Transgenic overexpression of neuromedin U promotes leanness and hypophagia in mice

Kowalski, Timothy J.; Spar, Brian D.; Markowitz, Lisa; Maguire, Mandy J.; Головко, Андрей; Yang, Shijun; Farley, Constance; Cook, John A.; Tetzloff, Glen; Hoos, Lizbeth; Vecchio, Robert A. Del; Kazdoba, Tatiana M.; McCool, Martha F.; Hwa, Joyce; Hyde, Lynn A.; Davis, Harry R.; Vassileva, Galya; Hedrick, Joseph A.; Gustafson, Eric L.

doi:10.1677/joe.1.05948

Cited by 68 publications

(57 citation statements)

References 60 publications

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“…We found that increased NMU in the xenograft tumors were associated with cancer cachexia in mice. NMU itself has an anorexigenic effect in animals (Howard et al, 2000;Hanada et al, 2004;Shousha et al, 2006), and transgenic overexpression of it promotes leanness in mice (Kowalski et al, 2005). As NMU can function as a proinflammatory mediator by promoting interleukin (IL)-6 production in Th2-type T cells or macrophages (Johnson et al, 2004;Moriyama et al, 2006) and inhibition of IL-6 can partially attenuate or reverse cancer cachexia (Strassmann and Kambayashi, 1995), this might be a mechanism underlying NMU-mediated cancer cachexia.…”

Section: Discussionmentioning

confidence: 99%

Neuromedin U is regulated by the metastasis suppressor RhoGDI2 and is a novel promoter of tumor formation, lung metastasis and cancer cachexia

McRoberts

Berr

et al. 2006

Oncogene

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Most deaths from urinary bladder cancer are owing to metastatic disease. A reduction in Rho GDP Dissociation Inhibitor 2 (RhoGDI2) protein has been associated with increased risk of metastasis in patients with locally advanced bladder cancer, whereas in animal models, RhoGDI2 reconstitution in cells without expression results in lung metastasis suppression. Recently, we noted an inverse correlation between tumor RhoGDI2 and Neuromedin U (NMU) expression, suggesting that NMU might be a target of the lung metastasis suppressor effect of RhoGDI2. Here we evaluated whether NMU is regulated by RhoGDI2 and is functionally important in tumor progression. We used small interfering RNA knockdown of endogenous RhoGDI2 in poorly tumorigenic and nonmetastatic human bladder cancer T24 cells and observed increased NMU RNA expression. Although NMU overexpression did not increase the monolayer growth of T24 or related T24T poorly metastatic human bladder cancer cells, it did augment anchorage-independent growth for the latter. Overexpression of NMU in T24 and T24T cells significantly promoted tumor formation of both cell lines in nude mice, but did not alter the growth rate of established tumors. Furthermore, NMU-overexpressing xenografts were associated with lower animal body weight than control tumors, indicating a possible role of NMU in cancer cachexia. NMU overexpression in T24T cells significantly enhanced their lung metastatic ability. Bioluminescent in vivo imaging revealed that lung metastases in T24T grew faster than the same tumors in the subcutaneous microenvironment. In conclusion, NMU is a RhoGDI2-regulated gene that appears important for tumorigenicity, lung metastasis and cancer cachexia, and thus a promising therapeutic target in cancer.

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Section: Discussionmentioning

confidence: 99%

Neuromedin U is regulated by the metastasis suppressor RhoGDI2 and is a novel promoter of tumor formation, lung metastasis and cancer cachexia

McRoberts

Berr

et al. 2006

Oncogene

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“…injection of NMU gives a clear catabolic response, increasing core body temperature and locomotor activity, reducing food intake (Nakazato et al 2000) and acute administration of NMU into the PVN has clear anorexigenic effects (Wren et al 2002); however, chronic injections of NMU into the PVN have no effect on food intake or body weight. Nevertheless, the NMU knockout mouse shows clear hyperphagia and obesity ) and the transgenic mouse overexpressing NMU is lean and hypophagic (Kowalski et al 2005). Recently, it has been demonstrated that at least some of the effects of leptin are mediated via NMU (Jethwa et al 2005).…”

Section: Discussionmentioning

confidence: 99%

“…It is also involved in the regulation of circadian rhythmicity (Nakahara et al 2004) and luteinizing hormone secretion (Quan et al 2003). The NMU knockout mouse is hyperphagic and obese , while the transgenic mouse, overexpressing NMU, is lean and hypophagic (Kowalski et al 2005) providing strong support for the role of NMU in energy balance.…”

