Pharmacological GHSR (ghrelin receptor) blockade reduces alcohol binge-like drinking in male and female mice

Ghrelin is a peptide that is produced by endocrine cells that are primarily localized in the stomach. Ghrelin receptors (GHSR) are expressed in the brain and periphery. Preclinical and clinical studies support a role for ghrelin in alcohol drinking and seeking. The GHSR has been suggested to be a po...

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Veröffentlicht in:Neuropharmacology 2023-11, Vol.238, p.109643-109643, Article 109643
Hauptverfasser: Richardson, Rani S., Sulima, Agnieszka, Rice, Kenner C., Kucharczk, Jed A., Janda, Kim D., Nisbett, Khalin E., Koob, George F., Vendruscolo, Leandro F., Leggio, Lorenzo
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Sprache:eng
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Zusammenfassung:Ghrelin is a peptide that is produced by endocrine cells that are primarily localized in the stomach. Ghrelin receptors (GHSR) are expressed in the brain and periphery. Preclinical and clinical studies support a role for ghrelin in alcohol drinking and seeking. The GHSR has been suggested to be a potential pharmacotherapeutic target for alcohol use disorder (AUD). However, the role of the ghrelin system and its potential modulation by biological sex on binge-like drinking has not been comprehensively investigated. The present study tested six GHSR antagonists in an alcohol binge-like drinking procedure in male and female mice. Systemic administration of the GHSR antagonists JMV2959, PF-5190457, PF-6870961, and HM-04 reduced alcohol intake in both male and female mice. YIL-781 decreased intake in males, and LEAP2 (likely peripherally restricted) did not reduce intake in mice of either sex. We also administered LEAP2 and JMV2959 intracerebroventricularly to investigate whether the effects of GHSR blockade on alcohol intake are mediated by central receptors. The central administration of LEAP2 and JMV2959 decreased alcohol intake, particularly in high-drinking animals. Finally, in a preliminary experiment, an anti-ghrelin vaccine was examined for its potential effect on binge-like drinking and had no effect. In all experiments, there was a lack of meaningful sex differences. These findings suggest that central GHSR mediates binge-like alcohol intake. These data reveal novel pharmacological compounds with translational potential in the treatment of AUD and provide further evidence of the GHSR as a potential treatment target for AUD. •Systemic administration of several GHSR antagonists, but not LEAP2, reduced alcohol intake in both male and female mice.•LEAP2 administered centrally reduced alcohol intake, particularly in high-drinking animals.•An anti-ghrelin vaccine had no effect on binge-like drinking.•No meaningful sex differences were seen in response to GHSR blockade.
ISSN:0028-3908
1873-7064
1873-7064
DOI:10.1016/j.neuropharm.2023.109643