Inhibition of hypothalamic neuropeptide Y gene expression by insulin.

Schwartz, Michael W.; Sipols, Alfred J.; Marks, Jonathan L.; Sanacora, Gerard; White, J.; Scheurink, Antonius; Kahn, Steven E.; Baskin, Denis G.; Woods, Stephen C.; Figlewicz, Dianne P.

doi:10.1210/endo.130.6.1597158

Cited by 417 publications

(133 citation statements)

References 25 publications

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“…Since obesity in these animals results from mutation of the leptin receptor (fa/fa) (3), our data suggest that normal leptin receptor function is required for the effect of icv leptin to influence hypothalamic NPY and CRH gene expression. These results are similar to those of previous studies demonstrating that icv administration of insulin lowers arcuate nucleus NPY mRNA levels during fasting in normal rats, but not in obese fa/fa rats (16,28). Insulin and leptin, therefore, both appear to contribute to the regulation of hypothalamic NPY gene expression during fasting.…”

Section: Discussionsupporting

confidence: 91%

Identification of targets of leptin action in rat hypothalamus.

Schwartz¹,

Seeley²,

Campfield³

et al. 1996

J. Clin. Invest.

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1,389

821

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The hypothesis that leptin (OB protein) acts in the hypothalamus to reduce food intake and body weight is based primarily on evidence from leptin-deficient, ob/ob mice. To investigate whether leptin exerts similar effects in normal animals, we administered leptin intracerebroventricularly (icv) to Long-Evans rats. Leptin administration (3.5 g icv) at the onset of nocturnal feeding reduced food intake by 50% at 1 h and by 42% at 4 h, as compared with vehicletreated controls (both P Ͻ 0.05). To investigate the basis for this effect, we used in situ hybridization (ISH) to determine whether leptin alters expression of hypothalamic neuropeptides involved in energy homeostasis. Two injections of leptin (3.5 g icv) during a 40 h fast significantly decreased levels of mRNA for neuropeptide Y (NPY, which stimulates food intake) in the arcuate nucleus ( Ϫ 24%) and increased levels of mRNA for corticotrophin releasing hormone (CRH, an inhibitor of food intake) in the paraventricular nucleus (by 38%) (both P Ͻ 0.05 vs. vehicle-treated controls). To investigate the anatomic basis for these effects, we measured leptin receptor gene expression in rat brain by ISH using a probe complementary to mRNA for all leptin receptor splice variants. Leptin receptor mRNA was densely concentrated in the arcuate nucleus, with lower levels present in the ventromedial and dorsomedial hypothalamic nuclei and other brain areas involved in energy balance. These findings suggest that leptin action in rat hypothalamus involves altered expression of key neuropeptide genes, and implicate leptin in the hypothalamic response to fasting. ( J. Clin. Invest. 1996. 98:1101-1106.)

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Section: Discussionsupporting

confidence: 91%

Identification of targets of leptin action in rat hypothalamus.

Schwartz¹,

Seeley²,

Campfield³

et al. 1996

J. Clin. Invest.

Self Cite

1,389

821

View full text Add to dashboard Cite

show abstract

“…The ARC is very rich in insulin receptors although their precise relationship to the NPY-synthesizing cells is not yet defined [ 1321. Insulin-injected ICV in food-deprived lean rats prevents the rise in NPY mRNA levels which normally occurs in the ARC, but in an interesting parallel with its appetite-suppressing effects, insulin fails to affect NPY mRNA in similarly treated f a / f u Zucker rats [ 142,1431. Insulin may, therefore, enter the hypothalamus from the circulation and inhibit the NPYergic projection from the ARC to the PVN.…”

Section: Insulin and Insulin Deficiencymentioning

confidence: 97%

“…This could readily explain the pathway's increased activity in food deprivation, diabetes, exercise and lactation as circulating insulin levels are substantially reduced in all these conditions. By contrast, the ARC-PVN pathway could be activated in genetically obese rodents because their hypothalamic NPYergic neurones are insensitive to inhibition by insulin, even at the grossly elevated circulating levels which characterize these syndromes [7,103,142].…”

Section: Insulin and Insulin Deficiencymentioning

confidence: 99%

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Neuropeptide Y and energy balance: one way ahead for the treatment of obesity?

