Your search keyword '"Grodsky, G M"' showing total 23 results

1. Effect of glucagon or somatostatin on desensitized insulin secretion.

Author

Bolaffi JL, Rodd G, Ma YH, and Grodsky GM

Subjects

Animals, B-Lymphocytes drug effects, Colforsin pharmacology, Glucagon metabolism, In Vitro Techniques, Insulin Secretion, Male, Rats, Rats, Inbred Strains, Somatostatin metabolism, Time Factors, Glucagon pharmacology, Insulin metabolism, Somatostatin pharmacology

Abstract

In this study we have examined the role of glucagon and somatostatin in regulating glucose-induced desensitization of insulin secretion from rat islets. Measured in batch incubations with medium routinely used to induce three phases of insulin secretion, secreted glucagon levels fell off over 24 h to 20% of peak secretion levels. Although more responsive to various secretagogues, somatostatin secretion also declined to the same degree. Thus, the A- and D-cells desensitize to chronic stimulation as does the B cell. In other experiments, added glucagon (10(-6) M) enhanced glucose (11 X 10(-3) M)-stimulated insulin secretion 34% in the first 3 h; however, islets became insensitive to continuous glucagon by 4 h. The exogenous glucagon did not prevent or delay glucose-induced desensitization of insulin secretion. When glucagon was administered as acute 1-h tests over continuous glucose administration, the degree of B-cell response did not differ in the 1st, 3rd, or 6th hours and appeared to increase in the 21st hour. When islets were perifused continuously with glucose (22 X 10(-3) M) plus 3 X 10(-7) M somatostatin, glucose-induced insulin secretion was suppressed 50% in the first 3 h, but this inhibitory effect disappeared after 6 h. Desensitization was slightly delayed, but not prevented. When somatostatin was administered as acute 1-h tests over continuous glucose perifusion, the B-cell response was relatively constant in the 3rd, 6th, and 21st hours. Results show that 1) islet release of glucagon and somatostatin desensitizes during constant stimulation; and 2) islet release of insulin desensitizes to chronic potentiation or inhibition, respectively, by these hormones. Furthermore, 3) changing B-cell sensitivity to either glucagon or somatostatin cannot account for observed desensitization of insulin secretion with chronic glucose exposure.

Published

1990

2. Calcium dependency of glucagon secretion from the in vitro perfused rat pancreas.

Author

Gerich JE, Frankel BJ, Fanska R, West L, Forsham PH, and Grodsky GM

Subjects

Animals, Arginine pharmacology, Drug Synergism, Glucose pharmacology, In Vitro Techniques, Insulin metabolism, Insulin Secretion, Male, Pancreas drug effects, Rats, Calcium pharmacology, Glucagon metabolism, Pancreas metabolism

Published

1974

3. Insulin within islets is a physiologic glucagon release inhibitor.

Author

Maruyama H, Hisatomi A, Orci L, Grodsky GM, and Unger RH

Subjects

Animals, Guinea Pigs, Insulin Antibodies, Islets of Langerhans metabolism, Male, Perfusion, Rats, Time Factors, Glucagon metabolism, Insulin physiology, Islets of Langerhans physiology

Abstract

To determine if glucagon secretion is under physiological control of intra-islet insulin, pancreata from normal rats were perfused at a 100 mg/dl glucose concentration with either guinea pig antiinsulin serum or normal guinea pig serum in a nonrecirculating system. Perfusion of antiserum was followed within 3 min by a significant rise in glucagon that reached peak levels three times the base-line values and assumed a hectic pattern that returned rapidly to base-line levels upon termination of the antiserum perfusion. Nonimmune guinea pig serum had no effect. To gain insight into the probable site of insulin neutralization, 125I-labeled human gamma-globulin was added to antiserum or nonimmune serum and perfused for 3 min. More than 83% of the radioactivity was recovered in the effluent within 3 min after termination of the infusion, and only 0.05 +/- 0.015% of the radioactivity injected was present in the pancreas 10 min after the perfusion. The maximal amount of insulin that could be completely bound to insulin antibody at a dilution and under conditions simulating those of the perfusion experiments was 20 mU/min. It is concluded that insulin maintains an ongoing restraint upon alpha cell secretion and in its absence causes hectic hypersecretion of glucagon. This restraint probably occurs largely in the intravascular compartment. Loss of this release-inhibiting action of insulin may account for initiation of hyperglucagonemia in insulin-deficient states.

