Effects of streptozotocin-induced diabetes and insulin treatment on the hypothalamic melanocortin system and muscle uncoupling protein 3 expression in rats.

Havel, Peter J.; Hahn, Tina M.; Sindelar, Dana K.; Baskin, Denis G.; Dallman, Mary F.; Weigle, David S.; Schwartz, Michael W.

doi:10.2337/diabetes.49.2.244

Cited by 128 publications

(105 citation statements)

References 55 publications

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“…However, increases of AgRP mRNA in response to both fasting and genetic leptin deficiency are substantially greater than observed for NPY mRNA levels, whereas such differences are not apparent in STZ-diabetic rats. 72 Thus, although NPY and AgRP are both upregulated in the arcuate nucleus in response to the same stimuli, the magnitude of this response may differ. Distinct mechanisms may therefore govern the control of NPY and AgRP biosynthesis.…”

Section: Agouti-related Peptide and The Melanocortin Systemmentioning

confidence: 99%

The NPY/AgRP neuron and energy homeostasis

2001

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Kennedy hypothesized nearly 50 y ago that negative feedback regulation of body fat stores involves hormones that circulate in proportion to adiposity and enter the brain, where they exert inhibitory effects on food intake and energy balance. Recent studies implicate leptin and insulin as 'adiposity signals' to the brain that promote negative energy balance in two ways: by inhibiting 'anabolic' hypothalamic neuronal circuits that stimulate food intake and promote weight gain, and by activating 'catabolic' pathways that reduce food intake and body weight. Chief among candidate 'anabolic' effector pathways is the NPY=AgRP neuron, found only in the hypothalamic arcuate nucleus. These neurons make peptides that potently stimulate food intake not only by increasing neuropeptide Y (NPY) signaling, but by reducing melanocortin signaling via the release of agoutirelated peptide (AgRP), an endogenous melanocortin 3=4 receptor antagonist. Since NPY=AgRP neurons express receptors for leptin and insulin and are inhibited by these hormones, they are activated by a decrease of leptin or insulin signaling. Fasting, uncontrolled diabetes, and genetic leptin deficiency are examples of conditions in which food intake increases via a mechanism hypothesized to involve NPY=AgRP neurons. Data are reviewed which illustrate the role of these neurons in adaptive and maladaptive states characterized by hyperphagia and weight gain.

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Section: Agouti-related Peptide and The Melanocortin Systemmentioning

confidence: 99%

The NPY/AgRP neuron and energy homeostasis

2001

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“…Recent investigations (13,21) have demonstrated that UCPs can prevent mitochondrial ROS formation. The different members of the UCP family have distinct tissue distributions (19,22,23). Tissue localization as well as regulation confer different roles for the family members.…”

mentioning

confidence: 99%

“…For example, UCP1 is strictly restricted to brown adipose tissue, and its principal function is believed to be the generation of body heat (19,24). UCP3 tissue distribution is predominantly limited to skeletal muscle, whereas UCP2 expression is widespread in spleen, lung, stomach, white adipose tissue, and brain (23,25). Both UCPs regulate energy metabolism and weight regulation (19,20,26).…”

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confidence: 99%

Uncoupling Proteins Prevent Glucose-Induced Neuronal Oxidative Stress and Programmed Cell Death

Vincent

Olzmann

Brownlee³

et al. 2004

Diabetes

156

137

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The central role of mitochondria in most pathways leading to programmed cell death (PCD) has focused our investigations into the mechanisms of glucose-induced neuronal degeneration. It has been postulated that hyperglycemic neuronal injury results from mitochondria membrane hyperpolarization and reactive oxygen species formation. The present study not only provides further evidence to support our model of glucose-induced PCD but also demonstrates a potent ability for uncoupling proteins (UCPs) to prevent this process. Dorsal root ganglion (DRG) neurons were screened for UCP expression by Western blotting and immunocytochemistry. The abilities of individual UCPs to prevent hyperglycemic PCD were assessed by adenovirus-mediated overexpression of UCP1 and UCP3. Interestingly, UCP3 is expressed not only in muscle, but also in DRG neurons under control conditions. UCP3 expression is rapidly downregulated by hyperglycemia in diabetic rats and by high glucose in cultured neurons. Overexpression of UCPs prevents glucose-induced transient mitochondrial membrane hyperpolarization, reactive oxygen species formation, and induction of PCD. The loss of UCP3 in DRG neurons may represent a significant contributing factor in glucose-induced injury. Furthermore, the ability to prevent UCP3 downregulation or to reproduce the uncoupling response in DRG neurons constitutes promising novel approaches to avert diabetic complications such as neuropathy. Diabetes 53: 726 -734, 2004

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“…Sub-populations of POMC neurons have been shown to co-express GABA and glutamate (Table 2). Perhaps not surprisingly, POMC/ CART neurons are regulated by insulin, leptin and ghrelin (Havel et al 2000, Cowley et al 2001, Balthasar et al 2004. Peripheral ghrelin peptide indirectly inhibits the activity of POMC/CART neurons in mice (Cowley et al 2003), but POMC/CART neurons may also be directly modulated by ghrelin-expressing neurons via synaptic communication (Guan et al 2008).…”

Section: Pomc/cart-expressing Neuronsmentioning

confidence: 99%

Neuroendocrine integration of nutritional signals on reproduction

Evans

Anderson

2017

Journal of Molecular Endocrinology

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Reproductive function in mammals is energetically costly and therefore tightly regulated by nutritional status. To enable this integration of metabolic and reproductive function, information regarding peripheral nutritional status must be relayed centrally to the gonadotropin-releasing hormone (GNRH) neurons that drive reproductive function. The metabolically relevant hormones leptin, insulin and ghrelin have been identified as key mediators of this 'metabolic control of fertility'. However, the neural circuitry through which they act to exert their control over GNRH drive remains incompletely understood. With the advent of Cre-LoxP technology, it has become possible to perform targeted gene-deletion and gene-rescue experiments and thus test the functional requirement and sufficiency, respectively, of discrete hormone-neuron signaling pathways in the metabolic control of reproductive function. This review discusses the findings from these investigations, and attempts to put them in context with what is known from clinical situations and wild-type animal models. What emerges from this discussion is clear evidence that the integration of nutritional signals on reproduction is complex and highly redundant, and therefore, surprisingly difficult to perturb. Consequently, the deletion of individual hormone-neuron signaling pathways often fails to cause reproductive phenotypes, despite strong evidence that the targeted pathway plays a role under normal physiological conditions. Although transgenic studies rarely reveal a critical role for discrete signaling pathways, they nevertheless prove to be a good strategy for identifying whether a targeted pathway is absolutely required, critically involved, sufficient or dispensable in the metabolic control of fertility.

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Effects of streptozotocin-induced diabetes and insulin treatment on the hypothalamic melanocortin system and muscle uncoupling protein 3 expression in rats.

Cited by 128 publications

References 55 publications

The NPY/AgRP neuron and energy homeostasis

The NPY/AgRP neuron and energy homeostasis

Uncoupling Proteins Prevent Glucose-Induced Neuronal Oxidative Stress and Programmed Cell Death

Neuroendocrine integration of nutritional signals on reproduction

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