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Insulin-induced hypoglycemia increases hepatic sensitivity to glucagon in dogs
Noelia Rivera, … , Peter J. Roach, Alan D. Cherrington
Noelia Rivera, … , Peter J. Roach, Alan D. Cherrington
Published November 15, 2010
Citation Information: J Clin Invest. 2010;120(12):4425-4435. https://doi.org/10.1172/JCI40919.
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Research Article Metabolism

Insulin-induced hypoglycemia increases hepatic sensitivity to glucagon in dogs

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Abstract

In individuals with type 1 diabetes, hypoglycemia is a common consequence of overinsulinization. Under conditions of insulin-induced hypoglycemia, glucagon is the most important stimulus for hepatic glucose production. In contrast, during euglycemia, insulin potently inhibits glucagon’s effect on the liver. The first aim of the present study was to determine whether low blood sugar augments glucagon’s ability to increase glucose production. Using a conscious catheterized dog model, we found that hypoglycemia increased glucagon’s ability to overcome the inhibitory effect of insulin on hepatic glucose production by almost 3-fold, an effect exclusively attributable to marked enhancement of the effect of glucagon on net glycogen breakdown. To investigate the molecular mechanism by which this effect comes about, we analyzed hepatic biopsies from the same animals, and found that hypoglycemia resulted in a decrease in insulin signaling. Furthermore, hypoglycemia and glucagon had an additive effect on the activation of AMPK, which was associated with altered activity of the enzymes of glycogen metabolism.

Authors

Noelia Rivera, Christopher J. Ramnanan, Zhibo An, Tiffany Farmer, Marta Smith, Ben Farmer, Jose M. Irimia, Wanda Snead, Margaret Lautz, Peter J. Roach, Alan D. Cherrington

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Figure 7

AMPK signaling.

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AMPK signaling.
AMPK phosphorylation at (A) Thr172 (index of activation)...
AMPK phosphorylation at (A) Thr172 (index of activation) and (B) Ser485 (index of inhibition by insulin) and (C) ACC (Ser79) phosphorylation, relative to levels observed in basal control animals. Values are mean ± SEM; n = 3–4 per group. §P < 0.05 vs. basal; *P < 0.05 vs. corresponding euglycemic group; †P < 0.05, GH vs. SH; #P < 0.05, GE vs. SE.

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