The effect of fasting, diet, and actinomycin D on insulin secretion in the rat.
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The results suggest that the impairment of glucose-stimulated insulin secretion during fasting and its restoration by refeeding are regulated by changes in a glucose-inducible enzyme system in the pancreatic beta cell.Abstract:
A BST R A C T The present studies were performed to elucidate the mechanisms responsible for the impairment of glucose-stimulated insulin secretion observed in fasting. Rats fasted for 48 hr displayed marked impairment in their insulin secretory response to both oral and intravenous glucose. Glucose-stimulated insulin secretion was restored within 24 hr by refeeding; actinomycin D given before refeeding blocked the expected return of normal glucose-stimulated insulin secretion despite adequate food intake. Fasted rats refed a diet devoid of carbohydrate failed to display a return of normal insulin secretory responsiveness to oral glucose in contrast to rats fed isocalorically a high carbohydrate diet. Differences in insulin secretion in fed, fasted, and fasted-refed rats could not be attributed to changes in pancreatic insulin content. There was no significant difference in the insulin secretory response to aminophylline of fed, fasted, or fasted-refed rats. The intermittent pulsing of fasted rats with hyperglycemic episodes by the injection of small amounts of glucose (500 mg) intraperitoneally every 8 hr ameliorated the impairment of glucose-stimulated insulin secretion characteristic of the fasting state. These results suggest that the impairment of glucose-stimulated insulin secretion during fasting and its restoration by refeeding are regulated by changes in a glucose-inducible enzyme system in the pancreatic beta cell.read more
Citations
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Preservation of glucose tolerance and insulin secretory response to repeated glucose loads by the feeding of minimal glucose during prolonged fasting
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Investigations on isolated islets in vitro. IX. Influence of food deprivation and glucose refeeding in vitro on insulin secretion
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TL;DR: Although the content of insulin as well as glucagon in the islets was reduced by food deprivation it is assumed that the islet hormone content is not responsible for the rise of the glucose threshold caused by starvation.
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Hepatic regulation of pancreatic α-cell function
TL;DR: A new hypothesis is proposed that the liver secretes a hormonal factor in response to its glycogen replenishment, a substance that inhibits pancreatic α cells, since the kidney, not the liver, is the main site of glucagon degradation and clearance.
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Effect of fasting on alanine-stimulated insulin and glucagon secretion
TL;DR: The hypothesis that the physiologic response to this amino acid with fasting may be partially responsible for the regulation of insulin secretion in this state is supported.
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Effect of starvation on pituitary and serum follicle-stimulating hormone and luteinizing hormone following ovariectomy in the rat.
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