Effects of 4-methyl-2-methylenevalerate,a non-metabolizable analogue of 2-ketoisocaproate,on insulin secretion and metabolism inob/ob mouse pancreatic islets

Summary To determine the importance of 2-ketoisocaproate metabolism in its insulin secretory action, 4-methyl-2-methylenevalerate, a non-metabolizable analogue, was tested for its ability to promote insulin secretion, and to interfere with the metabolism and insulin secretory action of 2-ketoisocaproate. 4-Methyl-2-methylenevalerate did not induce insulin release by isolatedob/ob mouse pancreatic islets, but it inhibited insulin release in response to 2-ketoisocaproate and reduced the rate of decarboxylation and oxidation of labeled 2-ketoisocaproate. The results suggest that 4-methyl-2-methylenevalerate interferes with the insulin secretory action of 2-ketoisocaproate, owing to their common brached-chain chemical structure.The skilful technical assistance of Miss S. Detels is gratefully acknowledged.     

Effects of pregnancy on the glucose-induced insulin release from cultivated pancreatic islets of the rat

Summary 7-day-cultured islets from pregnant Wistar rats released at 5.6 mM glucose significantly more insulin than islets from nonpregnant rats, whereas in vivo this heigthened glucose sensitivity is lost 48 h post partum.Investigations carried out as a part of the Forschungsprojekt Diabetes mellitus und Fettstoffwechselstörungen supported by the Ministry of Health of German Democratic Republic.     

Effects of pregnancy on the glucose-induced insulin release from cultivated pancreatic islets of the rat.

7-day-cultured islets from pregnant Wistar rats released at 5.6 mM glucose significantly more insulin than islets from nonpregnant rats, whereas in vivo this heigthened glucose sensitivity is lost 48 h post partum.     

Lack of influence of vitamin D deficiency on insulin release from the isolated pancreatic islets of rats

Pancreatic islets were isolated from young (100 g) and adult (390 g), normal and vitamin D deficient male Sprague-Dawley rats. The release of insulin from leucine-stimulated or glucose-stimulated islet was not altered by vitamin D deficiency. The in vitro addition of either 25-hydroxy- or 1,25-dihydroxyvitamin-D had no effect on insulin release from either normal or vitamin D deficient islets. We conclude that the earlier report (Normal et al., Science 209 (1980) 823-825) on vitamin D deficiency depressing insulin secretion from the perfused pancreas must be related to the vitamin's effect on insulin synthesis and not the islet's release of insulin.     

Kinetics of insulin secretion in response to glucose by isolated islands of Langerhans from the fetal rat]

Isolated islets of Langerhans from 21.5 day-old foetal Rats were studied in a perifusion system in vitro. The overall dynamics of insulin release by the foetal islets in response to glucose 13.9 mM is biphasic and qualitatively similar to that obtained with islets of adult Rats. The magnitude of the initial phase of insulin secretion is similar for the foetal and adult islets. The second phase is fourfold higher in the adult than in the foetus. The response of foetal islets occurs, 45 to 60 sec. after the increase of glucose concentration in the medium and a maximum insulin release for the first phase is obtained with a lag period of 2 min. The difference between foetal and adult islets is essentially quantitative.     

Insulin secretion and (pro)insulin biosynthesis of cultured mice islets after glibenclamide loading in vitro

Summary Isolated islets from C57B1/6J mice exposed to 10 mmoles/1 glucose supplemented with 5 g/ml glibenclamide for 48 h released significantly less insulin in the subsequent short-time incubation thanuntreated controls (without glibenclamide), whereas insulin biosynthesis was not suppressed by glibenclamide treatment.Investigations were carried out as a part of the ForschungsprojektDiabetes mellitus und Fettstoffwechselstörungen, supported by the Ministry of Health of the GDR.     

Insulin secretion and (pro)insulin biosynthesis of cultured mice islets after glibenclamide loading in vitro

Isolated islets from C57Bl/6J mice exposed to 10 mmoles/l glucose supplemented with 5 micrograms/ml glibenclamide for 48 h released significantly less insulin in the subsequent short-time incubation than untreated controls (without glibenclamide), whereas insulin biosynthesis was not suppressed by glibenclamide treatment.     

The effect of pentagastrin on the A1-cells of the pancreatic islets in guinea-pigs

Zusammenfassung Meerschweinchen wurden für 5 Tage mit Pentagastrin injiziert und die Kerngrössen in den Pankreas-Inseln mit Karyometrie bestimmt. Die Kerne der A₁-Zellen nahmen in den behandelten Tieren am Anfang ab und schienen kleiner als in den Kontrollen. In den A₂-und B-Zellen wurden keine Veränderungen nach Pentagastrin notiert. Die Resultate stützen die Auffassung, dass Gastrin in den A₁-Zellen produziert wird.

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The work was supported by grants from the Swedish Medical Research Council No. B70-2297-03. The pentagastrin (Peptavlon) was kindly supplied by Imperial Chemical Industries (ICI).     

Effect of gentamycin on insulin release and45Ca net uptake by isolated islets

Summary In isolated islets, gentamycin reduced both the⁴⁵Ca net uptake and insulin release induced by glucose, but failed to inhibit the insulin secretion provoked by the combination of Ba²⁺ and theophylline. This indicates that the inhibitory effect of gentamycin is due to a reduction of Ca²⁺ entry into B-cells instead of to a harmful effect upon the integrity of the effector system, responsible for the extrusion of the insulin containing granules.Supported by a Grant (No. 79/1872) from the São Paulo State Research Foundation (FAPESP), Brazil.     

Action of somatostatin and 3 analogs on external pancreatic secretion in the rat]

The effect os somatostatin (SS) and of its analogs D Trp 8-SS and Asn 5-SS was studied upon the external pancreatic secretion of the Rat after stimulation by 2 deoxy-D-glucose. The secretion of sodium and bicarbonate was similarly inhibited by all four peptides. The analog D Trp 8-SS was more effective in inhibiting pancreatic protein excretion.