Hepatic Gadd45β promotes hyperglycemia and glucose intolerance through DNA demethylation of PGC-1α

Although widely used for their potent anti-inflammatory and immunosuppressive properties, the prescription of glucocorticoid analogues (e.g., dexamethasone) has been associated with deleterious glucose metabolism, compromising their long-term therapeutic use. However, the molecular mechanism remains poorly understood. In the present study, through transcriptomic and epigenomic analysis of two mouse models, we identified a growth arrest and DNA damage-inducible β (Gadd45β)–dependent pathway that stimulates hepatic glucose production (HGP). Functional studies showed that overexpression of Gadd45β in vivo or in cultured hepatocytes activates gluconeogenesis and increases HGP. In contrast, liver-specific Gadd45β-knockout mice were resistant to high-fat diet– or steroid-induced hyperglycemia. Of pathophysiological significance, hepatic Gadd45β expression is up-regulated in several mouse models of obesity and diabetic patients. Mechanistically, Gadd45β promotes DNA demethylation of PGC-1α promoter in conjunction with TET1, thereby stimulating PGC-1α expression to promote gluconeogenesis and hyperglycemia. Collectively, these findings unveil an epigenomic signature involving Gadd45β/TET1/DNA demethylation in hepatic glucose metabolism, enabling the identification of pathogenic factors in diabetes.

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Mechanisms of the free fatty acid-induced increase in hepatic glucose production

AJP Endocrinology and Metabolism ◽

10.1152/ajpendo.00033.2003 ◽

2003 ◽

Vol 284 (5) ◽

pp. E863-E873 ◽

Cited By ~ 131

Author(s):

Tony K. T. Lam ◽

André Carpentier ◽

Gary F. Lewis ◽

Gérald van de Werve ◽

I. George Fantus ◽

...

Keyword(s):

Diabetes Mellitus ◽

Insulin Resistance ◽

Glucose Metabolism ◽

Recent Progress ◽

Hepatic Glucose Production ◽

Glucose Production ◽

Controversial Issues ◽

Hepatic Glucose Metabolism ◽

Hepatic Glucose

The associations between obesity, insulin resistance, and type 2 diabetes mellitus are well documented. Free fatty acids (FFA), which are often elevated in obesity, have been implicated as an important link in these associations. Contrary to muscle glucose metabolism, the effects of FFA on hepatic glucose metabolism and the associated mechanisms have not been extensively investigated. It is still controversial whether FFA have substantial effects on hepatic glucose production, and the mechanisms responsible for these putative effects remain unknown. We review recent progress in this area and try to clarify controversial issues regarding the mechanisms responsible for the FFA-induced increase in hepatic glucose production in the postabsorptive state and during hyperinsulinemia.

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O-GlcNAcylated p53 in the liver modulates hepatic glucose production

Nature Communications ◽

10.1038/s41467-021-25390-0 ◽

2021 ◽

Vol 12 (1) ◽

Author(s):

Maria J. Gonzalez-Rellan ◽

Marcos F. Fondevila ◽

Uxia Fernandez ◽

Amaia Rodríguez ◽

Marta Varela-Rey ◽

...

Keyword(s):

Glucose Homeostasis ◽

Transcriptional Activation ◽

Cellular Response ◽

Hepatic Glucose Production ◽

Glucose Production ◽

Diabetic Patients ◽

Type 2 Diabetic Patients ◽

Protein Levels ◽

Hepatic Glucose

Abstractp53 regulates several signaling pathways to maintain the metabolic homeostasis of cells and modulates the cellular response to stress. Deficiency or excess of nutrients causes cellular metabolic stress, and we hypothesized that p53 could be linked to glucose maintenance. We show here that upon starvation hepatic p53 is stabilized by O-GlcNAcylation and plays an essential role in the physiological regulation of glucose homeostasis. More specifically, p53 binds to PCK1 promoter and regulates its transcriptional activation, thereby controlling hepatic glucose production. Mice lacking p53 in the liver show a reduced gluconeogenic response during calorie restriction. Glucagon, adrenaline and glucocorticoids augment protein levels of p53, and administration of these hormones to p53 deficient human hepatocytes and to liver-specific p53 deficient mice fails to increase glucose levels. Moreover, insulin decreases p53 levels, and over-expression of p53 impairs insulin sensitivity. Finally, protein levels of p53, as well as genes responsible of O-GlcNAcylation are elevated in the liver of type 2 diabetic patients and positively correlate with glucose and HOMA-IR. Overall these results indicate that the O-GlcNAcylation of p53 plays an unsuspected key role regulating in vivo glucose homeostasis.