Published

1984

4. Inhibition by somatostatin of glucagon and insulin release from the perfused rat pancreas in response to arginine, isoproterenol and theophylline: evidence for a preferential effect on glucagon secretion.

Author

Gerich JE, Lovinger R, and Grodsky GM

Subjects

Animals, Dose-Response Relationship, Drug, Insulin Secretion, Male, Perfusion, Rats, Arginine antagonists & inhibitors, Glucagon metabolism, Insulin metabolism, Isoproterenol antagonists & inhibitors, Pancreas metabolism, Peptides pharmacology, Theophylline antagonists & inhibitors

Abstract

To determine whether somatostatin inhibits glucagon secretion directly at the pancreatic level and to study quantitatively the relative effects of somatostatin on glucagon and insulin secretion, the effects of various concentrations of somatostatin on glucagon and insulin release from the in vitro perfused rat pancreas in response to arginine (14.2 mM), isoproterenol (2 mg/ml) and theophylline (10 MM) were studied. Glucagon and insulin responses to arginine were progressively inhibited by somatostatin over a concentration range from 0.1-100 ng/ml. At all doses, somatostatin caused greater inhibition of glucagon secretion than of insulin secretion. Approximately 4 ng/ml somatostatin reduced glucagon responses 50%, whereas 90 ng/ml was required to produce comparable inhibition of insulin responses. Glucagon responses to isoproterenol, an activator of adenylate cyclase, and to theophylline, a phosphodiesterase inhibitor, were completely abolished by 100 ng/ml somatostatin. Isoproterenol did cause insulin release in this system, but insulin responses to theophylline were diminished by somatostatin. The present studies thus indicate that somatostatin is a potent inhibitor of both glucagon and insulin secretion and indicate that it acts directly on the pancreatic alpha and beta cells. Glucagon secretion is approximately 20 times more sensitive to the inhibitory effects of somatostatin than is insulin secretion. Furthermore, the present results suggest that somatostatin may act by modifying cAMP-dependent systems rather than by altering cAMP levels.

Published

1975

5. Characterization of the effects of arginine and glucose on glucagon and insulin release from the perfused rat pancreas.

Author

Gerich JE, Charles MA, and Grodsky GM

Subjects

Arginine administration & dosage, Dose-Response Relationship, Drug, Drug Interactions, Glucose administration & dosage, Glucose antagonists & inhibitors, Insulin Secretion, Pancreas cytology, Pancreas drug effects, Secretory Rate drug effects, Stimulation, Chemical, Arginine pharmacology, Glucagon metabolism, Glucose pharmacology, Insulin metabolism, Pancreas metabolism

