G protein-coupled receptors as potential targets for nonalcoholic fatty liver disease treatment

doi:10.3748/wjg.v27.i8.677

Advanced Search

BPG is committed to discovery and dissemination of knowledge

Home / Archive / Volume 27, Issue 8

This Article

Academic Content and Language Evaluation of This Article

CrossCheck and Google Search of This Article

Academic Rules and Norms of This Article

Citation of this article

Corresponding Author of This Article

Research Domain of This Article

Article-Type of This Article

Open-Access Policy of This Article

Times Cited Counts in Google of This Article

Number of Hits and Downloads for This Article

Total Article Views (10206)

All Articles published online

The chart showing PDF series, WORD series, HTML series, Figures (1-2) series, Tables (1-2) series.

Item

Count

PDF

779

WORD

252

HTML

5950

Figures (1-2)

651

Tables (1-2)

318

Sum=7950

Featured Article

The chart showing Browse series, Download series.

Item

Count

Browse

291

Download

485

Sum=776

Publishing Process of This Article

Item

Count

Browse

652

Download

828

Sum=1480

Feb 28, 2021 (publication date) through Apr 25, 2024

Times Cited of This Article

Times Cited (26)

Journal Information of This Article

Publication Name

World Journal of Gastroenterology

ISSN

1007-9327

Publisher of This Article

Baishideng Publishing Group Inc, 7041 Koll Center Parkway, Suite 160, Pleasanton, CA 94566, USA

Review

World J Gastroenterol. Feb 28, 2021; 27(8): 677-691
Published online Feb 28, 2021. doi: 10.3748/wjg.v27.i8.677

Table 2 G protein-coupled receptor-mediated treatment in nonalcoholic fatty liver disease

GPCRs	Treatment	Study	Effect	Ref.
GPRC6A	Metabolitin, a peptide hormone	Mice	Specifically deleting Gprc6a in mouse hepatocytes caused hepatic fat accumulation. Metabolitin can significantly ameliorate NAFLD symptoms and inhibit gut triglyceride and cholesterol absorption and insulin resistance via GPRC6A-mediated activation of the 5’ AMP-activated protein kinase signaling pathway	[44,91]
GPR39	Agonist TC-G1008	Mice	Oral administration of TC-G1008 inhibited hepatic cell necrosis in concanavalin A-induced hepatitis liver in mice. In addition, acute administration of TC-G1008 reduced ethanol intake	[93,94]
GPR40	Agonist SCO-267	Mice	GPR40 deficiency was associated with hepatic inflammation and steatosis in low-fat diet-fed mice. Oral administration of SCO-267 reduced HFD-induced increase in liver weight, triglyceride and collagen production, and serum alanine aminotransferase	[95,96]
GPR40	Docosahexaenoic acid	Primary hepatocytes, HFD-fed mice	Treatment with DHA, an omega-3 fatty acid, inhibited lipid droplets by interacting with GPR40 in primary hepatocytes via reduced expression of lipogenic enzymes. In addition, it significantly reduced the HFD-induced liver steatosis score in mice	[99]
GPR43	Compound probiotics	Rats	Overexpressing GPR43 in adipose tissue kept mice lean on a HFD diet. Compound probiotics can modulate gut microbiota dysbiosis, SCFAs, and their receptors, like GPR43, in NAFLD rats	[30,102]
GPR84	Antagonist PBI-4547GPR84 Antagonists CpdA and CpdB	Gpr84^-/- mice; Wild-type mice	PBI-4547 treatment ameliorated NAFLD-associated metabolic dysregulation, hepatic steatosis and ballooning, which was depleted in Gpr84^-/- mice. Inhibition of GPR84 with antagonists CpdA and CpdB significantly reduced myeloid cell infiltration and ameliorated inflammation and fibrosis in acute liver injury	[100,101]
GPR120	TUG-891Agonist III	Hepatocytes; Mice	Agonist TUG-891 inhibited lipid accumulation in hepatocytes. Agonist III significantly suppressed macrophage infiltration, ROS production, hepatic inflammation, ER stress, and steatohepatitis	[97,98]

DHA: Docosahexaenoic acid; ER: endoplasmic reticulum; GPCRs: G protein-coupled receptors; HFD: High-fat diet; NAFLD: Nonalcoholic fatty liver disease; NASH: Nonalcoholic steatohepatitis; ROS: Reactive oxygen species; SCFA: Short-chain fatty acid.

Citation: Yang M, Zhang CY. G protein-coupled receptors as potential targets for nonalcoholic fatty liver disease treatment. World J Gastroenterol 2021; 27(8): 677-691
URL: https://www.wjgnet.com/1007-9327/full/v27/i8/677.htm
DOI: https://dx.doi.org/10.3748/wjg.v27.i8.677