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Publication : Pharmacology, physiology, and mechanisms of incretin hormone action.

First Author  Campbell JE Year  2013
Journal  Cell Metab Volume  17
Issue  6 Pages  819-37
PubMed ID  23684623 Mgi Jnum  J:199265
Mgi Id  MGI:5501387 Doi  10.1016/j.cmet.2013.04.008
Citation  Campbell JE, et al. (2013) Pharmacology, physiology, and mechanisms of incretin hormone action. Cell Metab 17(6):819-37
abstractText  Incretin peptides, principally GLP-1 and GIP, regulate islet hormone secretion, glucose concentrations, lipid metabolism, gut motility, appetite and body weight, and immune function, providing a scientific basis for utilizing incretin-based therapies in the treatment of type 2 diabetes. Activation of GLP-1 and GIP receptors also leads to nonglycemic effects in multiple tissues, through direct actions on tissues expressing incretin receptors and indirect mechanisms mediated through neuronal and endocrine pathways. Here we contrast the pharmacology and physiology of incretin hormones and review recent advances in mechanisms coupling incretin receptor signaling to pleiotropic metabolic actions in preclinical studies. We discuss whether mechanisms identified in preclinical studies have potential translational relevance for the treatment of human disease and highlight controversies and uncertainties in incretin biology that require resolution in future studies.
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