A Comparative Study of Two Insulin Secretion Inhibitors: Somatostatin and Diazoxide

Sodium salicylate poisoning increased glucose-induced insulin secretion by slices of rat pancreas. The alpha adrenergic blocker phentolamine, but not salicylate poisoning, overcame the inhibitory effect of epinephrine on insulin secretion. Theophylline (5, 10 and 15 mM) significantly increased the insulin secretion induced by 11 mM glucose. The highest insulin response was obtained when theophylline was used at a 10 mM concentration. However, when pancreas slices from salicylate poisoned rats were used, a 5 mM concentration was sufficient to achieve maximal insulin response. Salicylate poisoning diminished the free tubulin pool, an action that was impaired by imidazole; however, imidazole did not modify the effect of the ionophore A23187. The results suggest that: a) sodium salicylate poisoning increases B-cell response to glucose; b) changes in alpha adrenergic activity are not related to the mechanism of action of salicylate; c) an increment in the cAMP concentration may mediate the stimulatory effect of salicylate poisoning on insulin secretion; d) the effect of salicylate on the microtubular system is indirect and probably mediated through an increment in pancreatic cAMP.

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Effect of salicylate poisoning on insulin secretion. Studies on its mechanism of action

Arata

Karabatas

Fernández

et al. 1983

Acta diabet. lat

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Insulin secretion induced by alloantigens. Mechanisms of action

et al. 1989

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Basal insulin secretion stimulated by allogeneic lymphocyte injection was inhibited by SRIF, diazoxide and verapamil but was not affected by theophylline or imidazole. Glucose stimulated insulin secretion induced by alloantigens was inhibited by imidazole. Maximum insulin secretion was achieved with 2.1 mg/ml theophylline in allogeneized mouse pancreata and with 4.2 mg/ml in control pancreata. Propranolol also blocked allogen-induced glucose-stimulated insulin secretion. Phentolamine enhanced insulin secretion from both experimental groups, but phentolamine plus epinephrine only stimulated insulin secretion in control pancreata. Verapamil, diazoxide and SRIF diminished insulin secretion in both experimental groups. These results suggest that: a) basal insulin secretion induced by alloantigens may be mediated by an increase in calcium translocation, and b) glucose-stimulated insulin secretion induced by alloantigen may be mediated by a rise in B-cell cAMP.

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Diabetes prevention in BB rats by inhibition of endogenous insulin secretion

1991

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A Comparative Study of Two Insulin Secretion Inhibitors: Somatostatin and Diazoxide

Cited by 6 publications

References 7 publications

Effect of salicylate poisoning on insulin secretion. Studies on its mechanism of action

Effect of salicylate poisoning on insulin secretion. Studies on its mechanism of action

Insulin secretion induced by alloantigens. Mechanisms of action

Diabetes prevention in BB rats by inhibition of endogenous insulin secretion

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