Additive effect of contraction and insulin on glucose uptake and glycogen synthase in muscle with different glycogen contents

Author:

Lai Yu-Chiang12,Zarrinpashneh Elham3,Jensen Jørgen1

Affiliation:

1. Department of Physiology, National Institute of Occupational Health and

2. Department of Physical Performance, Norwegian School of Sport Sciences Oslo, Norway; and

3. Medical Research Council Protein Phosphorylation Unit, College of Life Science, University of Dundee, Dundee, United Kingdom

Abstract

Insulin and contraction regulate glucose uptake and glycogen synthase (GS) via distinct mechanisms in skeletal muscles, and an additive effect has been reported. Glycogen content is known to influence both contraction- and insulin-stimulated glucose uptake and GS activity. Our study reports that contraction and insulin additively stimulate glucose uptake in rat epitrochlearis muscles with normal (NG) and high (HG) glycogen contents, but the additive effect was only partial. In muscles with low glycogen (LG) content no additive effect was seen, but glucose uptake was higher in LG than in NG and HG during contraction, insulin stimulation, and when the two stimuli were combined. In LG, contraction-stimulated AMP-activated protein kinase (AMPK) activity and insulin-stimulated PKB phosphorylation were higher than in NG and HG, but phosphorylation of Akt substrate of 160 kDa was not elevated correspondingly. GLUT4 content was 50% increased in LG (rats fasted 24 h), which may explain the increased glucose uptake. Contraction and insulin also additively increased GS fractional activity in NG and HG but not in LG. GS fractional activity correlated most strongly with GS Ser641phosphorylation ( R −0.94, P < 0.001). GS fractional activity also correlated with GS Ser7,10phosphorylation, but insulin did not reduce GS Ser7,10phosphorylation. In conclusion, an additive effect of contraction and insulin on glucose uptake and GS activity occurs in muscles with normal and high glycogen content but not in muscles with low glycogen content. Furthermore, contraction, insulin, and glycogen content all regulate GS Ser641phosphorylation and GS fractional activity in concert.

Publisher

American Physiological Society

Subject

Physiology (medical),Physiology

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