Abstract

To characterize the mechanisms by which arginine and glucose affect pancreatic alpha and beta cell function, the effects of these agents over their full dose response, both alone and in various combinations, were studied using the perfused rat pancreas. Arginine (0-38 mM), in the absence of glucose, stimulated biphasic glucagon (IRG) secretion (Km approximately 3-4 mM) at concentrations less than 1 mM and caused nonphasic insulin (IRI) release (Km approximately 12-13 mM) but only at concentrations greater than 6 mM. Glucose (0-27.5 mM) alone stimulated biphasic IRI release (Km approximately 9-10 mM) at concentrations in excess of 5.5 mM and caused nonphasic inhibition of IRG secretion (Kt approximately 5-6 mM) at concentrations as low as 4.1 mM. These results demonstrate fundamental differences in pancreatic alpha and beta cell secretory patterns in response to glucose and arginine and suggest that glucagon secretion is more sensitive to the effect of both glucose and arginine. Various concentrations of arginine in the presence of 5.5 mM glucose stimulated biphasic IRG and IRI release: IRG responses were diminished and IRI responses were enhanced compared with those seen with arginine in the absence of glucose. Glucose (0-27.5 mM) in the presence of 3.2 or 19.2 mM arginine caused similar inhibition of IRG secretion (Km approximately 5-6 mM) and stimulation of IRI release (Km approximately 9-10 mM) as that seen with glucose alone, although greater IRG and IRI release occurred. This augmentation of IRI secretion was greater than that expected from mere additive effects of glucose and arginine. Classical Lineweaver-Burk analysis of these results indicates that glucose is a non-competitive inhibitor arginine-stimulated glucagon secretion and suggests that glucose and arginine affect pancreatic alpha and beta cell function via different mechanisms. In addition, comparison of simultaneous insulin and glucagon secretion patterns under various conditions suggests that endogenous insulin per se has little or no direct effect on IRG secretion and that endogenous glucagon does not appreciably affect pancreatic beta cell function.

Published

1974

6. Regulation of pancreatic insulin and glucagon secretion.

Author

Gerich JE, Charles MA, and Grodsky GM

Subjects

Adenosine Triphosphate metabolism, Amino Acids pharmacology, Animals, Calcium metabolism, Catecholamines pharmacology, Diabetes Mellitus metabolism, Diet, Fatty Acids, Nonesterified pharmacology, Glucose pharmacology, Hormones pharmacology, Humans, Hypothalamus physiology, Insulin Secretion, Ketone Bodies pharmacology, Kinetics, Microtubules physiology, Models, Biological, Nucleotides, Cyclic metabolism, Pancreas innervation, Pancreas ultrastructure, Parasympathetic Nervous System physiology, Receptors, Drug, Sympathetic Nervous System physiology, Glucagon metabolism, Insulin metabolism, Pancreas metabolism

Published

1976

7. Direct calcium-stimulated release of glucagon from the isolation perfused rat pancreas and the effect of chemical sympathectomy.

Author

Lundquist I, Fanska R, and Grodsky GM

Subjects

Animals, Arginine pharmacology, Neurons drug effects, Pancreas drug effects, Pancreas innervation, Perfusion, Rats, Serotonin pharmacology, Stimulation, Chemical, Calcium pharmacology, Glucagon metabolism, Pancreas metabolism, Sympathetic Nervous System drug effects

Abstract

"Staircase" increments of calcium (from 0.5 to 15 mEq/L) were added to the perfused rat pancreas in the absence of glucagon secretogogues. Large spikes of glucagon release resulted, particularly at the small and large calcium concentrations. Insulin secretion was undetectable. Selective destruction of peripheral adrenergic neurons by pretreatment of the rats with 6-hydroxydopamine reduced the basal glucagon secretion to about 50% and specifically suppressed the calcium-induced glucagon release at the lower calcium steps. The response to a subsequent stimulation by arginine/calcium was not inhibited. Results suggest that glucagon secretion is modulated by a stimulant effect of the pancreatic adrenergic nerves (norepinephrine?) and that calcium in part positively affects release by permitting this neural stimulation.

Published

1976

8. Interaction of calcium and glucose on glucagon secretion.

Author

Lundquist I, Fanska R, and Grodsky GM

Subjects

Animals, Dose-Response Relationship, Drug, Drug Interactions, Egtazic Acid pharmacology, Insulin metabolism, Insulin Secretion, Kinetics, Male, Pancreas drug effects, Rats, Calcium pharmacology, Glucagon metabolism, Glucose pharmacology, Pancreas metabolism