Section: Introductionmentioning

confidence: 99%

Negative energy balance and leptin regulate neuromedin-U expression in the rat pars tuberalis

Nogueiras¹,

Tovar²,

Mitchell³

et al. 2006

Journal of Endocrinology

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Central neuromedin U (NMU) functions in energy balance, the hypothalamic-pituitary-adrenal axis, LH release and circadian rhythmicity. In rats, high levels of NMU occur in the hypothalamic suprachiasmatic nuclei and the pars tuberalis of the pituitary. NMU expression in the pars tuberalis appears to be downregulated in the Zucker fatty (fa/fa) rat, lacking functional leptin receptors. In contrast, in the dorsomedial (DMH) nuclei of the mouse, NMU expression is higher in the ob/ob mouse, lacking leptin, and is upregulated by fasting. However, leptin appears not to change NMU gene expression in either the mouse DMH or the rat pars tuberalis. Thus, the present study aims to better identify factors influencing central NMU expression in the rat pars tuberalis. SpragueDawley rats were fasted and/or challenged with intracerebroventricular leptin or ghrelin and gene expression was measured using real-time reverse transcriptase-PCR and quantitative in situ hybridisation with riboprobes specific for NMU and NMU receptor (NMU-R2). NMU expression in the rat pars tuberalis was elevated by fasting. Ghrelin administration had no effect on the level of NMU expression, but leptin was found to diminish the expression in a concentration-and time-dependent manner. NMU-R2 expression was unchanged in any of the groups measured. These results suggest that NMU expression in rat pars tuberalis is upregulated in states of negative energy balance, and this may be mediated indirectly by changes in leptin levels. These results demonstrate a link between energy balance and NMU expression in the pars tuberalis of the pituitary.

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“…These mice also develop late-onset hyperglycemia and hyperlipidemia [75]. Transgenic mice that overexpress NMU are hypophagic, and have reduced body weight, low somatic and liver fat, and improved insulin sensitivity [76]. On a high fat diet, these mice remain lighter than wild types and eat less [76].…”

Section: Neuromedin Umentioning

confidence: 99%

“…Transgenic mice that overexpress NMU are hypophagic, and have reduced body weight, low somatic and liver fat, and improved insulin sensitivity [76]. On a high fat diet, these mice remain lighter than wild types and eat less [76]. A variant in the human NMU gene has also been linked to obesity in the human population [77].…”

Section: Neuromedin Umentioning

confidence: 99%

Peptides and Their Potential Role in the Treatment of Diabetes and Obesity

Greenwood

Bloom²,

Murphy

2011

Rev Diabet Stud

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■ AbstractIt is estimated that 347 million people worldwide have diabetes and that over 1.5 billion adults worldwide are overweight. Predictions suggest these rates are increasing. Diabetes is a common complication in overweight and obese subjects, and in 2004, an estimated 3.4 million people died from consequences of high blood sugar. Thus, there is great interest in revealing the physiological systems that regulate body weight and blood sugar. Several peptidergic systems within the central nervous system and the periphery regulate energy homeostasis. A number of these systems have been investigated as potential treatments for obesity and the metabolic syndrome. However, manipulation of peptidergic systems poses many problems. This review discusses the peptidergic systems currently attracting research interest for their clinical potential to treat obesity. We consider first neuropeptides in the brain, including the orexigenic neuropeptide Y and melanin-concentrating hormone, and anorectic factors such as the melanocortins, ciliary neurotrophic factor, and neuromedin U. We subsequently discuss the utility of targeting peripheral gut peptides, including pancreatic polypeptide, peptide YY, amylin, and the gastric hormone ghrelin. Also, we analyze the evidence that these factors or drugs based on them may be therapeutically useful, while considering the disadvantages of using such peptides in a clinical context.

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Transgenic overexpression of neuromedin U promotes leanness and hypophagia in mice

Cited by 68 publications

References 60 publications

Neuromedin U is regulated by the metastasis suppressor RhoGDI2 and is a novel promoter of tumor formation, lung metastasis and cancer cachexia

Neuromedin U is regulated by the metastasis suppressor RhoGDI2 and is a novel promoter of tumor formation, lung metastasis and cancer cachexia

Negative energy balance and leptin regulate neuromedin-U expression in the rat pars tuberalis

Peptides and Their Potential Role in the Treatment of Diabetes and Obesity

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