Literature DB >> 19237543

FGF15/FGFR4 integrates growth factor signaling with hepatic bile acid metabolism and insulin action.

Dong-Ju Shin1, Timothy F Osborne.   

Abstract

The current studies show FGF15 signaling decreases hepatic forkhead transcription factor 1 (FoxO1) activity through phosphatidylinositol (PI) 3-kinase-dependent phosphorylation. The bile acid receptor FXR (farnesoid X receptor) activates expression of fibroblast growth factor (FGF) 15 in the intestine, which acts through hepatic FGFR4 to suppress cholesterol-7alpha hydroxylase (CYP7A1) and limit bile acid production. Because FoxO1 activity and CYP7A1 gene expression are both increased by fasting, we hypothesized CYP7A1 might be a FoxO1 target gene. Consistent with recently reported results, we show CYP7A1 is a direct target of FoxO1. Additionally, we show that the PI 3-kinase pathway is key for both the induction of CYP7A1 by fasting and the suppression by FGF15. FGFR4 is the major hepatic FGF receptor isoform and is responsible for the hepatic effects of FGF15. We also show that expression of FGFR4 in liver was decreased by fasting, increased by insulin, and reduced by streptozotocin-induced diabetes, implicating FGFR4 as a primary target of insulin regulation. Because insulin and FGF both target the PI 3-kinase pathway, these observations suggest FoxO1 is a key node in the convergence of FGF and insulin signaling pathways and functions as a key integrator for the regulation of glucose and bile acid metabolism.

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Year:  2009        PMID: 19237543      PMCID: PMC2670116          DOI: 10.1074/jbc.M808747200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  72 in total

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  44 in total

1.  [Hormonal and metabolic functions of the small intestine].

Authors:  H Wittenburg; U Tennert; J Mössner
Journal:  Internist (Berl)       Date:  2010-06       Impact factor: 0.743

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Authors:  Wook Ha Park; Youngmi Kim Pak
Journal:  Exp Mol Med       Date:  2011-10-31       Impact factor: 8.718

3.  FoxO transcription factors are required for hepatic HDL cholesterol clearance.

Authors:  Samuel X Lee; Markus Heine; Christian Schlein; Rajasekhar Ramakrishnan; Jing Liu; Gabriella Belnavis; Ido Haimi; Alexander W Fischer; Henry N Ginsberg; Joerg Heeren; Franz Rinninger; Rebecca A Haeusler
Journal:  J Clin Invest       Date:  2018-03-19       Impact factor: 14.808

4.  Selective activation of FGFR4 by an FGF19 variant does not improve glucose metabolism in ob/ob mice.

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Review 5.  Bile Acids as Hormones: The FXR-FGF15/19 Pathway.

Authors:  Steven A Kliewer; David J Mangelsdorf
Journal:  Dig Dis       Date:  2015-05-27       Impact factor: 2.404

6.  Differential regulation of bile acid and cholesterol metabolism by the farnesoid X receptor in Ldlr -/- mice versus hamsters.

Authors:  Christophe Gardès; Evelyne Chaput; Andreas Staempfli; Denise Blum; Hans Richter; G Martin Benson
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7.  Individual bile acids have differential effects on bile acid signaling in mice.

Authors:  Peizhen Song; Cheryl E Rockwell; Julia Yue Cui; Curtis D Klaassen
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8.  First High-Density Linkage Map and QTL Fine Mapping for Growth-Related Traits of Spotted Sea bass (Lateolabrax maculatus).

Authors:  Yang Liu; Haolong Wang; Haishen Wen; Yue Shi; Meizhao Zhang; Xin Qi; Kaiqiang Zhang; Qingli Gong; Jifang Li; Feng He; Yanbo Hu; Yun Li
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9.  Cholesteryl ester transfer protein protects against insulin resistance in obese female mice.

Authors:  David A Cappel; Brian T Palmisano; Christopher H Emfinger; Melissa N Martinez; Owen P McGuinness; John M Stafford
Journal:  Mol Metab       Date:  2013-09-02       Impact factor: 7.422

10.  Role of FGF19 induced FGFR4 activation in the regulation of glucose homeostasis.

Authors:  Xinle Wu; Yang Li
Journal:  Aging (Albany NY)       Date:  2009-12-09       Impact factor: 5.682

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