A Choline-Deficient Diet Exacerbates Fatty Liver but Attenuates Insulin Resistance and Glucose Intolerance in Mice Fed a High-Fat Diet

Raubenheimer, Peter; Nyirenda, Moffat; Walker, Brian R.

doi:10.2337/db06-0097

Cited by 164 publications

(118 citation statements)

References 40 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Several studies indicate a link between liver lipid content and hepatic insulin resistance (46)(47)(48). However, other studies conclude that elevated liver fat per se does not impair hepatic insulin sensitivity (49,50). With these current data, it is important to consider that hepatic TGs are lowered in Lepr loxTB × POMC-cre mice versus Lepr loxTB littermates, but they are not normalized to WT levels.…”

Section: Figurementioning

confidence: 83%

Direct leptin action on POMC neurons regulates glucose homeostasis and hepatic insulin sensitivity in mice

et al. 2012

View full text Add to dashboard Cite

Leptin action on its receptor (LEPR) stimulates energy expenditure and reduces food intake, thereby lowering body weight. One leptin-sensitive target cell mediating these effects on energy balance is the proopiomelanocortin (POMC) neuron. Recent evidence suggests that the action of leptin on POMC neurons regulates glucose homeostasis independently of its effects on energy balance. Here, we have dissected the physiological impact of direct leptin action on POMC neurons using a mouse model in which endogenous LEPR expression was prevented by a LoxP-flanked transcription blocker (loxTB), but could be reactivated by Cre recombinase. Mice homozygous for the Lepr loxTB allele were obese and exhibited defects characteristic of LEPR deficiency. Reexpression of LEPR only in POMC neurons in the arcuate nucleus of the hypothalamus did not reduce food intake, but partially normalized energy expenditure and modestly reduced body weight. Despite the moderate effects on energy balance and independent of changes in body weight, restoring LEPR in POMC neurons normalized blood glucose and ameliorated hepatic insulin resistance, hyperglucagonemia, and dyslipidemia.Collectively, these results demonstrate that direct leptin action on POMC neurons does not reduce food intake, but is sufficient to normalize glucose and glucagon levels in mice otherwise lacking LEPR. IntroductionLeptin is an adipose-derived hormone that acts on its cognate receptors (LEPR) expressed by multiple neuronal groups in distinct areas of the brain (1). The canonical effect of leptin action in the brain is to regulate food intake and energy expenditure and thus body weight (2-4). In addition, leptin regulates several other physiological processes, including hepatic glucose production, insulin action, and glucagon levels (5-10). It is still unclear, however, which neurons mediate the varied physiological effects of leptin.One population of neurons targeted by leptin is proopiomelanocortin (POMC) cells in the arcuate nucleus of the hypothalamus (ARH) and nucleus of the solitary tract (NTS) (2, 3). Leptin action on POMC neurons in the ARH is considered a prototypical site of action in the control of energy balance. This view is partly based on results showing that loss of LEPR in POMC neurons increases body weight (8,11,12). Conversely, LEPR reexpression in the ARH (13), overexpression in the ARH (14-17), and transgenic expression in POMC neurons (18) lower body weight. Interestingly, these latter studies also show lowered blood glucose, suggesting that leptin-sensitive POMC neurons in the ARH directly modulate metabolism (13-18). In the current study, we developed what we believe to be a novel LEPR-null mouse model in which endogenous LEPR expression can be reexpressed in cells that normally express leptin receptors. Here, we reexpress LEPR only in POMC neurons to delineate the physiological effects on energy and metabolic homeostasis.

