Glucagon and lipid interactions in the regulation of hepatic AMPK signaling and expression of PPARα and FGF21 transcripts in vivo

Berglund, Eric D.; Li, Kang; Lee, Robert S.; Hasenour, Clinton M.; Lustig, Daniel G.; Lynes, Sara E.; Donahue, E. Patrick; Swift, Larry L.; Charron, Maureen J.; Wasserman, David H.

doi:10.1152/ajpendo.00263.2010

Cited by 90 publications

(84 citation statements)

References 50 publications

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“…Our finding is consistent with Heiker et al (16), who showed that increased serum adiponectin results in an increase in AMPK activation via ADRs. Our results are also consistent with glucagon-mediated activation of AMPK in the liver (4,28). We demonstrated that fasting glucagon had a tendency to be decreased in the HFDϩPL compared with the HFDϩRIM group, which is cosnsistent with the results obtained for AMPK activation.…”

Section: Discussionsupporting

confidence: 91%

CB1R antagonist increases hepatic insulin clearance in fat-fed dogs likely via upregulation of liver adiponectin receptors

Kabir

Iyer

Richey

et al. 2015

American Journal of Physiology-Endocrinology and Metabolism

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The improvement of hepatic insulin sensitivity by the cannabinoid receptor 1 (CB1R) antagonist rimonabant (RIM) has been recently been reported to be due to upregulation of adiponectin. Several studies demonstrated that improvement in insulin clearance accompanies the enhancement of hepatic insulin sensitivity. However, the effects of RIM on hepatic insulin clearance (HIC) have not been fully explored. The aim of this study was to explore the molecular mechanism(s) by which RIM affects HIC, specifically to determine whether upregulation of liver adiponectin receptors (ADRs) and other key genes regulated by adiponectin mediate the effects. To induce insulin resistance in skeletal muscle and liver, dogs were fed a hypercaloric high-fat diet (HFD) for 6 wk. Thereafter, while still maintained on a HFD, animals received RIM (HFDϩRIM; n ϭ 11) or placebo (HFDϩPL; n ϭ 9) for an additional 16 wk. HIC, calculated as the metabolic clearance rate (MCR), was estimated from the euglycemichyperinsulinemic clamp. The HFDϩPL group showed a decrease in MCR; in contrast, the HFDϩRIM group increased MCR. Consistently, the expression of genes involved in HIC, CEACAM-1 and IDE, as well as gene expression of liver ADRs, were increased in the HFDϩRIM group, but not in the HFDϩPL group. We also found a positive correlation between CEACAM-1 and the insulin-degrading enzyme IDE with ADRs. Interestingly, expression of liver genes regulated by adiponectin and involved in lipid oxidation were increased in the HFDϩRIM group. We conclude that in fat-fed dogs RIM enhances HIC, which appears to be linked to an upregulation of the adiponectin pathway. CB1R antagonist; dogs; insulin resistance; insulin clearance; liver THE METABOLIC SYNDROME is a cluster of abnormalities [abdominal obesity, dyslipidemia, hypertension, and nonalcoholic steatohepatitis (NASH)] that are related to insulin resistance and subsequent development of type 2 diabetes. The endocannabinoid system has garnered a great deal of attention as a potential therapeutic target in combating obesity as well as its associated metabolic abnormalities. Compared with their corresponding controls, patients with obesity and type 2 diabetes exhibit higher levels of endocannabinoids in the visceral fat and serum, respectively (32). Chronic treatment with the cannabinoid (CB) receptor (CB1R) antagonist rimonabant (RIM) leads to weight loss and improved insulin sensitivity in obese rodents (15, 43), canines (44), and humans (51). Moreover, several studies have recently shown that RIM has beneficial effects on the liver (14, 15). RIM has been shown to reverse steatohepatitis and related features of metabolic syndrome (15, 49). Thus, although the commercial cannabinoid receptor antagonist RIM has been withdrawn from the market, it remains important to study the cannabinoid receptor system if additional non-centrally-acting antagonists become available (50). Also, the tremendous increase in cannabinoid intake in the U.S. and elsewhere (10) supports studies of the effects of these agonists and their...

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Section: Discussionsupporting

confidence: 91%

CB1R antagonist increases hepatic insulin clearance in fat-fed dogs likely via upregulation of liver adiponectin receptors

Kabir

Iyer

Richey

et al. 2015

American Journal of Physiology-Endocrinology and Metabolism

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“…Recently, it has been shown that glucagon modulates Fgf-21 expression [12][13][14][15]. Here, we extend these observations by reporting for the first time that glucagon increases, independently of endogenous insulin levels, circulating levels of FGF-21 in humans and rodents.…”

Section: Discussionsupporting

confidence: 78%

“…* p <0.05, ** p <0.01 and *** p <0.001 vs vehicle-treated groups (indicated as -). Each experiment was repeated three times The increase of FGF-21 plasma concentration by exogenous glucagon regardless of endogenous insulin production is somehow intriguing, in view of the contradictory results of earlier studies showing that insulin regulates FGF-21 [12,15,17,30]. Exogenous insulin increased plasma FGF-21 and Fgf-21 mRNA expression in skeletal muscle in humans [30].…”

