The Nociceptin/Orphanin FQ Receptor Agonist Ro 64-6198 Reduces Alcohol Self-Administration and Prevents Relapse-Like Alcohol Drinking

Kuzmin, Alexander; Kreek, Mary Jeanne; Bakalkin, Georgy; Liljequist, Sture

doi:10.1038/sj.npp.1301169

Cited by 85 publications

(90 citation statements)

References 45 publications

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“…Our findings are in agreement with previous studies showing that NOP receptors regulate the rewarding effects of various drugs of abuse (145,302,303). Specifically, previous studies have shown that activation of NOP receptors reduces anxiety (142), attenuates alcohol self-administration as well as cue-and stress-induced reinstatement of alcohol seeking (143). Cue-and stressinduced reinstatement to drug seeking are mediated by distinct brain pathways that ultimately converge, with cue-induced reinstatement primarily mediated by the mesolimbic DA system and stress-induced reinstatement primarily mediated by CRH and noradrenaline (304,305).…”

Section: Operant Self-administration Progressive Ratio Responding Ansupporting

confidence: 83%

“…These results are supported by previous findings where activation of NOP receptors decreases alcohol self-administration (141,143,298). The operant self-administration model better reflects motivation to obtain alcohol compared to home cage drinking which further strengthens these results.…”

Section: Operant Self-administration Progressive Ratio Responding Ansupporting

confidence: 82%

“…Our results are in parallel support and expand on previous findings by Kuzmin and colleagues that NOP agonism potently and selectively suppresses alcohol selfadministration, motivation to seek alcohol, as well as cue-and stress-induced reinstatement of alcohol seeking (143). …”

Section: Operant Self-administration Progressive Ratio Responding Ansupporting

confidence: 81%

“…It has also been demonstrated that the NOP agonist Ro64-6198 significantly blocks acquisition, expression and reinstatement of alcohol-induced CPP, self-administration and prevents relapse-like alcohol drinking (143,155). The NOP antagonist J-113397 blocks the effects of the NOP receptor agonist Ro65-6570 on the acquisition of opiateand psychostimulant-induced conditioned place preference in rats.…”

Section: The Nociceptin/orphanin Fq System In Alcohol Use Disordermentioning

confidence: 99%

“…For example ICV administration of NOP reduced voluntary alcohol-intake in the alcohol-preferring msP rat (139)(140)(141). In addition systemic (IP) administration of the NOP receptor agonist Ro64-6198 reduced anxiety (142) and alcohol selfadministration and prevented relapse-like behavior in an alcohol deprivation model in rats (143). It has also been reported that ICV administration of nociceptin reduces the rewarding effects of several drugs of abuse in the conditioned place preference (CPP) paradigm.…”

Section: The Role Of Nociceptin/orphanin Fq System In Reward Processingmentioning

confidence: 99%

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Neuropeptide Receptors as Treatment Targets in Alcohol Use Disorders

Aziz¹

2017

Linköping University Medical Dissertations

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Alcohol use disorder (AUD) is a complex disorder with multiple pathophysiological processes contributing to the initiation, progression and development of the disease state. AUD is a chronic relapsing disease with escalation of alcohol-intake over time in repeated cycles of tolerance, abstinence and relapse and hence, it is very difficult to treat. There are only a few currently available treatments with narrow efficacy and variable patient response. Thus it is important to find new, more effective medications to increase the number of patients who can benefit from pharmacological treatment of AUD.The research presented in this thesis work focuses on the critical involvement of central neuropeptides in alcohol-related behaviors. The overall aim was to evaluate the nociceptin/orphanin FQ (NOP) receptor, the neuropeptide Y (NPY) Y2 receptor and the melanin-concentrating hormone (MCH) receptor 1 as novel and potential pharmacological treatment targets for AUD by testing the NOP receptor agonist SR-8993, the NPY-Y2 receptor antagonist CYM-9840 and the MCH1 receptor antagonist GW803430 in established animal models.In the first study (Paper I), the novel and selective NOP agonist SR-8993 was assessed in rat models of motivation to obtain alcohol and relapse to alcohol-seeking behavior using the operant self-administration (SA) paradigm. Firstly, treatment with SR-8993 (1 mg/kg) showed a mildly anxiolytic effect and reversed acute alcohol withdrawal-induced "hangover" anxiety in the elevated plus-maze (EPM). Next, it potently attenuated alcohol SA and motivation to obtain alcohol in the progressive ratio responding (PRR) and reduced both alcohol cue-induced and yohimbine stressinduced reinstatement of alcohol seeking, without affecting the pharmacology and metabolism of alcohol nor other control behaviors. To extend these findings, SR-8993 was evaluated in escalated alcohol-intake in rats. Treatment with SR-8993 significantly suppressed alcohol-intake and preference in rats that were trained to consume high amounts of alcohol in the two-bottle free choice intermittent access (IA) paradigm. SR-8993 also blocked operant SA of alcohol in rats that showed robust escalation in operant alcohol SA following chronic IA exposure to alcohol.In the second study (Paper II), SR-8993 was further evaluated in a model for escalated alcohol-intake induced by long-term IA exposure to alcohol. The effect of previous experience on operant alcohol SA on two-bottle free choice preference drinking was evaluated and sensitivity to treatment with SR-8993 was tested in rats selected for escalated and non-escalated alcohol seeking behavior. We found that rats exposed to the combined SA-IA paradigm showed greater sensitivity to SR-8993 treatment. In addition, acute escalation of alcohol SA after a three-week period of abstinence was completely abolished by pretreatment with SR-8993.In the third study (Paper III), the effects of the novel, small molecule NPY-Y2 antagonist CYM-9840 were tested in operant alcohol SA, PRR which is a model for...