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In vivo metabolic changes as studied longitudinally after ventromedial hypothalamic lesions

AJP Endocrinology and Metabolism ◽

10.1152/ajpendo.1986.250.6.e662 ◽

1986 ◽

Vol 250 (6) ◽

pp. E662-E668 ◽

Cited By ~ 1

Author(s):

L. Penicaud ◽

F. Rohner-Jeanrenaud ◽

B. Jeanrenaud

Keyword(s):

Glucose Metabolism ◽

Hepatic Glucose Production ◽

Glucose Production ◽

Tissue Response ◽

Insulin Concentration ◽

Insulin Resistant ◽

Hepatic Glucose ◽

Insulin Responsiveness ◽

Total Glucose

Ventromedial hypothalamic (VMH)-lesioned rats were tested 1 and 6 wk after the lesions to determine, by euglycemic-hyperinsulinemic clamps, their tissue response to insulin. One week after the lesions, total glucose metabolism was more sensitive and responsive to insulin than in age-matched controls. In the two groups, hepatic glucose production was suppressed at almost identical insulin concentrations (approximately 550 microU/ml). Six weeks after the VMH lesions, the increased insulin responsiveness of total glucose metabolism disappeared and glucose metabolism became less insulin sensitive (right, shifted dose-response curve) than that of control animals. Furthermore, hepatic glucose production of VMH-lesioned rats was now inhibited by 45% at most and at the supraphysiological insulin concentration of 16,000 microU/ml, while it was totally suppressed by 550 microU/ml of the hormone in age-matched controls. This defect was accompanied by a lack of decrease in plasma glucagon levels during the clamps carried out at maximal insulin concentration. In summary, in a first phase after VMH lesion, rats are hypersensitive and hyperresponsive to insulin; and in a later phase, when obesity is well established, VMH-lesioned rats become insulin resistant and are characterized by a decreased in vivo sensitivity and responsiveness of liver and muscles to the hormone.

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Effects of intraportal exenatide on hepatic glucose metabolism in the conscious dog

AJP Endocrinology and Metabolism ◽

10.1152/ajpendo.00160.2013 ◽

2013 ◽

Vol 305 (1) ◽

pp. E132-E139 ◽

Cited By ~ 1

Author(s):

Dale S. Edgerton ◽

Zhibo An ◽

Kathryn M. S. Johnson ◽

Tiffany Farmer ◽

Ben Farmer ◽

...

Keyword(s):

Glucose Metabolism ◽

Hepatic Glucose Production ◽

Area Under The Curve ◽

Glucose Production ◽

Experimental Period ◽

Whole Body ◽

Saline Control ◽

Hepatic Glucose Metabolism ◽

Hyperglycemic Clamp ◽

Hepatic Glucose

Incretins improve glucose metabolism through multiple mechanisms. It remains unclear whether direct hepatic effects are an important part of exenatide's (Ex-4) acute action. Therefore, the objective of this study was to determine the effect of intraportal delivery of Ex-4 on hepatic glucose production and uptake. Fasted conscious dogs were studied during a hyperglycemic clamp in which glucose was infused into the hepatic portal vein. At the same time, portal saline (control; n = 8) or exenatide was infused at low (0.3 pmol·kg−1·min−1, Ex-4-low; n = 5) or high (0.9 pmol·kg−1·min−1, Ex-4-high; n = 8) rates. Arterial plasma glucose levels were maintained at 160 mg/dl during the experimental period. This required a greater rate of glucose infusion in the Ex-4-high group (1.5 ± 0.4, 2.0 ± 0.7, and 3.7 ± 0.7 mg·kg−1·min−1between 30 and 240 min in the control, Ex-4-low, and Ex-4-high groups, respectively). Plasma insulin levels were elevated by Ex-4 (arterial: 4,745 ± 428, 5,710 ± 355, and 7,262 ± 1,053 μU/ml; hepatic sinusoidal: 14,679 ± 1,700, 15,341 ± 2,208, and 20,445 ± 4,020 μU/ml, 240 min, area under the curve), whereas the suppression of glucagon was nearly maximal in all groups. Although glucose utilization was greater during Ex-4 infusion (5.92 ± 0.53, 6.41 ± 0.57, and 8.12 ± 0.54 mg·kg−1·min−1), when indices of hepatic, muscle, and whole body glucose uptake were expressed relative to circulating insulin concentrations, there was no indication of insulin-independent effects of Ex-4. Thus, this study does not support the notion that Ex-4 generates acute changes in hepatic glucose metabolism through direct effects on the liver.

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The impact of obesity, sex, and diet on hepatic glucose production in cats

AJP Regulatory Integrative and Comparative Physiology ◽

10.1152/ajpregu.90771.2008 ◽

2009 ◽

Vol 296 (4) ◽

pp. R936-R943 ◽

Cited By ~ 28

Author(s):

Saskia Kley ◽

Margarethe Hoenig ◽

John Glushka ◽

Eunsook S. Jin ◽

Shawn C. Burgess ◽

...

