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Diabetes, Vol 42, Issue 5 757-763, Copyright © 1993 by American Diabetes Association
Fasting does not impair insulin-stimulated glucose uptake but alters intracellular glucose metabolism in conscious rats
JH Youn and TA Buchanan
Department of Physiology and Biophysics, University of Southern California School of Medicine, Los Angeles 90033.
Effects of 24-h and 48-h fasting on maximal insulin-stimulated whole-body
and muscle glucose uptake, glycogen synthesis, and glycolysis were studied
in conscious rats by combining the glucose clamp technique with tracer
methods. Fasting decreased body weight and basal plasma glucose, plasma
insulin, hepatic glucose output, and glucose clearance (P < 0.05 for
all). However, maximal insulin-stimulated whole-body glucose uptake,
normalized to body weight, was almost identical in fed, 24-h fasted, and
48-h fasted rats (191 +/- 8, 185 +/- 14, and 182 +/- 5 mumol.kg-1.min-1,
respectively; P > 0.7). Similarly, rates of insulin-stimulated glucose
uptake by four different skeletal muscles, estimated by the 2-deoxyglucose
injection technique, were not different among the three groups. In contrast
to glucose uptake, insulin-stimulated whole-body glycolysis was decreased
significantly after fasting (36% after 48 h fasting; P < 0.05), whereas
insulin-stimulated whole-body glycogen synthesis was increased (44% after
48 h fasting; P < 0.05). In fed rats, glycolysis was the major pathway
for glucose metabolism during hyperinsulinemia, accounting for 60 +/- 5% of
glucose uptake. This fraction was decreased significantly by fasting (P
< 0.01), so that after a 48-h fast, glycolysis accounted for only 40 +/-
3% of insulin-stimulated glucose uptake and glycogen synthesis became
predominant pathway, accounting for 60 +/- 3% of whole-body glucose
utilization. Whole-body patterns of glucose metabolism during
hyperinsulinemia were paralleled by glucose metabolism in individual
muscles.(ABSTRACT TRUNCATED AT 250 WORDS)

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Copyright © 1993 by the American Diabetes Association.
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