Section: Discussionmentioning

confidence: 96%

“…In rodents glucagon seems to stimulate Fgf-21 expression in vitro and in vivo [12][13][14][15], and these effects are somewhat augmented by NEFA [15]. However, another study reported that glucagon fails to stimulate hepatic Fgf-21 mRNA expression in rodents [16].…”

Section: Introductionmentioning

confidence: 99%

“…Discrepant observations were also reported regarding the role of insulin in glucagon-stimulated FGF-21 production [15]. In non-diabetic humans, an approximately sevenfold increase in circulating insulin was associated with a minimal elevation of FGF-21 [17].…”

Section: Introductionmentioning

confidence: 99%

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Glucagon increases circulating fibroblast growth factor 21 independently of endogenous insulin levels: a novel mechanism of glucagon-stimulated lipolysis?

et al. 2012

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Aims/hypothesis Glucagon reduces body weight by modifying food intake, glucose/lipid metabolism and energy expenditure. All these physiological processes are also controlled by fibroblast growth factor 21 (FGF-21), a circulating hepatokine that improves the metabolic profile in obesity and type 2 diabetes. Animal experiments have suggested a possible interaction between glucagon and FGF-21 however, the metabolic consequences of this crosstalk are not understood. Methods The effects of exogenous glucagon on plasma FGF-21 levels and lipolysis were evaluated in healthy volunteers and humans with type 1 diabetes, as well as in rodents with streptozotocin (STZ)-induced insulinopenic diabetes. In vitro, the role of glucagon on FGF-21 secretion and lipolysis was studied using isolated primary rat hepatocytes and adipocytes. Fgf-21 expression in differentiated rat pre-adipocytes was suppressed by small interfering RNA and released FGF-21 was immunoneutralised by polyclonal antibodies. Results Glucagon induced lipolysis in healthy human volunteers, patients with type 1 diabetes, mice and rats with STZ-induced insulinopenic diabetes, and in adipocytes isolated from diabetic and non-diabetic animals. In addition, glucagon increased circulating FGF-21 in healthy humans and rodents, as well as in patients with type 1 diabetes, and insulinopenic rodents. Glucagon stimulated FGF-21 secretion from isolated primary hepatocytes and adipocytes derived from animals with insulinopenic diabetes. Furthermore, FGF-21 stimulated lipolysis in primary adipocytes isolated from non-diabetic and diabetic rats. Reduction of Fgf-21 expression (by approximately 66%) or immunoneutralisation of released FGF-21 markedly attenuated glucagon-stimulated lipolysis in adipocytes. Conclusions/interpretation These results indicate that glucagon increases circulating FGF-21 independently of endogenous insulin levels. FGF-21 participates in glucagon-induced stimulation of lipolysis.

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Physical activity and liver diseases

2015

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Regular physical activity beneficially impacts the risk of onset and progression of several chronic diseases. However, research regarding the effects of exercising on chronic liver diseases is relatively recent. Most researchers focused on nonalcoholic fatty liver disease (NAFLD), in which increasing clinical and experimental data indicate that skeletal muscle crosstalking to the adipose tissue and the liver regulates intrahepatic fat storage. In this setting, physical activity is considered to be required in combination with calories restriction to allow an effective decrease of intrahepatic lipid component, and despite that evidence is not conclusive, some studies suggest that vigorous activity might be more beneficial than moderate activity to improve NAFLD/nonalcoholic steatohepatitis. Evidence regarding the effects of exercise on the risk of hepatocellular carcinoma is scarce; some epidemiological studies indicate a lower risk in patients regularly and vigorously exercising. In compensated cirrhosis, exercise acutely increases portal pressure, but in the longer term it has been proved safe and probably beneficial. Decreased aerobic capacity (VO2) correlates with mortality in patients with decompensated cirrhosis, who are almost invariably sarcopenic. In these patients, VO2 is improved by physical activity, which might also reduce the risk of hepatic encephalopathy through an increase in skeletal muscle mass. In solid organ transplantation recipients, exercise is able to improve lean mass, muscle strength, and, as a consequence, aerobic capacity. Few data exist in liver transplant recipients, in whom exercise should be an object of future studies given its high potential of providing long‐term beneficial effects. Conclusions: Despite that evidence is far from complete, physical activity should be seen as an important part of the management of patients with liver disease in order to improve their clinical outcome. (Hepatology 2016;63:1026–1040)

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Glucagon and lipid interactions in the regulation of hepatic AMPK signaling and expression of PPARα and FGF21 transcripts in vivo

Cited by 90 publications

References 50 publications

CB1R antagonist increases hepatic insulin clearance in fat-fed dogs likely via upregulation of liver adiponectin receptors

CB1R antagonist increases hepatic insulin clearance in fat-fed dogs likely via upregulation of liver adiponectin receptors

Glucagon increases circulating fibroblast growth factor 21 independently of endogenous insulin levels: a novel mechanism of glucagon-stimulated lipolysis?

Physical activity and liver diseases

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