Abstract

The interrelationship between calcium ion and glucose on glucagon release was studied in the in vitro perfused pancreas. Spontaneous release during perfusion with glucose-free, calcium-depleted (0.2 mEq/l calcium) medium was completely abolished by ethylene glycol bis (beta-aminoethyl ether)-N,N'-tetraacetic acid (EGTA; 0.2 mM). Glucose added to calcium-depleted perfusate caused only partial inhibition of glucagon release, even at concentrations of 500 mg/dl, and there was no evidence of a paradoxical increase in secretion with time. When calcium was added in a series of steps (in the absence of additional secretagogues) more than half of the increased glucagon released was elicited by the first step (0.5 mEq/l). Release patterns at subsequent steps suggested that higher concentrations of calcium may cause mixed stimulation and inhibition. With 70 mg/dl glucose, calcium-stimulated release was partially suppressed at all calcium concentrations up through 9 mEq/l. With 150 mg/dl glucose, addition of the normally stimulating 0.5 mEq/l calcium caused abrupt and complete inhibition of glucagon secretion, and this persisted at all higher calcium concentrations. Insulin release, when high enough to be detected, did not correlate with the glucose/calcium suppression of glucagon. In other experiments, control results and all insulin secretion patterns were qualitatively similar to those reported by other investigators; however, various attempts to demonstrate a paradoxical increase glucagon secretion by glucose during calcium deprivation were unsuccessful. It is concluded that small amounts of calcium are normally required for glucagon secretion, although at higher concentrations the effects become complex. In addition, glucagon suppression by glucose is calcium-requiring. Thus, changes in glucagon secretion caused by addition or depletion of calcium can depend on the relative amount of glucose in the milieu.

Published

1976

9. Abnormal secretion of insulin and glucagon by the in vitro perfused pancreas of the genetically diabetic Chinese hamster.

Author

Frankel BJ, Gerich JE, Hagura R, Fanska RE, Gerritsen GC, and Grodsky GM

Subjects

Animals, Blood Glucose analysis, Cattle, Cricetinae, Diabetes Mellitus genetics, Diabetes Mellitus veterinary, Drug Combinations, Female, Glucose metabolism, Hyperglycemia metabolism, In Vitro Techniques, Insulin analysis, Insulin Secretion, Male, Pancreas analysis, Pancreas pathology, Pancreas physiopathology, Perfusion, Rats, Swine, Theophylline metabolism, Diabetes Mellitus physiopathology, Disease Models, Animal, Glucagon metabolism, Insulin metabolism, Pancreas metabolism

Abstract

Hereditary insulin-deficient diabetes mellitus occurs in certain sublines of nonobese Chinese hamsters. Several characteristics of this syndrome are similar to those seen in insulin-deficient human diabetics. Therefore, to characterize pancreatic islet function, dynamic insulin and glucagon release from normal and nonketotic diabetic hamster pancreases in response to glucose (300 mg/100 ml) and theophylline (10 mM), infused singly and together, was studied in vitro.20-min glucose infusions of normal hamster pancreases caused biphasic insulin release, consisting of a rapid first peak and a gradually rising second phase, similar to that reported for man in vivo. Both phases were significantly reduced in the diabetic pancreases. Theophylline alone stimulated similar nonphasic insulin release in both the normal and the diabetic pancreases. Glucose and theophylline together caused greater insulin release than either stimulant alone in both normals and diabetics; however, the diabetic response was still subnormal. Glucose suppressed glucagon release from normal pancreases; suppression was significantly impaired in diabetics. Theophylline stimulated nonphasic glucagon release in both the normals and diabetics. Glucose partially suppressed the theophylline-stimulated release in both groups.Insulin/glucagon molar ratios of the diabetics were consistently subnormal, although individual hormone levels often overlapped into the normal range. IN SUMMARY, THE PANCREASES OF GENETICALLY DIABETIC CHINESE HAMSTERS PERFUSED IN VITRO SHOWED: (a) decreased first and second phase insulin release in response to glucose-containing stimuli-only partially ameliorated by theophylline-, and (b) impaired suppression of glucagon in response to glucose, resulting in (c) a decreased insulin/glucagon molar ratio. These data support the suggestion that both alpha and beta cells of diabetic pancreases may be insensitive to glucose.