Keyword(s):

Phosphoenolpyruvate Carboxykinase ◽

Citrate Synthase ◽

Hepatic Glucose Production ◽

Glucose Production ◽

Endogenous Glucose Production ◽

Hepatic Glucose Metabolism ◽

Peripheral Insulin Resistance ◽

Pyruvate Cycling ◽

Hepatic Glucose ◽

The Impact

Obesity is a risk factor for type 2 diabetes in cats. The risk of developing diabetes is severalfold greater for male cats than for females, even after having been neutered early in life. The purpose of this study was to investigate the role of different metabolic pathways in the regulation of endogenous glucose production (EGP) during the fasted state considering these risk factors. A triple tracer protocol using 2H2O, [U-13C3]propionate, and [3,4-13C2]glucose was applied in overnight-fasted cats (12 lean and 12 obese; equal sex distribution) fed three different diets. Compared with lean cats, obese cats had higher insulin ( P < 0.001) but similar blood glucose concentrations. EGP was lower in obese cats ( P < 0.001) due to lower glycogenolysis and gluconeogenesis (GNG; P < 0.03). Insulin, body mass index, and girth correlated negatively with EGP ( P < 0.003). Female obese cats had ∼1.5 times higher fluxes through phosphoenolpyruvate carboxykinase ( P < 0.02) and citrate synthase ( P < 0.05) than male obese cats. However, GNG was not higher because pyruvate cycling was increased 1.5-fold ( P < 0.03). These results support the notion that fasted obese cats have lower hepatic EGP compared with lean cats and are still capable of maintaining fasting euglycemia, despite the well-documented existence of peripheral insulin resistance in obese cats. Our data further suggest that sex-related differences exist in the regulation of hepatic glucose metabolism in obese cats, suggesting that pyruvate cycling acts as a controlling mechanism to modulate EGP. Increased pyruvate cycling could therefore be an important factor in modulating the diabetes risk in female cats.

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Involvement of the vagus nerves in the regulation of basal hepatic glucose production in conscious dogs

AJP Endocrinology and Metabolism ◽

10.1152/ajpendo.00566.2001 ◽

2002 ◽

Vol 283 (5) ◽

pp. E958-E964 ◽

Cited By ~ 14

Author(s):

Sylvain Cardin ◽

Konstantin Walmsley ◽

Doss W. Neal ◽

Phillip E. Williams ◽

Alan D. Cherrington

Keyword(s):

Hepatic Glucose Production ◽

Control Period ◽

Glucose Production ◽

Heart Rate Change ◽

Vagus Nerves ◽

Hepatic Glucose Metabolism ◽

Vagal Blockade ◽

Hepatic Glucose ◽

Cooling Coils ◽

Glucose Output

We determined if blocking transmission in the fibers of the vagus nerves would affect basal hepatic glucose metabolism in the 18-h-fasted conscious dog. A pancreatic clamp (somatostatin, basal portal insulin, and glucagon) was employed. A 40-min control period was followed by a 90-min test period. In one group, stainless steel cooling coils (Sham, n = 5) were perfused with a 37°C solution, while in the other (Cool, n = 6), the coils were perfused with −20°C solution. Vagal blockade was verified by heart rate change (80 ± 9 to 84 ± 14 beats/min in Sham; 98 ± 12 to 193 ± 22 beats/min in Cool). The arterial glucose level was kept euglycemic by glucose infusion. No change in tracer-determined glucose production occurred in Sham, whereas in Cool it dropped significantly (2.4 ± 0.4 to 1.9 ± 0.4 mg · kg−1· min−1). Net hepatic glucose output did not change in Sham but decreased from 1.9 ± 0.3 to 1.3 ± 0.3 mg · kg−1· min−1in the Cool group. Hepatic gluconeogenesis did not change in either group. These data suggest that vagal blockade acutely modulates hepatic glucose production by inhibiting glycogenolysis.

