Naringenin Prevents Obesity, Hepatic Steatosis, and Glucose Intolerance in Male Mice Independent of Fibroblast Growth Factor 21-Reference-Cited by-同舟云学术

Naringenin Prevents Obesity, Hepatic Steatosis, and Glucose Intolerance in Male Mice Independent of Fibroblast Growth Factor 21

Published:2015-06-01 Issue:6 Volume:156 Page:2087-2102
ISSN:0013-7227
Container-title:Endocrinology
language:en
Short-container-title:

Author:

Assini Julia M.¹²,Mulvihill Erin E.¹²,Burke Amy C.¹²,Sutherland Brian G.¹,Telford Dawn E.¹³,Chhoker Sanjiv S.¹²,Sawyez Cynthia G.¹³,Drangova Maria¹⁴⁵,Adams Andrew C.¹⁶,Kharitonenkov Alexei¹⁶,Pin Christopher L.¹⁷,Huff Murray W.¹³

Affiliation:

1. Department of Vascular Biology (J.M.A., E.E.M., A.C.B., B.G.S., D.E.T., S.S.C., C.G.S., M.W.H.) Robarts Research Institute, London, Ontario, Canada N6A 5B7;

2. Departments of Biochemistry (J.M.A., E.E.M., A.C.B., S.S.C., M.W.H.), The University of Western Ontario, London, Ontario, Canada N6A 5B7;

3. Medicine (D.E.T., C.G.S., M.W.H.), The University of Western Ontario, London, Ontario, Canada N6A 5B7;

4. Imaging Research Laboratories (M.D.), Robarts Research Institute, London, Ontario, Canada N6A 5B7;

5. Medical Biophysics (M.D.) The University of Western Ontario, London, Ontario, Canada N6A 5B7;

6. Lilly Research Laboratories (A.C.A., A.K.), Division of Eli Lilly and Company, Indianapolis, Indiana 46285

7. Children's Health Research Institute and Departments of Paediatrics, Physiology and Pharmacology, and Oncology (C.L.P.);

Abstract

Abstract The molecular mechanisms and metabolic pathways whereby the citrus flavonoid, naringenin, reduces dyslipidemia and improves glucose tolerance were investigated in C57BL6/J wild-type mice and fibroblast growth factor 21 (FGF21) null (Fgf21−/−) mice. FGF21 regulates energy homeostasis and the metabolic adaptation to fasting. One avenue of this regulation is through induction of peroxisome proliferator-activated receptor-γ coactivator-1α (Pgc1a), a regulator of hepatic fatty acid oxidation and ketogenesis. Because naringenin is a potent activator of hepatic FA oxidation, we hypothesized that induction of FGF21 might be an integral part of naringenin's mechanism of action. Furthermore, we predicted that FGF21 deficiency would potentiate high-fat diet (HFD)-induced metabolic dysregulation and compromise metabolic protection by naringenin. The absence of FGF21 exacerbated the response to a HFD. Interestingly, naringenin supplementation to the HFD robustly prevented obesity in both genotypes. Gene expression analysis suggested that naringenin was not primarily targeting fatty acid metabolism in white adipose tissue. Naringenin corrected hepatic triglyceride concentrations and normalized hepatic expression of Pgc1a, Cpt1a, and Srebf1c in both wild-type and Fgf21−/− mice. HFD-fed Fgf21−/− mice displayed greater muscle triglyceride deposition, hyperinsulinemia, and impaired glucose tolerance as compared with wild-type mice, confirming the role of FGF21 in insulin sensitivity; however, naringenin supplementation improved these metabolic parameters in both genotypes. We conclude that FGF21 deficiency exacerbates HFD-induced obesity, hepatic steatosis, and insulin resistance. Furthermore, FGF21 is not required for naringenin to protect mice from HFD-induced metabolic dysregulation. Collectively these studies support the concept that naringenin has potent lipid-lowering effects and may act as an insulin sensitizer in vivo.

Publisher

The Endocrine Society

Subject

Endocrinology

Link

http://academic.oup.com/endo/article-pdf/156/6/2087/8991257/endo2087.pdf

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