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Diabetes, Vol 48, Issue 10 1930-1936, Copyright © 1999 by American Diabetes Association
Calorie restriction increases insulin-stimulated glucose transport in skeletal muscle from IRS-1 knockout mice
AC Gazdag, CL Dumke, CR Kahn and GD Cartee
Department of Nutritional Sciences, University of Wisconsin, Madison 53706, USA.
Calorie restriction (CR), even for brief periods (4-20 days), results in
increased whole-body insulin sensitivity, in large part due to enhanced
insulin-stimulated glucose transport by skeletal muscle. Evidence suggests
that the cellular alterations leading to this effect are postreceptor steps
in insulin signaling. To determine whether insulin receptor substrate
(IRS)-1 is essential for the insulin-sensitizing effect of CR, we measured
in vitro 2-deoxyglucose (2DG) uptake in the presence and absence of insulin
by skeletal muscle isolated from wild-type (WT) mice and transgenic mice
lacking IRS-1 (knockout [KO]) after either ad libitum (AL) feeding or 20
days of CR (60% of ad libitum intake). Three muscles (soleus, extensor
digitorum longus [EDL], and epitrochlearis) from male and female mice
(4.5-6 months old) were studied. In each muscle, insulin-stimulated 2DG
uptake was not different between genotypes. For EDL and epitrochlearis,
insulin-stimulated 2DG uptake was greater in CR compared to AL groups,
regardless of sex. Soleus insulin-stimulated 2DG uptake was greater in CR
compared with AL in males but not females. The diet effect on 2DG uptake
was not different for WT and KO animals. Genotype also did not alter the
CR-induced decrease in plasma constituents (glucose, insulin, and leptin)
or body composition (body weight, fat pad/body weight ratio). Consistent
with previous studies in rats, IRS-1 protein expression in muscle was
reduced in WT-CR compared with WT-AL mice, and muscle IRS-2 abundance was
unchanged by diet. Skeletal muscle IRS-2 protein expression was
significantly lower in WT compared with KO mice. These data demonstrate
that IRS-1 is not essential for the CR-induced increase in
insulin-stimulated glucose transport in skeletal muscle, and the absence of
IRS-1 does not modify any of the characteristic adaptations of CR that were
evaluated.

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Copyright © 1999 by the American Diabetes Association.
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