Glucocorticoid Receptor Antagonist Mifepristone Does Not Alter Innate Anxiety-Like Behavior in Genetically-Selected Marchigian Sardinian (msP) Rats

Vozella, Valentina; Cruz, Bryan; Natividad, Luis A.; Benvenuti, Federica; Cannella, Nazzareno; Edwards, Scott; Zorrilla, Eric P.; Ciccocioppo, Roberto; Roberto, Marisa

doi:10.3390/ijms22063095

Cited by 12 publications

(9 citation statements)

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“…Case in point, Marchigian Sardinian alcohol preferring (msP) rats (a genetically selected rat model of AUD with phenotypic trait resembling anxiety and stress-related disorders such as PTSD) were less responsive to mifepristone's ability to reduce alcohol self-administration 78 or anxiety-like behaviour and startle responses. 79 Our results are also consistent with the previous baboon study where mifepristone did not reduce alcohol consumption, 18 supporting the hypothesis that in an individual with severe AUD who consumes large amounts of alcohol, mifepristone pharmacokinetics may be non-linear. In summary, given (1) the floor effect during the alcohol self-administration in the bar laboratory; (2) the unlikely ability that naturalistic drinking may be changed in an AUD population of non-treatment seekers; (3) the known differences between treatment-seekers versus non-treatment seekers for AUD 80 ; (4) the fact that, unlike in our study, previous work 14 reported an effect of mifepristone in reducing alcohol drinking in people with AUD; and…”

Section: Discussionsupporting

confidence: 91%

“…The lack of mifepristone effect during the naturalistic drinking (outpatient setting) could be due to our sample being individuals with high family history of AUD and history of early trauma. Case in point, Marchigian Sardinian alcohol preferring (msP) rats (a genetically selected rat model of AUD with phenotypic trait resembling anxiety and stress‐related disorders such as PTSD) were less responsive to mifepristone's ability to reduce alcohol self‐administration 78 or anxiety‐like behaviour and startle responses 79 . Our results are also consistent with the previous baboon study where mifepristone did not reduce alcohol consumption, 18 supporting the hypothesis that in an individual with severe AUD who consumes large amounts of alcohol, mifepristone pharmacokinetics may be non‐linear.…”

Section: Discussionmentioning

confidence: 99%

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Mifepristone as a pharmacological intervention for stress‐induced alcohol craving: A human laboratory study

et al. 2023

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Preclinical and clinical work suggests that mifepristone may be a viable treatment for alcohol use disorder (AUD). This was a Phase 1/2, outpatient, cross-over, randomized, double-blind, placebo-controlled trial with non-treatment-seeking individuals with AUD (N = 32). We assessed safety, alcohol craving and consumption, after 1-week mifepristone 600 mg/day administration, in a human laboratory study comprised of a single oral yohimbine administration (32.4 mg), a cue-reactivity procedure and alcohol self-administration. Safety was monitored by adverse events and hemodynamic parameters, alcohol craving by alcohol craving questionnaire and cue-induced saliva output. During the alcohol self-administration, we assessed alcohol pharmacokinetics, subjective effects and consumption. Outcomes were assessed using Generalized Estimating Equations and mediation analysis. Mild-moderate adverse events were reported in both conditions. There was no statistically significant difference between mifepristone and placebo in alcohol pharmacokinetics and subjective effects. Furthermore, blood pressure increased only in the placebo condition after the stress-induced laboratory procedures. Mifepristone, compared to placebo, significantly reduced Clinical trial registration: Clinicaltrials.gov; NCT02243709 IND/FDA: 121984, mifepristone and yohimbine (Holder: Haass-Koffler).