Published

1974

10. Insulin and glucagon release in the diabetic Chinese hamster: differences among inbred sublines.

Author

Frankel BJ, Heldt AM, and Grodsky GM

Subjects

Animals, Arginine, Blood Glucose analysis, Female, Glucose, Male, Perfusion, Sex Factors, Species Specificity, Cricetinae metabolism, Cricetulus metabolism, Diabetes Mellitus, Experimental metabolism, Glucagon metabolism, Insulin metabolism, Pancreas metabolism

Abstract

Release of insulin and glucagon from perfused pancreases in vitro of 40 normal male and female Chinese hamsters (from one inbred subline) and 110 male and female diabetic hamsters (from three inbred sublines) was measured in response to glucose plus arginine, theophylline alone, or potassium alone, in order to determine if differences in hormone secretion exist among different diabetic sublines. Glucose plus arginine and potassium produced subnormal insulin responses in all three diabetic sublines, whereas theophylline induced 'normal' or above normal insulin responses. Excessive glucagon release was consistently seen in only one diabetic subline. The female normal animals showed greater insulin release than the male normal hamsters in response to glucose plus arginine. This sex difference was not seen in the diabetic animals.

Published

1982

11. Stimulatory effects of tolbutamide infusion on plasma glucagon in insulin-dependent diabetic subjects.

Author

Bohannon NV, Lorenzi M, Grodsky GM, and Karam JH

Subjects

Adult, Blood Glucose metabolism, C-Peptide blood, Female, Humans, Kinetics, Male, Middle Aged, Diabetes Mellitus blood, Glucagon blood, Tolbutamide pharmacology

Abstract

The effect of iv tolbutamide on endogenous glucagon levels was measured in nine insulin-dependent diabetic patients chosen because they evidenced no C-peptide response to beta-cell secretagogues. Basal glucagon levels were not suppressed by a sustained tolbutamide infusion; in fact, a slight stimulatory effect was observed at 5, 10, 30, and 45 min. In the absence of detectable insulin secretory capacity and suboptimal insulin replacement, tolbutamide appears to be a stimulus, not a suppressant, of glucagon secretion.

Published

1982

12. Islet transplantation into rat liver: in vitro secretion of insulin from the isolated perfused liver and in vivo glucagon suppression.

Author

Charles MA, Imagawa W, Forsham PH, and Grodsky GM

Subjects

Animals, Blood Glucose metabolism, Diabetes Mellitus chemically induced, Diabetes Mellitus therapy, Insulin Secretion, Islets of Langerhans metabolism, Male, Perfusion, Portal Vein surgery, Rats, Rats, Inbred Lew, Streptozocin, Transplantation, Isogeneic, Glucagon metabolism, Insulin metabolism, Islets of Langerhans Transplantation, Liver metabolism

Abstract

Islet isografts were injected into the portal veins of rats made diabetic with streptozotocin. The isografts normalized not only plasma glucose and insulin levels but also the elevated plasma immunoreactive glucagon level. The in vitro basal insulin secretion and prompt sensitivity to glucose were shown directly by perfusing isolated livers containing transplanted islets. In vitro glucagon secretion to an arginine stimulus could not be demonstrated, although it would have been expected demonstrated, although it would have been expected in normal islets. Thus, it appears that insulin derived from transplanted islets is capable of correcting endogenous hyperglucagonemia and of ameliorating the effects of experimental diabetes while transplanted islet glucagon secretion is relatively suppressed.

