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Central injection of fibroblast growth factor 1 induces sustained remission of diabetic hyperglycemia in rodents.

Citation
Scarlett, J. M., et al. “Central Injection Of Fibroblast Growth Factor 1 Induces Sustained Remission Of Diabetic Hyperglycemia In Rodents.”. Nature Medicine, pp. 800-6.
Center University of Washington
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Author Jarrad M Scarlett, Jennifer M Rojas, Miles E Matsen, Karl J Kaiyala, Darko Stefanovski, Richard N Bergman, Hong T Nguyen, Mauricio D Dorfman, Louise Lantier, David H Wasserman, Zaman Mirzadeh, Terry G Unterman, Gregory J Morton, Michael W Schwartz
Abstract

Type 2 diabetes (T2D) is among the most common and costly disorders worldwide. The goal of current medical management for T2D is to transiently ameliorate hyperglycemia through daily dosing of one or more antidiabetic drugs. Hypoglycemia and weight gain are common side effects of therapy, and sustained disease remission is not obtainable with nonsurgical approaches. On the basis of the potent glucose-lowering response elicited by activation of brain fibroblast growth factor (FGF) receptors, we explored the antidiabetic efficacy of centrally administered FGF1, which, unlike other FGF peptides, activates all FGF receptor subtypes. We report that a single intracerebroventricular injection of FGF1 at a dose one-tenth of that needed for antidiabetic efficacy following peripheral injection induces sustained diabetes remission in both mouse and rat models of T2D. This antidiabetic effect is not secondary to weight loss, does not increase the risk of hypoglycemia, and involves a novel and incompletely understood mechanism for increasing glucose clearance from the bloodstream. We conclude that the brain has an inherent potential to induce diabetes remission and that brain FGF receptors are potential pharmacological targets for achieving this goal.

Year of Publication
2016
Journal
Nature medicine
Volume
22
Issue
7
Number of Pages
800-6
Date Published
12/2016
ISSN Number
1546-170X
DOI
10.1038/nm.4101
Alternate Journal
Nat. Med.
PMID
27213816
PMCID
PMC4938755
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