Glucagon induces the hepatic expression of inflammatory markers in vitro and in vivo

Francesco Andreozzi; Concetta Di Fatta; Rosangela Spiga; Gaia Chiara Mannino; Elettra Mancuso; Carolina Averta; Carmen De Caro; Martina Tallarico; Antonio Leo; Rita Citraro; Emilio Russo; Giovambattista De Sarro; Giorgio Sesti

doi:10.1111/dom.14902

Glucagon induces the hepatic expression of inflammatory markers in vitro and in vivo

Diabetes Obes Metab. 2023 Feb;25(2):556-569. doi: 10.1111/dom.14902. Epub 2022 Nov 15.

Affiliations

¹ Department of Medical and Surgical Sciences, University Magna Graecia of Catanzaro, Catanzaro, Italy.
² Research Center for the Prevention and Treatment of Metabolic Diseases (CR METDIS), University Magna Graecia of Catanzaro, Catanzaro, Italy.
³ Department of Science of Health, University Magna Graecia of Catanzaro, Catanzaro, Italy.
⁴ Department of Clinical and Molecular Medicine, University of Rome-Sapienza, Rome, Italy.

PMID: 36305474
DOI: 10.1111/dom.14902

Abstract

Glucagon exerts multiple hepatic actions, including stimulation of glycogenolysis/gluconeogenesis. The liver plays a crucial role in chronic inflammation by synthesizing proinflammatory molecules, which are thought to contribute to insulin resistance and hyperglycaemia. Whether glucagon affects hepatic expression of proinflammatory cytokines and acute-phase reactants is unknown. Herein, we report a positive relationship between fasting glucagon levels and circulating interleukin (IL)-1β (r = 0.252, p = .042), IL-6 (r = 0.230, p = .026), fibrinogen (r = 0.193, p = .031), complement component 3 (r = 0.227, p = .024) and high sensitivity C-reactive protein (r = 0.230, p = .012) in individuals without diabetes. In CD1 mice, 4-week continuous treatment with glucagon induced a significant increase in circulating IL-1β (p = .02), and IL-6 (p = .001), which was countered by the contingent administration of the glucagon receptor antagonist, GRA-II. Consistent with these results, we detected a significant increase in the hepatic activation of inflammatory pathways, such as expression of NLRP3 (p < .02), and the phosphorylation of nuclear factor kappaB (NF-κB; p < .02) and STAT3 (p < .01). In HepG2 cells, we found that glucagon dose-dependently stimulated the expression of IL-1β (p < .002), IL-6 (p < .002), fibrinogen (p < .01), complement component 3 (p < .01) and C-reactive protein (p < .01), stimulated the activation of NLRP3 inflammasome (p < .01) and caspase-1 (p < .05), induced the phosphorylation of TRAF2 (p < .01), NF-κB (p < .01) and STAT3 (p < .01). Preincubating cells with GRA-II inhibited the ability of glucagon to induce an inflammatory response. Using HepaRG cells, we confirmed the dose-dependent ability of glucagon to stimulate the expression of NLRP3, the phosphorylation of NF-κB and STAT3, in the absence of GRA-II. These results suggest that glucagon has proinflammatory effects that may participate in the pathogenesis of hyperglycaemia and unfavourable cardiometabolic risk profile.

Keywords: NF-κB pathway; NLRP3 inflammasome; cytokines; glucagon; liver inflammation; low-grade inflammation.

MeSH terms

Animals
Complement C3 / pharmacology
Glucagon / pharmacology
Inflammasomes / metabolism
Interleukin-1beta / metabolism
Interleukin-1beta / pharmacology
Interleukin-6
Liver / metabolism
Mice
NF-kappa B* / metabolism
NF-kappa B* / pharmacology
NLR Family, Pyrin Domain-Containing 3 Protein* / metabolism
Signal Transduction

Substances

NF-kappa B
NLR Family, Pyrin Domain-Containing 3 Protein
Glucagon
Complement C3
Interleukin-6
Inflammasomes
Interleukin-1beta