Nervous glucose sensing regulates postnatal β cell proliferation and glucose homeostasis
David Tarussio, … , Marc Foretz, Bernard Thorens
David Tarussio, … , Marc Foretz, Bernard Thorens
Published December 16, 2013
Citation Information: J Clin Invest. 2014;124(1):413-424. https://doi.org/10.1172/JCI69154.
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Research Article Metabolism

Nervous glucose sensing regulates postnatal β cell proliferation and glucose homeostasis

Abstract

How glucose sensing by the nervous system impacts the regulation of β cell mass and function during postnatal development and throughout adulthood is incompletely understood. Here, we studied mice with inactivation of glucose transporter 2 (Glut2) in the nervous system (NG2KO mice). These mice displayed normal energy homeostasis but developed late-onset glucose intolerance due to reduced insulin secretion, which was precipitated by high-fat diet feeding. The β cell mass of adult NG2KO mice was reduced compared with that of WT mice due to lower β cell proliferation rates in NG2KO mice during the early postnatal period. The difference in proliferation between NG2KO and control islets was abolished by ganglionic blockade or by weaning the mice on a carbohydrate-free diet. In adult NG2KO mice, first-phase insulin secretion was lost, and these glucose-intolerant mice developed impaired glucagon secretion when fed a high-fat diet. Electrophysiological recordings showed reduced parasympathetic nerve activity in the basal state and no stimulation by glucose. Furthermore, sympathetic activity was also insensitive to glucose. Collectively, our data show that GLUT2-dependent control of parasympathetic activity defines a nervous system/endocrine pancreas axis that is critical for β cell mass establishment in the postnatal period and for long-term maintenance of β cell function.

Authors

David Tarussio, Salima Metref, Pascal Seyer, Lourdes Mounien, David Vallois, Christophe Magnan, Marc Foretz, Bernard Thorens

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Figure 7

Reduced islet number but same islet size distribution in control and NG2KO mice.

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Reduced islet number but same islet size distribution in control and NG2...
(A) Insulin staining of pancreatic sections from 24-week-old NC-fed control and NG2KO mice. Scale bars: 2 mm. (B) Islet number per pancreas section is reduced in adult NG2KO as compared with control mice. (C) Total pancreatic insulin content in 24-week-old control and NG2KO mice. (D) Islet size distribution in control (C) and NG2KO (KO) mice at the indicated age and fed NC or a HFD. Numbers within the bars indicate the frequency in percentage of the corresponding islet size. (E) Pancreas weight of control and NG2KO mice at the indicated age and fed NC or a HFD. Data are mean ± SEM; n = 4–6. *P < 0.05; **P < 0.01.