Published

1976

13. Effects of K+ and arginine on insulin, glucagon, and somatostatin release from the in vitro perfused rat pancreas.

Author

Frankel BJ, Heldt AM, and Grodsky GM

Subjects

Animals, In Vitro Techniques, Insulin Secretion, Pancreas drug effects, Perfusion, Rats, Arginine pharmacology, Glucagon metabolism, Insulin metabolism, Pancreas metabolism, Potassium pharmacology, Somatostatin metabolism

Abstract

Rat pancreases were perfused in vitro for 5-min periods with K+ alone (8, 10, and 12 mM) or in the presence of arginine (10 mM). Alone, K+ caused bursts of insulin, glucagon, and somatostatin (SRIF) release; with arginine, it caused a burst of insulin and sustained SRIF release, but caused sustained suppression of glucagon. This suppression correlated better with SRIF than insulin release. Therefore, if a paracrine effect is responsible for the inhibition of glucagon secretion under these circumstances, SRIF is a more likely candidate than insulin.

Published

1982

14. Insulin, glucagon, and somatostatin release from the prediabetic Chinese hamster.

Author

Frankel BJ, Heldt AM, Gerritsen GC, and Grodsky GM

Subjects

Aging, Animals, Arginine pharmacology, Cricetinae, Cricetulus, Glucose pharmacology, Insulin Secretion, Islets of Langerhans drug effects, Islets of Langerhans growth & development, Kinetics, Male, Mutation, Diabetes Mellitus, Experimental physiopathology, Glucagon metabolism, Insulin metabolism, Islets of Langerhans metabolism, Prediabetic State physiopathology, Somatostatin metabolism

Abstract

Diabetes mellitus in the adult Chinese hamster is characterized by subnormal pancreatic insulin release in vitro, decreased insulin content, and lack of obesity. The cause of the islet B-cell failure is not clear. We measured insulin, glucagon, and somatostatin release from in vitro perfused pancreases of young (mean age 10 and 20 weeks), genetically diabetic animals (subline AC, mean plasma glucose 8.0 and 16.6 mmol/l, respectively). Compared to age- and sex-matched normal hamsters (subline M, mean plasma glucose 5.3 mmol/l), the younger diabetic animals had a significantly elevated mean plasma glucose level, but net in vitro pancreatic release of insulin, glucagon, and somatostatin was normal. Pancreatic content of insulin and glucagon was also not significantly different from normal. At age 20 weeks, when the plasma glucose of the diabetic animals was even more elevated, pancreatic content and release of insulin were significantly subnormal, whereas glucagon and somatostatin release were normal, and pancreatic content of glucagon was normal. In a similar group of young (mean age 10 weeks) diabetic animals, non-fasting plasma insulin levels were within the normal range, but the corresponding glucose levels were excessive in most of the animals (13 out of 19). In conclusion, 10-week-old diabetic hamsters show mild hyperglycaemia which cannot be accounted for directly by decreased pancreatic release in response to a glucose plus arginine stimulus in vitro. Decreased ability of the B cell to respond in vivo to hyperglycaemia or peripheral resistance to insulin may contribute to later B-cell failure in the older diabetic hamster.

Published

1984

15. Interrelationships between alpha and beta-anomers of glucose affecting both insulin and glucagon secretion in the perfused rat pancreas. II.

Author

Grodsky GM, Fanska R, and Lundquist I

Subjects

Animals, Insulin Secretion, Perfusion, Rats, Glucagon metabolism, Glucose pharmacology, Insulin metabolism, Pancreas drug effects

Abstract

Temporal and quantitative relationships between the alpha and beta anomers of glucose on insulin and glucagon secretion were studied in two surgical preparations of the in vitro perfused rat pancreas. Alpha-Glucose was a more effective stimulator of insulin release. Beta-Glucose, however, though less effective, was a positive modulator when admixed with alpha-glucose. Dose-response studies showed that alpha-glucose probably had a smaller apparent Km for insulin secretion, while the Vmax for the two anomers was the same-the effects of the two anomers being indistinguishable at high glucose concentrations (300 mg/dl). Alpha-Anomeric stereospecificity was demonstrable equally on both phases of insulin release and was maintained throughout 60-min perfusions. Spontaneous or arginine-stimulated glucagon release was also preferentially inhibited by alpha-glucose. Since others have shown that glucose uptake and phosphorylation in islets are not alpha-stereospecific, the data suggest that the initial signal for the first and second phases of insuulin release and glucose suppression of glucagon secretion is at the level of a glucoreceptor prior to, or indedendent of, major pathways of glucose metabolism.

