Genetic or pharmacological GHSR blockade has sexually dimorphic effects in rodents on a high-fat diet

Author:

Leggio Lorenzo1,Leko Andras1,Gregory-Flores Adriana1,Marchette Renata2ORCID,Gomez Juan3,Vendruscolo Janaina4,Repunte-Canonigo Vez5,Chuong Vicky1ORCID,Deschaine Sara1,Whiting Kimberly1,Jackson Shelley4,Cornejo Maria6,Perello Mario6,You Zhi-Bing1,Eckhaus Michael3,Janda Kim5ORCID,Zorman Barry7,Sumazin Pavel7ORCID,Koob George4,Michaelides Michael3ORCID,Sanna Pietro Paolo5ORCID,Vendruscolo Leandro4ORCID

Affiliation:

1. National Institutes of Health

2. National Institutes on Alcohol Abuse and Alcoholism

3. NIH

4. National Institute on Drug Abuse

5. The Scripps Research Institute

6. Instituto Multidisciplinario de Biología Celular

7. Baylor College of Medicine

Abstract

Abstract The stomach-derived hormone ghrelin regulates essential physiological functions. The ghrelin receptor (GHSR) has ligand-independent actions, therefore, GHSR gene deletion may be a reasonable approach to investigate the role of this system in feeding behaviors and diet-induced obesity (DIO). Here we investigated the effects of a long-term (12 month) high-fat (HFD) versus regular diet on obesity-related measures in global GHSR-KO and wild type (WT) Wistar male and female rats. Our main findings were that the GHSR gene deletion protects against DIO and decreases food intake during HFD in male but not in female rats. GHSR gene deletion increased thermogenesis and brain glucose uptake in male rats and modified the effects of HFD on brain glucose metabolism in a sex-specific manner, as assessed with small animal positron emission tomography. RNA-sequencing was also used to show that GHSR-KO rats had upregulated expression of genes responsible for fat oxidation in brown adipose tissue. Central administration of a novel GHSR inverse agonist, PF-5190457, attenuated ghrelin-induced food intake, but only in male, not in female mice. HFD-induced binge-like eating was reduced by inverse agonism in both sexes. Our results support GHSR as a promising target for new pharmacotherapies for obesity.

Publisher

Research Square Platform LLC

Reference69 articles.

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2. Organization, W.H.: Obesity and overweight, (2021). https://www.who.int/en/news-room/fact-sheets/detail/obesity-and-overweight

3. From Hunger Hormone to It's Complicated: Ghrelin Beyond Feeding Control;Deschaine SL;Physiol. (Bethesda),2022

4. The Role of the Ghrelin System in Drug Addiction;Zallar LJ;Int. Rev. Neurobiol.,2017

5. Ghrelin is a growth-hormone-releasing acylated peptide from stomach;Kojima M;Nature,1999

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