PPL-138 (BU10038): a bifunctional NOP/mu partial agonist that reduces cocaine self-administration in rats
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Authors
Cippitelli, AndreaMartinez, Madeline
Zribi, Gilles
Cami-Kobeci, Gerta
Husbands, Stephen M.
Toll, Lawrence
Issue Date
2022-06-15Subjects
BU10038cocaine
intermittent access
NOP
opioid
self-administration
Subject Categories::B210 Pharmacology
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The search for new and effective treatments for cocaine use disorder (CUD) is a priority. We determined whether PPL-138 (BU10038), a compound with partial agonist activity at both nociceptin opioid peptide (NOP) and mu-opioid receptors, reduces cocaine consumption, reinstatement, and whether the compound itself produces reinforcing effects in rats. Using an intermittent access (IntA) cocaine self-administration procedure, we found that PPL-138 (0.1 and 0.3 mg/kg) effectively decreased the total number of cocaine infusions and burst-like cocaine intake in both male and female rats. Responses for food in an IntA model of food self-administration were not altered for either sex, although locomotor activity was increased in female but not male rats. Blockade of NOP receptors with the selective antagonist J-113397 (5 mg/kg) did not prevent the PPL-138-induced suppression of cocaine self-administration, whereas blockade of mu-opioid receptors by naltrexone (1 mg/kg) reversed such effect. Consistently, treatment with morphine (1, 3, and 10 mg/kg) dose-dependently reduced IntA cocaine self-administration measures. PPL-138 also reduced reinstatement of cocaine seeking at all doses examined. Although an initial treatment with PPL-138 (2.5, 10, and 40 μg/kg/infusion) appeared rewarding, the compound did not maintain self-administration behavior. Animals treated with PPL-138 showed initial suppression of cocaine self-administration, which was eliminated following repeated daily dosing. However, suppression of cocaine self-administration was retained when subsequent PPL-138 treatments were administered 48 h apart. These findings demonstrate that the approach of combining partial NOP/mu-opioid activation successfully reduces cocaine use, but properties of PPL-138 seem to depend on the timing of drug administration.Citation
Cippitelli A, Martinez M, Zribi G, Cami-Kobeci G, Husbands SM, Toll L (2022) 'PPL-138 (BU10038): a bifunctional NOP/mu partial agonist that reduces cocaine self-administration in rats', Neuropharmacology, 211 (109045).Publisher
ElsevierJournal
NeuropharmacologyPubMed ID
35378170Type
ArticleLanguage
enISSN
0028-3908EISSN
1873-7064Sponsors
This work was supported by the National Institutes of Health R01DA023281.ae974a485f413a2113503eed53cd6c53
10.1016/j.neuropharm.2022.109045
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