show abstract

Section: Figurementioning

confidence: 83%

Direct leptin action on POMC neurons regulates glucose homeostasis and hepatic insulin sensitivity in mice

et al. 2012

View full text Add to dashboard Cite

show abstract

“…Although we did not use a glucose-tolerance or euglycemic insulin-clamp test to verify whether mice with chronic (11-month) high-fat diet-induced obesity were insulinresistant or glucose-intolerant, the higher levels of blood glucose and serum insulin exhibited in these mice (Figures 2b and c) should indicate insulin resistance or glucose intolerance according to the previous literature in which male C57BL/6 mice were fed a high-fat diet for only 4 or 8 weeks. 48,49 Interestingly, these increases in the liver may have been due to elevation of Bmal1 and Crys expression, and elevation of CK1e expression did not abrogate or attenuate this augmentation. Further study is needed to confirm this contention.…”

Section: Discussionmentioning

confidence: 99%

Abnormal expressions of circadian-clock and circadian clock-controlled genes in the livers and kidneys of long-term, high-fat-diet-treated mice

Hsieh

et al. 2009

Int J Obes

100

View full text Add to dashboard Cite

Objectives: Physiological and behavioral circadian rhythmicities are exhibited by all mammals and are generated by intracellular levels of circadian oscillators, which are composed of transcriptional/translational feedback loops involving a set of circadianclock genes, such as Clock, Per1-3, Cry1-2, Bmal1, Dbp, E4BP4 and CK1e. These circadian-clock genes play important roles in regulating circadian rhythms and also energy homeostasis and metabolism. Determining whether obesity induced by high-fat diet affected the expressions of circadian-clock genes and their related genes in peripheral tissues, was the main focus of this study. To address this issue, we fed male C57BL/6 mice a high-fat diet for 11 months to induce obesity, hyperglycemic, hypercholesterolemic and hyperinsulinemic symptoms, and used quantitative real-time reverse transcription-PCR to measure gene expression levels. Results: We found that the expressions of circadian-clock genes and circadian clock-controlled genes, including Per1-3, Cry1-2, Bmal1, Dbp, E4BP4, CK1e, PEPCK, PDK4 and NHE3, were altered in the livers and/or kidneys. Conclusions: These results indicate that obesity induced by high-fat diet alters the circadian-clock system, and obesity and metabolic syndrome are highly correlated with the expressions of circadian-clock genes and their downstream, circadian clockcontrolled genes.

show abstract

“…Recently, studies suggested that manipulation of dietary choline or alteration of pathways in choline metabolism may influence energy expenditure and adiposity. Mice fed a methionine-and choline-deficient diet were hypermetabolic, lost weight (49), and had better insulin sensitivity and glucose tolerance (50). Mice with the Pemt gene (making PtdCho from phosphatidylethanolamine) deleted had normal metabolic parameters on a regular chow diet compared with wild type controls; however, when fed a high fat diet, they had increased oxygen consumption and RER, accumulated less body fat, and had increased glucose sensitivity (51).…”

Section: Discussionmentioning

confidence: 99%

Mouse Betaine-Homocysteine S-Methyltransferase Deficiency Reduces Body Fat via Increasing Energy Expenditure and Impairing Lipid Synthesis and Enhancing Glucose Oxidation in White Adipose Tissue

Teng

Ellis

Coleman

et al. 2012

Journal of Biological Chemistry

View full text Add to dashboard Cite

A Choline-Deficient Diet Exacerbates Fatty Liver but Attenuates Insulin Resistance and Glucose Intolerance in Mice Fed a High-Fat Diet

Cited by 164 publications

References 40 publications

Direct leptin action on POMC neurons regulates glucose homeostasis and hepatic insulin sensitivity in mice

Direct leptin action on POMC neurons regulates glucose homeostasis and hepatic insulin sensitivity in mice

Abnormal expressions of circadian-clock and circadian clock-controlled genes in the livers and kidneys of long-term, high-fat-diet-treated mice

Mouse Betaine-Homocysteine S-Methyltransferase Deficiency Reduces Body Fat via Increasing Energy Expenditure and Impairing Lipid Synthesis and Enhancing Glucose Oxidation in White Adipose Tissue

Contact Info

Product

Resources

About