To examine the relationship between the plasma glucose concentration (PG) and the pathways of hepatic glucose production (HGP), five groups of conscious rats were studied after a 6-h fast: (a) control rats (PG = 8.0±0.2 mM); (b) control rats (PG = 7.9±0.2 mM) with somatostatin and insulin replaced at the basal level; (c) control rats (PG = 18.1±0.2 mM) with somatostatin, insulin replaced at the basal level, and glucose infused to acutely raise plasma glucose by 10 mM; (d) control rats (PG = 18.0±0.2 mM) with somatostatin and glucose infusions to acutely reproduce the metabolic conditions of diabetic rats, i.e., hyperglycemia and moderate hypoinsulinemia; (e) diabetic rats (PG = 18.4±2.3 mM). All rats received an infusion of [3-3H]glucose and [U-14C]lactate. The ratio between hepatic [14C]UDP-glucose sp act (SA) and 2X [14C]-phosphoenolpyruvate (PEP) SA (the former reflecting glucose-6-phosphate SA) measured the portion of total glucose output derived from PEP-gluconeogenesis. In control rats, HGP was decreased by 58% in hyperglycemic compared to euglycemic conditions (4.5±0.3 vs. 10.6±0.2 mg/kg·min; P <0.01). When evaluated under identical glycemic conditions, HGP was significantly increased in diabetic rats (18.9±1.4 vs. 6.2±0.4 mg/kg·min; P < 0.01). In control rats, hyperglycemia increased glucose cycling (by 2.5-fold) and the contribution of gluconeogenesis to HGP (91% vs. 45%), while decreasing that of glycogenolysis (9% vs. 55%). Under identical plasma glucose and insulin concentrations, glucose cycling in diabetic rats was decreased (by 21%) and the percent contribution of gluconeogenesis to HGP (73%) was similar to that of controls (84%). These data indicate that: (a) hyperglycemia causes a marked inhibition of HGP mainly through the suppression of glycogenolysis and the increase in glucokinase flux, with no apparent changes in the fluxes through gluconeogenesis and glucose-6-phosphatase; under similar hyperglycemic hypoinsulinemic conditions: (b) HGP is markedly increased in diabetic rats; however, (c) the contribution of glycogenolysis and gluconeogenesis to HGP is similar to control animals.
CITATION STYLE
Rossetti, L., Giaccari, A., Barzilai, N., Howard, K., Sebel, G., & Hu, M. (1993). Mechanism by which hyperglycemia inhibits hepatic glucose production in conscious rats: Implications for the pathophysiology of fasting hyperglycemia in diabetes. Journal of Clinical Investigation, 92(3), 1126–1134. https://doi.org/10.1172/JCI116681
Mendeley helps you to discover research relevant for your work.