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Importance of the route of insulin delivery to its control of glucose metabolism

AJP Endocrinology and Metabolism ◽

10.1152/ajpendo.00628.2020 ◽

2021 ◽

Author(s):

Dale S. Edgerton ◽

Mary Courtney Moore ◽

Justin M. Gregory ◽

Guillaume Kraft ◽

Alan D. Cherrington

Keyword(s):

Insulin Secretion ◽

Glucose Metabolism ◽

Glucose Uptake ◽

Hepatic Glucose Production ◽

Glucose Production ◽

The Body ◽

Whole Body ◽

Direct Effects ◽

Pancreatic Insulin ◽

Hepatic Glucose

Pancreatic insulin secretion produces an insulin gradient at the liver compared to the rest of the body (approximately 3:1). This physiologic distribution is lost when insulin is injected subcutaneously, causing impaired regulation of hepatic glucose production and whole body glucose uptake, as well as arterial hyperinsulinemia. Thus, the hepatoportal insulin gradient is essential to the normal control of glucose metabolism during both fasting and feeding. Insulin can regulate hepatic glucose production and uptake through multiple mechanisms, but its direct effects on the liver are dominant under physiologic conditions. Given the complications associated with iatrogenic hyperinsulinemia in patients treated with insulin, insulin designed to preferentially target the liver may have therapeutic advantages.

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Starvation-Induced Changes of Hepatic Glucose Metabolism in Hypo- and Hyperthyroid Rats in Vivo

Journal of Nutrition ◽

10.1093/jn/111.8.1370 ◽

1981 ◽

Vol 111 (8) ◽

pp. 1370-1379 ◽

Cited By ~ 13

Author(s):

Manfred James Müller ◽

Hans Joachim Seitz

Keyword(s):

Glucose Metabolism ◽

Hepatic Glucose Metabolism ◽

Hepatic Glucose ◽

Induced Changes

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Arrestin domain-containing 3 (Arrdc3) modulates insulin action and glucose metabolism in liver

Proceedings of the National Academy of Sciences ◽

10.1073/pnas.1922370117 ◽

2020 ◽

Vol 117 (12) ◽

pp. 6733-6740 ◽

Cited By ~ 2

Author(s):

Thiago M. Batista ◽

Sezin Dagdeviren ◽

Shannon H. Carroll ◽

Weikang Cai ◽

Veronika Y. Melnik ◽

...

Keyword(s):

Messenger Rna ◽

Insulin Action ◽

Hepatic Glucose Production ◽

Glycogen Synthesis ◽

Glucose Production ◽

Hepatic Glycogen ◽

Glycogen Accumulation ◽

Hepatic Glucose ◽

Glucose Output

Insulin action in the liver is critical for glucose homeostasis through regulation of glycogen synthesis and glucose output. Arrestin domain-containing 3 (Arrdc3) is a member of the α-arrestin family previously linked to human obesity. Here, we show thatArrdc3is differentially regulated by insulin in vivo in mice undergoing euglycemic-hyperinsulinemic clamps, being highly up-regulated in liver and down-regulated in muscle and fat. Mice with liver-specific knockout (KO) of the insulin receptor (IR) have a 50% reduction inArrdc3messenger RNA, while, conversely, mice with liver-specific KO ofArrdc3(L-Arrdc3KO) have increased IR protein in plasma membrane. This leads to increased hepatic insulin sensitivity with increased phosphorylation of FOXO1, reduced expression of PEPCK, and increased glucokinase expression resulting in reduced hepatic glucose production and increased hepatic glycogen accumulation. These effects are due to interaction of ARRDC3 with IR resulting in phosphorylation of ARRDC3 on a conserved tyrosine (Y382) in the carboxyl-terminal domain. Thus,Arrdc3is an insulin target gene, and ARRDC3 protein directly interacts with IR to serve as a feedback regulator of insulin action in control of liver metabolism.

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Glucagon Deficiency Reduces Hepatic Glucose Production and Improves Glucose Tolerance In Adult Mice

Endocrine Reviews ◽

10.1210/edrv.31.4.9983 ◽

2010 ◽

Vol 31 (4) ◽

pp. 606-606

Author(s):

Aidan S. Hancock ◽

Aiping Du ◽

Jingxuan Liu ◽

Mayumi Miller ◽

Catherine L. May

Keyword(s):

Glucose Homeostasis ◽

Hepatic Glucose Production ◽

Glucose Production ◽

Postprandial Glucose ◽

Glucagon Receptor ◽

Glucose Levels ◽

Adult Mice ◽

Hepatic Glucose ◽

Knockout Animals

Abstract The major role of glucagon is to promote hepatic gluconeogenesis and glycogenolysis to raise blood glucose levels during hypoglycemic conditions. Several animal models have been established to examine the in vivo function of glucagon in the liver through attenuation of glucagon via glucagon receptor knockout animals and pharmacological interventions. To investigate the consequences of glucagon loss to hepatic glucose production and glucose homeostasis, we derived mice with a pancreas specific ablation of the α-cell transcription factor, Arx, resulting in a complete loss of the glucagon-producing pancreatic α-cell. Using this model, we found that glucagon is not required for the general health of mice but is essential for total hepatic glucose production. Our data clarifies the importance of glucagon during the regulation of fasting and postprandial glucose homeostasis.

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