| Literature DB >> 31105045 |
Grzegorz Godlewski1, Resat Cinar2, Nathan J Coffey2, Jie Liu2, Tony Jourdan2, Bani Mukhopadhyay2, Lee Chedester2, Ziyi Liu2, Douglas Osei-Hyiaman2, Malliga R Iyer2, Joshua K Park2, Roy G Smith3, Hiroshi Iwakura4, George Kunos5.
Abstract
Endocannabinoids acting on the cannabinoid-1 receptor (CB1R) or ghrelin acting on its receptor (GHS-R1A) both promote alcohol-seeking behavior, but an interaction between the two signaling systems has not been explored. Here, we report that the peripheral CB1R inverse agonist JD5037 reduces ethanol drinking in wild-type mice but not in mice lacking CB1R, ghrelin peptide or GHS-R1A. JD5037 treatment of alcohol-drinking mice inhibits the formation of biologically active octanoyl-ghrelin without affecting its inactive precursor desacyl-ghrelin. In ghrelin-producing stomach cells, JD5037 reduced the level of the substrate octanoyl-carnitine generated from palmitoyl-carnitine by increasing fatty acid β-oxidation. Blocking gastric vagal afferents abrogated the ability of either CB1R or GHS-R1A blockade to reduce ethanol drinking. We conclude that blocking CB1R in ghrelin-producing cells reduces alcohol drinking by inhibiting the formation of active ghrelin and its signaling via gastric vagal afferents. Thus, peripheral CB1R blockade may have therapeutic potential in the treatment of alcoholism. Published by Elsevier Inc.Entities:
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Year: 2019 PMID: 31105045 PMCID: PMC6551287 DOI: 10.1016/j.cmet.2019.04.012
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 27.287