swain, Peter Muelken, Annika Skansberg, Danielle Lanzdorf, Zachary Haave, Mark G. LeSage, Jonathan C. Gewirtz, Andrew C. Harris

Psychology (Twin Cities)

Research output: Contribution to journal › Article › peer-review

12 Scopus citations

Abstract

Rationale: Understanding factors contributing to individual differences in vulnerability to opioid addiction is essential for developing more effective preventions and treatments, yet few reliable behavioral predictors of subsequent opioid self-administration have been identified in rodents. Sensitivity to the acute effects of initial drug exposure predicts later addiction vulnerability in both humans and animals, but the relationship between sensitivity to withdrawal from initial drug exposure and later drug use vulnerability is unclear. Objective: The goal of the current study was to evaluate whether the degree of anhedonia experienced during withdrawal from early opioid exposure predicts subsequent vulnerability to opioid self-administration. Methods: Rats were first tested for withdrawal sensitivity following acute injections of morphine (i.e., “acute dependence”), measured as elevations in intracranial self-stimulation (ICSS) thresholds (anhedonia-like behavior) during naloxone-precipitated and spontaneous withdrawal. Rats were then tested for addiction-like behavior using various measures of i.v. morphine self-administration (MSA) including acquisition, demand, extinction, and reinstatement induced by morphine, stress, and/or drug-associated cues. Results: Greater naloxone-precipitated withdrawal across repeated morphine injections and greater peak spontaneous withdrawal severity following a single morphine injection were associated with lower addiction-like behavior on multiple MSA measures. Withdrawal-induced anhedonia predicted a wider range of MSA measures than did any individual measure of MSA itself. Conclusions: Our data establish WIA as one of the first behavioral measures to predict individual differences in opioid SA in rodents. This model promises to be useful for furthering our understanding of behavioral and neurobiological mechanisms underlying vulnerability to opioid addiction.

Original language	English (US)
Pages (from-to)	2279-2291
Number of pages	13
Journal	Psychopharmacology
Volume	237
Issue number	8
DOIs	https://doi.org/10.1007/s00213-020-05532-w
State	Published - Aug 1 2020

Bibliographical note

Funding Information:
Supported by NIH/NIDA grant R21 DA037728 (Gewirtz/Harris, Co-PIs), the Hennepin Healthcare Research Institute (formerly Minneapolis Medical Research Foundation) Translational Addiction Research Program (Harris PI), a Hennepin Healthcare Research Institute Career Development Award for PhD Investigators (Harris PI), and NIDA training grant T32 DA007097 (Swain, Y; Molitor T, PI). Acknowledgments

Publisher Copyright:
© 2020, Springer-Verlag GmbH Germany, part of Springer Nature.

Keywords

Anhedonia
Intracranial self-stimulation
Opioid
Self-administration
Withdrawal

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title = "Higher anhedonia during withdrawal from initial opioid exposure is protective against subsequent opioid self-administration in rats",

abstract = "Rationale: Understanding factors contributing to individual differences in vulnerability to opioid addiction is essential for developing more effective preventions and treatments, yet few reliable behavioral predictors of subsequent opioid self-administration have been identified in rodents. Sensitivity to the acute effects of initial drug exposure predicts later addiction vulnerability in both humans and animals, but the relationship between sensitivity to withdrawal from initial drug exposure and later drug use vulnerability is unclear. Objective: The goal of the current study was to evaluate whether the degree of anhedonia experienced during withdrawal from early opioid exposure predicts subsequent vulnerability to opioid self-administration. Methods: Rats were first tested for withdrawal sensitivity following acute injections of morphine (i.e., “acute dependence”), measured as elevations in intracranial self-stimulation (ICSS) thresholds (anhedonia-like behavior) during naloxone-precipitated and spontaneous withdrawal. Rats were then tested for addiction-like behavior using various measures of i.v. morphine self-administration (MSA) including acquisition, demand, extinction, and reinstatement induced by morphine, stress, and/or drug-associated cues. Results: Greater naloxone-precipitated withdrawal across repeated morphine injections and greater peak spontaneous withdrawal severity following a single morphine injection were associated with lower addiction-like behavior on multiple MSA measures. Withdrawal-induced anhedonia predicted a wider range of MSA measures than did any individual measure of MSA itself. Conclusions: Our data establish WIA as one of the first behavioral measures to predict individual differences in opioid SA in rodents. This model promises to be useful for furthering our understanding of behavioral and neurobiological mechanisms underlying vulnerability to opioid addiction.",

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note = "Funding Information: Supported by NIH/NIDA grant R21 DA037728 (Gewirtz/Harris, Co-PIs), the Hennepin Healthcare Research Institute (formerly Minneapolis Medical Research Foundation) Translational Addiction Research Program (Harris PI), a Hennepin Healthcare Research Institute Career Development Award for PhD Investigators (Harris PI), and NIDA training grant T32 DA007097 (Swain, Y; Molitor T, PI). Acknowledgments Publisher Copyright: {\textcopyright} 2020, Springer-Verlag GmbH Germany, part of Springer Nature.",

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AU - Harris, Andrew C.

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N2 - Rationale: Understanding factors contributing to individual differences in vulnerability to opioid addiction is essential for developing more effective preventions and treatments, yet few reliable behavioral predictors of subsequent opioid self-administration have been identified in rodents. Sensitivity to the acute effects of initial drug exposure predicts later addiction vulnerability in both humans and animals, but the relationship between sensitivity to withdrawal from initial drug exposure and later drug use vulnerability is unclear. Objective: The goal of the current study was to evaluate whether the degree of anhedonia experienced during withdrawal from early opioid exposure predicts subsequent vulnerability to opioid self-administration. Methods: Rats were first tested for withdrawal sensitivity following acute injections of morphine (i.e., “acute dependence”), measured as elevations in intracranial self-stimulation (ICSS) thresholds (anhedonia-like behavior) during naloxone-precipitated and spontaneous withdrawal. Rats were then tested for addiction-like behavior using various measures of i.v. morphine self-administration (MSA) including acquisition, demand, extinction, and reinstatement induced by morphine, stress, and/or drug-associated cues. Results: Greater naloxone-precipitated withdrawal across repeated morphine injections and greater peak spontaneous withdrawal severity following a single morphine injection were associated with lower addiction-like behavior on multiple MSA measures. Withdrawal-induced anhedonia predicted a wider range of MSA measures than did any individual measure of MSA itself. Conclusions: Our data establish WIA as one of the first behavioral measures to predict individual differences in opioid SA in rodents. This model promises to be useful for furthering our understanding of behavioral and neurobiological mechanisms underlying vulnerability to opioid addiction.

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Higher anhedonia during withdrawal from initial opioid exposure is protective against subsequent opioid self-administration in rats

Abstract

Bibliographical note

Keywords

UN SDGs

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