Synthetic Gastric Inhibitory Polypeptide Stimulatory Effect on Insulin and Glucagon Secretion in the Rat

Author:

Taminato Tomohiko1,Seino Yutaka1,Goto Yasuo1,Inoue Yoshimichi1,Kadowaki Seizo1,Mori Kozaburo1,Nozawa Masumi1,Yajima Haruaki1,Imura Hiroo1

Affiliation:

1. Division, Department of Medicine, Kobe University School of Medicine, the Department of Surgery, Osaka Medical School, and the Faculty of Pharmaceutical Sciences, Kyoto University Kobe, Japan

Abstract

Effect of synthetic gastric inhibitory polypeptide (GIP) on insulin and glucagon secretion was studied in vivo and in vitro in the rat. Intravenous administration of 1 μg./kg. GIP along with 0.625 gm./kg. glucose caused a more prominent rise of plasma insulin than did 0.625 gm./kg. glucose alone. The suppression of plasma glucagon levels induced by glucose was attenuated partially but not significantly by the concomitant administration of GIP. GIP (1 μg./kg. i.v.) alone raised both plasma insulin and glucagon levels. In in-vi tro experiments with isolated pancreatic islets, GIP significantly augmented insulin release induced by either 8.3 mM or 16.7 mM glucose, whereas the augmentation of glucagon release was observed at 3.3 mM, 8.3 mM, and 16.7 mM glucose concentrations. Three peptides, consisting of 1–28, 22–43, and 15–43 ammo acids of GIP, failed to potentiate insulin and glucagon secretion. These results suggest that synthetic GIP has a stimulating effect on insulin and glucagon secretion.

Publisher

American Diabetes Association

Subject

Endocrinology, Diabetes and Metabolism,Internal Medicine

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