Dryden

Frankish

Wang

et al. 1994

Eur J Clin Investigation

122

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Abstract. Obesity is a vast and ever-expanding problem in affluent societies, which we have so far failed to confront. Over 20% of Western European and North American adults are overweight to a degree which may potentially shorten their life expectancy. Obesity has well-known associations with non-insulin-dependent diabetes (NIDDM), hypertension, dyslipidaemia and coronary heart disease, as well as less obvious links with diseases such as osteoarthrosis and various malignancies; it also causes considerable problems through reduced mobility and decreased quality of life. The overall financial burden of obesity is impossible to calculate precisely, but may account for 6-8% of total health-care expenditure in North America [ 13 (similar estimates probably apply to Western Europe).Obesity is difficult to treat and many patients remain obstinately overweight despite our best efforts. The available options range from behavioural therapy to gastrointestinal surgery and include numerous drugs designed to suppress appetite or increase energy expenditure. As in many other areas of medicine, the length and diversity of this list are reliable signs that effective treatment is still beyond our reach.This article argues that new anti-obesity drugs may emerge from recent advances in understanding the control of energy balance in rodents. The discussion is structured around neuropeptide Y (NPY), a major brain peptide which at present appears to be important in regulating energy balance and seems a promising candidate for therapeutic exploitation.

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“…Importantly, these 2 populations of neurons have opposing effects on food intake and body weight; the activation of POMC neurons results in reduced food intake and weight loss, whereas the activation of NPY/AgRP neurons results in increased food intake and weight gain. Direct delivery of insulin into the brain increases the expression of anorexigenic peptides α-melanocyte stimulating hormone and cocaine- and amphetamine-regulated transcript, and decreases the expression of the orexigenic peptides NPY and AgRP [64,65,66]. Accordingly, central and intranasal delivery of insulin resulted in reduced food intake in rats, baboons, and humans [67,68,69].…”

Section: Ir Expression In the Cns And Its Signaling Pathwaysmentioning

confidence: 99%

Hypothalamic Insulin Resistance in Obesity: Effects on Glucose Homeostasis

Chen

Balland

Cowley³

2017

Neuroendocrinology

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The central link between obesity and type 2 diabetes is the development of insulin resistance. To date, it is still not clear whether hyperinsulinemia causes insulin resistance, which underlies the pathogenesis of obesity-associated type 2 diabetes, owing to the sophisticated regulatory mechanisms that exist in the periphery and in the brain. In recent years, accumulating evidence has demonstrated the existence of insulin resistance within the hypothalamus. In this review, we have integrated the recent discoveries surrounding both central and peripheral insulin resistance to provide a comprehensive overview of insulin resistance in obesity and the regulation of systemic glucose homeostasis. In particular, this review will discuss how hyperinsulinemia and hyperleptinemia in obesity impair insulin sensitivity in tissues such as the liver, skeletal muscle, adipose tissue, and the brain. In addition, this review highlights insulin transport into the brain, signaling pathways associated with hypothalamic insulin receptor expression in the regulation of hepatic glucose production, and finally the perturbation of systemic glucose homeostasis as a consequence of central insulin resistance. We also suggest future approaches to overcome both central and peripheral insulin resistance to treat obesity and type 2 diabetes.

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Inhibition of hypothalamic neuropeptide Y gene expression by insulin.

Cited by 417 publications

References 25 publications

Identification of targets of leptin action in rat hypothalamus.

Identification of targets of leptin action in rat hypothalamus.

Neuropeptide Y and energy balance: one way ahead for the treatment of obesity?

Hypothalamic Insulin Resistance in Obesity: Effects on Glucose Homeostasis

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