Model of negative affect induced by withdrawal from acute and chronic morphine administration in male mice

Ozdemir, Dersu; Meyer, Judith; Kieffer, Brigitte L.; Darcq, Emmanuel

doi:10.1038/s41598-024-60759-3

Sci Rep

2024

DOI: 10.1038/s41598-024-60759-3

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Model of negative affect induced by withdrawal from acute and chronic morphine administration in male mice

Dersu Ozdemir,

Judith Meyer,

Brigitte L. Kieffer

et al.

Abstract: Opioid use disorder (OUD) is a chronic relapsing disorder that is a major burden for the lives of affected individuals, and society as a whole. Opioid withdrawal is characterized by strong physical symptoms, along with signs of negative affect. Negative affect due to opioid withdrawal is a major obstacle to recovery and relapse prevention. The mechanisms behind negative affect due to either spontaneous or antagonist-precipitated opioid withdrawal are not well known, and more animal models need be developed. He… Show more

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2024

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Cited by 2 publications

References 44 publications

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Translating human drug use patterns into rat models: exploring spontaneous interindividual differences via refined drug self-administration procedures

D’Ottavio,

Pezza,

Modoni

et al. 2024

Preprint

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Heroin and cocaine users tailor their dosage and frequency of use, as well as their method of administration, to maximize the drugs’ pleasurable effects and prevent withdrawal symptoms. On the other hand, many preclinical self-administration and choice experiments employ fixed unit doses and mandatory timeouts after doses (known as discrete dimension procedures). These restrictions fail to consider the distinct pharmacokinetic properties of heroin and cocaine, leading to uniform and comparable behaviors (including drug-taking patterns). This uniformity contrasts sharply with the significantly different ways humans use heroin and cocaine, which are characterized by highly individualized drug use behaviors. Here, we introduce a no-timeout procedure that overcomes this limitation (continuous dimension procedure).We analyzed the heroin and cocaine taking- and seeking-patterns and estimated drug-brain levels in the presence or absence of timeout between drug injections. We further assessed how absence of timeout and the availability of drug or social peer (access time to the two rewards) affect drug preference. Removing the timeout had a profound effect on pattern of heroin taking and seeking, promoting the emergence of burst-like drug intake and social withdrawal as revealed by a discrete choice procedure. On the other hand, timeout removal had a lesser impact on cocaine taking and seeking and did not impact social preference. By removing timeout during self-administration and increasing the access time during choice resulted in a self-administration procedure that more closely mimic human heroin intake, offering a platform to identify novel medications.

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Translating human drug use patterns into rat models: exploring spontaneous interindividual differences via refined drug self-administration procedures

D’Ottavio,

Pezza,

Modoni

et al. 2024

Preprint

View full text Add to dashboard Cite

show abstract

Disrupted Maternal Behavior in Morphine-Dependent Pregnant Rats and Anhedonia in their Offspring

Searles,

Vogt,

Adedokun

et al. 2024

Preprint

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It is currently estimated that every 15 minutes an infant is born with opioid use disorder and undergoes intense early life trauma due to opioid withdrawal. Clinical research on the long-term consequences of gestational opioid exposure reports increased rates of social, conduct, and emotional disorders in these children. Here, we investigate the impact of perinatal opioid exposure (POE) on behaviors associated with anhedonia and stress in male and female Sprague Dawley rats. Young adult female rats were administered morphine via programmable, subcutaneous micro-infusion pumps before, during, and through one week post gestation. Maternal behavior was examined for fragmentation and entropy for the first two postnatal weeks; offspring were assessed for sucrose preference, social behavior, and stress responsivity. Overall, dams that received morphine across gestation displayed significantly less pup-directed behavior with increased fragmentation for nursing and higher entropy scores. In adolescence, male and female rat offspring exposed to morphine displayed reduced sucrose preference and, as adults, spent significantly less time socially interacting with familiar conspecifics. Changes in social behaviors were linked to increased activity in nondopaminergic mesolimbic reward brain regions. Although no treatment effects were observed in forced swim test performance, corticosterone levels were significantly increased in POE adult males. Together, these results suggest that perinatal morphine exposure results in anhedonic behavior, possibly due to fragmented and unpredictable maternal behavior in opioid-dependent dams.

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Model of negative affect induced by withdrawal from acute and chronic morphine administration in male mice

Cited by 2 publications

References 44 publications

Translating human drug use patterns into rat models: exploring spontaneous interindividual differences via refined drug self-administration procedures

Translating human drug use patterns into rat models: exploring spontaneous interindividual differences via refined drug self-administration procedures

Disrupted Maternal Behavior in Morphine-Dependent Pregnant Rats and Anhedonia in their Offspring

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