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Section: Operant Self-administration Progressive Ratio Responding Ansupporting

confidence: 83%

Section: Operant Self-administration Progressive Ratio Responding Ansupporting

confidence: 82%

Section: Operant Self-administration Progressive Ratio Responding Ansupporting

confidence: 81%

Section: The Nociceptin/orphanin Fq System In Alcohol Use Disordermentioning

confidence: 99%

Section: The Role Of Nociceptin/orphanin Fq System In Reward Processingmentioning

confidence: 99%

See 3 more Smart Citations

Neuropeptide Receptors as Treatment Targets in Alcohol Use Disorders

Aziz¹

2017

Linköping University Medical Dissertations

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Therapeutic potentials of NOP and MOP receptor coactivation for the treatment of pain and opioid abuse

Kiguchi

Ding

2020

J of Neuroscience Research

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Following the identification of the nociceptin/orphanin FQ (N/OFQ) peptide (NOP) as an endogenous ligand for the NOP receptor, ample evidence has revealed unique functional profiles of the N/OFQ-NOP receptor system. NOP receptors are expressed in key neural substrates involved in pain and reward modulation. In non-human primates (NHPs), NOP receptor activation effectively exerts antinociception and anti-hypersensitivity at the spinal and supraspinal levels. Moreover, NOP receptor activation inhibits dopaminergic transmission and synergistically enhances mu-opioid peptide (MOP) receptor-mediated analgesia. In this article, we discuss the functional profiles of ligands with dual NOP and MOP receptor agonist activities and highlight their optimal functional efficacy for pain relief and drug abuse treatment. Through coactivation of NOP and MOP receptors, bifunctional NOP/MOP receptor "partial" agonists (e.g., AT-121, BU08028, and BU10038) reveal a wider therapeutic window with fewer side effects. These newly developed ligands potently induce antinociception without MOP receptor agonist-associated side effects such as abuse potential, respiratory depression, itch sensation, and physical dependence. In addition, in both rodent and NHP models, bifunctional NOP/MOP receptor agonists can attenuate reward processing and/or the reinforcing effects of opioids and other abused drugs. While a mixed NOP/opioid receptor "full" agonist cebranopadol is undergoing clinical trials, bifunctional NOP/MOP "partial" agonists exhibit promising therapeutic profiles in translational NHP models for the treatment of pain and opioid abuse. This class of drugs demonstrates the therapeutic advantage of NOP and MOP receptor coactivation, indicating a greater potential for future development.

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Advancing Pharmacotherapy Development from Preclinical Animal Studies

Egli

2018

The Neuropharmacology of Alcohol

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Animal models provide rapid, inexpensive assessments of an investigational drug's therapeutic potential. Ideally, they support the plausibility of therapeutic efficacy and provide a rationale for further investigation. Here, I discuss how the absence of clear effective-ineffective categories for alcohol use disorder (AUD) medications and biases in the clinical and preclinical literature affect the development of predictive preclinical alcohol dependence (AD) models. Invoking the analogical argument concept from the philosophy of science field, I discuss how models of excessive alcohol drinking support the plausibility of clinical pharmacotherapy effects. Even though these models are not likely be completely discriminative, they are sensitive to clinically effective medications and have revealed dozens of novel medication targets. In that context, I discuss recent preclinical work on GLP-1 receptor agonists, phosphodiesterase inhibitors, glucocorticoid receptor antagonists, nociception agonists and antagonists, and CRF1 antagonists. Clinically approved medications are available for each of these drug classes. I conclude by advocating a translational approach in which drugs are evaluated highly congruent preclinical models and human laboratory studies. Once translation is established, I suggest the burden is to develop hypothesis-based therapeutic interventions maximizing the impact of the confirmed pharmacotherapeutic effects in the context of additional variables falling outside the model.

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The Nociceptin/Orphanin FQ Receptor Agonist Ro 64-6198 Reduces Alcohol Self-Administration and Prevents Relapse-Like Alcohol Drinking

Cited by 85 publications

References 45 publications

Neuropeptide Receptors as Treatment Targets in Alcohol Use Disorders

Neuropeptide Receptors as Treatment Targets in Alcohol Use Disorders

Therapeutic potentials of NOP and MOP receptor coactivation for the treatment of pain and opioid abuse

Advancing Pharmacotherapy Development from Preclinical Animal Studies

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