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1. Regulation of astrocyte metabolism by mitochondrial translocator protein 18kDa.

2. The contribution of hypothalamic macroglia to the regulation of energy homeostasis.

3. Evidence for a novel functional role of astrocytes in the acute homeostatic response to high-fat diet intake in mice.

4. Gender-specific roles for the melanocortin-3 receptor in the regulation of the mesolimbic dopamine system in mice.

5. Obesity induced by a high-fat diet is associated with increased immune cell entry into the central nervous system.

6. Translocator protein 18 kDa (TSPO) is regulated in white and brown adipose tissue by obesity.

7. Regional astrogliosis in the mouse hypothalamus in response to obesity.

8. High-fat diet acutely affects circadian organisation and eating behavior.

9. Neurovascular unit on a chip: implications for translational applications.

10. Toll-like receptor 4 deficiency promotes the alternative activation of adipose tissue macrophages.

11. Melanocortin-3 receptor regulates the normal fasting response.

12. Melanocortin-4 receptor signaling is required for weight loss after gastric bypass surgery.

13. Physiological roles of the melanocortin MC₃ receptor.

14. Characterization of the hyperphagic response to dietary fat in the MC4R knockout mouse.

15. Assessment of feeding behavior in laboratory mice.

16. Mouse models of the metabolic syndrome.

17. Obesity-induced inflammation in white adipose tissue is attenuated by loss of melanocortin-3 receptor signaling.

18. Role of the central melanocortin circuitry in adaptive thermogenesis of brown adipose tissue.

19. The role of the central melanocortin system in the regulation of food intake and energy homeostasis: lessons from mouse models.

20. Characterization of leptin-responsive neurons in the caudal brainstem.

21. Interactions between gut peptides and the central melanocortin system in the regulation of energy homeostasis.

22. Characterization of a naturally-occurring polymorphism in the UHR-1 gene encoding the putative rat prolactin-releasing peptide receptor.

23. Peptide YY3-36 inhibits food intake in mice through a melanocortin-4 receptor-independent mechanism.

24. Cholecystokinin-mediated suppression of feeding involves the brainstem melanocortin system.

25. The central melanocortin system and the integration of short- and long-term regulators of energy homeostasis.

26. Repeated administration of the anorectic factor prolactin-releasing peptide leads to tolerance to its effects on energy homeostasis.

27. PRL-releasing peptide reduces food intake and may mediate satiety signaling.

28. PRL-releasing peptide interacts with leptin to reduce food intake and body weight.

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