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Hexose metabolism in pancreatic islets. Regulation of aerobic glycolysis and pyruvate decarboxylation.
Authors:W J Malaisse  J Rasschaert  I Conget  A Sener
Institution:Labortory of Experimental Medicine, Brussels Free University, Belgium.
Abstract:1. D-Glucose (0.5-16.7 mM) preferentially stimulates aerobic glycolysis and D-3,4-14C]glucose oxidation, relative to D-5-3H]glucose utilization in rat pancreatic islets, the concentration dependency of such a preferential effect displaying a sigmoidal pattern. 2. Inorganic and organic calcium antagonists, as well as Ca2+ deprivation, only cause a minor decrease in the ratio between D-3,4-14C]glucose oxidation and D-5-3H]glucose utilization in islets exposed to a high concentration of the hexose (16.7 mM). 3. Non-glucidic nutrient secretagogues such as 2-aminobicyclo2,2,1]heptane-2-carboxylate (BCH), 2-ketoisocaproate and 3-phenylpyruvate fail to stimulate aerobic glycolysis and D-3,4-14C]glucose oxidation in islets exposed to 6.0 mM D-glucose. Nevertheless, BCH augments 1-14C]pyruvate and 2-14C]pyruvate oxidation. 4. The glucose-induced increment in the paired ratio between D-3,4-14C]glucose oxidation and D-5-3H]glucose utilization is impaired in the presence of either cycloheximide or ouabain. 5. These findings suggest that the preferential effect of D-glucose upon aerobic glycolysis and pyruvate decarboxylation is not attributable solely to a Ca(2+)-induced activation of FAD-linked glycerophosphate dehydrogenase and/or pyruvate dehydrogenase, but may also involve an ATP-modulated regulatory process.
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