Published

1975

16. The diabetic Chinese hamster: in vitro insulin and glucagon release; the ""chemical diabetic";; and the effect of diet on ketonuria.

Author

Grodsky GM, Frankel BJ, Gerich KE, and Gerritsen GC

Subjects

Animals, Arginine pharmacology, Diabetes Mellitus genetics, Diabetic Ketoacidosis metabolism, Disease Models, Animal, Female, Glucose pharmacology, Glucose Tolerance Test, Glycosuria metabolism, Immunoassay, Insulin Secretion, Male, Pancreas drug effects, Theophylline pharmacology, Cricetinae, Diabetes Mellitus metabolism, Glucagon metabolism, Insulin metabolism, Pancreas metabolism

Published

1974

17. The effect of potassium and valinomycin on insulin and glucagon secretion in the perfused rat pancreas.

Author

Epstein G, Fanska R, and Grodsky GM

Subjects

Animals, Arginine pharmacology, Diabetes Mellitus, Experimental physiopathology, Ethanol pharmacology, Insulin Secretion, Kinetics, Pancreas drug effects, Perfusion, Rats, Glucagon metabolism, Insulin metabolism, Pancreas metabolism, Potassium pharmacology, Valinomycin pharmacology

Published

1978

18. Production of glucagon antibodies and their role in metabolism and immunoassay of glucagon.

Author

GRODSKY GM, HAYASHIDA T, PENG CT, and GESCHWIND II

Subjects

Humans, Antibodies, Glucagon, Immunoassay

Published

1961

19. Effect of selected hexoses, of epinephrine and of glucagon on insulin secretion in man.

Author

Karam JH, Grasso SG, Wegienka LC, Grodsky GM, and Forsham PH

Subjects

Humans, Epinephrine pharmacology, Glucagon pharmacology, Hexoses pharmacology, Insulin metabolism

Published

1966

20. Stimulation of insulin release by glucagon in noninsulin-dependent diabetics.

Author

Simpson RG, Benedetti A, Grodsky GM, Karam JH, and Forsham PH

Subjects

Blood Glucose, Diabetes Mellitus blood, Drug Synergism, Humans, Diabetes Mellitus physiopathology, Glucagon pharmacology, Glucose pharmacology, Insulin blood, Insulin metabolism, Islets of Langerhans physiopathology

Published

1966

21. Exaggerated insulin response to glucagon in simple obesity.

Author

Benedetti A, Simpson RG, Grodsky GM, and Forsham PH

Subjects

Adult, Female, Glucose Tolerance Test, Humans, Male, Middle Aged, Glucagon pharmacology, Insulin metabolism, Obesity metabolism

Published

1967

22. Effect of pulse administration of glucose or glucagon on insulin secretion in vitro.

Author

Grodsky GM, Bennett LL, Smith DF, and Schmid FG

Subjects

Adenine Nucleotides metabolism, Animals, Caseins pharmacology, Endopeptidases metabolism, In Vitro Techniques, Iodine Isotopes, Male, Pancreas physiology, Rats, Secretory Rate, Theophylline pharmacology, Glucagon pharmacology, Glucose pharmacology, Insulin physiology

Published

1967

23. In vitro inhibition of pancreatic glucagon secretion by diphenylhydantoin.

Author

Gerich JE, Charles MA, Levin SR, Forsham PH, and Grodsky GM

Subjects

Animals, Arginine pharmacology, Depression, Chemical, Diabetes Mellitus drug therapy, In Vitro Techniques, Insulin metabolism, Insulin Secretion, Male, Pancreas metabolism, Perfusion, Phenytoin therapeutic use, Radioimmunoassay, Rats, Glucagon metabolism, Pancreas drug effects, Phenytoin pharmacology

Published

1972