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Section: Discussionsupporting

confidence: 91%

Section: Discussionmentioning

confidence: 99%

Mifepristone as a pharmacological intervention for stress‐induced alcohol craving: A human laboratory study

et al. 2023

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“…This greater efficacy of mifepristone in dependent rats is in line with previous studies likely reflecting increased CeA GR function in alcohol dependence and protracted withdrawal ( Vendruscolo et al, 2015 ). Indeed, mifepristone has been shown to be most efficacious in reducing excessive alcohol drinking in animal models of binge-like drinking, heavy drinking, and alcohol dependence all of which are strong stressors per se while mixed effects of mifepristone on alcohol consumption or anxiety-related behaviors in non-dependent animals as well as in strains genetically-selected for innate high anxiety levels such as the Marchigian Sardinian rats have been reported ( Benvenuti et al, 2021 ; Calvo and Volosin, 2001 ; Fahlke et al, 1995 ; Holtyn and Weerts, 2019 ; Jacquot et al, 2008 ; Koenig and Olive, 2004 ; Newman et al, 2018 ; O’Callaghan et al, 2005 ; Ostroumov et al, 2016 ; Repunte-Canonigo et al, 2015 ; Savarese et al, 2020 ; Simms et al, 2012 ; Vendruscolo et al, 2015 ; Vendruscolo et al, 2012 ; Vozella et al, 2021 ; Yang et al, 2008 ).…”

Section: Discussionmentioning

confidence: 99%

Alcohol dependence and withdrawal increase sensitivity of central amygdalar GABAergic synapses to the glucocorticoid receptor antagonist mifepristone in male rats

Khom

Rodriguez

Gandhi

et al. 2022

Neurobiology of Disease

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“…Anxiety-like behaviour was assessed using novelty-induced hypophagia (NIH) procedures as previously described (Vozella et al, 2021).…”

Section: Novelty-induced Hypophagiamentioning

confidence: 99%

Sexually dimorphic effects of monoacylglycerol lipase inhibitor MJN110 on stress‐related behaviour and drinking in Marchigian Sardinian alcohol‐preferring rats

Vozella,

Cruz,

Feldman

et al. 2023

British J Pharmacology

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Background and PurposeStress‐related disorders are often intertwined with alcohol use disorder (AUD). The endocannabinoid (eCB) system, which comprises the lipid mediators anandamide (AEA) and 2‐arachidonoylglycerol (2‐AG), plays an important homeostatic role in the regulation of stress circuits and has emerged as a therapeutic target to treat stress disorders and AUD. Extensive research has elucidated the role of AEA, but less is known about 2‐AG‐mediated signaling.Experimental ApproachWe pharmacologically enhanced the eCB signaling by inhibiting the 2‐AG metabolizing enzyme, monoacylglycerol lipase (MAGL), in male and female Marchigian‐Sardinian alcohol preferring (msP) rats, a model of innate alcohol preference and stress hypersensitivity, and control Wistar rats. We tested the acute effect of the selective MAGL inhibitor MJN110 in alleviating symptoms of alcohol drinking, anxiety, irritability, and fear in both male and female rats.Key ResultsA single systemic administration of MJN110 increased 2‐AG levels in the central amygdala, prelimbic, and infralimbic cortex, but did not acutely alter alcohol drinking. MAGL inhibition reduced aggressive behaviors in female msPs and increased defensive behaviors in male msPs, during the irritability test. Moreover, in the novelty‐induced hypophagia test, MJN110 selectively enhanced palatable food consumption in females, mitigating stress‐induced food suppression. Lastly, msP rats showed increased conditioned fear behavior compared to Wistar rats, and MJN110 reduced context‐associated conditioned fear responses, but not cue‐probed fear expression, in male msPs.Conclusion and ImplicationsAcute inhibition of MAGL attenuated some stress‐related responses in msP rats but not voluntary alcohol drinking. Our results provide new insights into the sex dimorphism documented in stress‐induced responses and suggest that sex‐specific endocannabinoid‐based approaches should be considered in the clinical development of therapeutics.

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Glucocorticoid Receptor Antagonist Mifepristone Does Not Alter Innate Anxiety-Like Behavior in Genetically-Selected Marchigian Sardinian (msP) Rats

Cited by 12 publications

References 50 publications

Mifepristone as a pharmacological intervention for stress‐induced alcohol craving: A human laboratory study

Mifepristone as a pharmacological intervention for stress‐induced alcohol craving: A human laboratory study

Alcohol dependence and withdrawal increase sensitivity of central amygdalar GABAergic synapses to the glucocorticoid receptor antagonist mifepristone in male rats

Sexually dimorphic effects of monoacylglycerol lipase inhibitor MJN110 on stress‐related behaviour and drinking in Marchigian Sardinian alcohol‐preferring rats

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