Glucagonostatic and Insulinotropic Action of Glucagonlike Peptide I-(7–36)-Amide

Author:

Komatsu Ryoya1,Matsuyama Tatsuo1,Namba Mitsuyoshi1,Watanabe Nobuaki1,Itoh Hidehiko1,Kono Norio1,Tarui Seiichiro1

Affiliation:

1. The Second Department of Internal Medicine, Osaka University Medical School, and the Division of Clinical Laboratory, National Cardiovascular Center Hospital Osaka, Japan

Abstract

We examined the effect of glucagonlike peptides (GLPs), which are cleaved from preproglucagon in the enteroglucagon cells, on rat endocrine pancreas with the isolated perfused system. GLP-I-(7–36)-amide, a truncated form of full-sequence GLP-I-(1–37), showed a potent inhibitory effect on glucagon secretion. This inhibitory effect of GLP-I-(7–36)-amide was demonstrated at concentrations of 0.25, 2.5, and 25 nM in 11.2 and 2.8 mM glucose. In contrast, insulin release was significantly stimulated by GLP-I-(7–36)-amide at its concentration from 0.025 to 25 nM in a high glucose concentration, whereas in a low glucose concentration, the stimulation was seen only at the highest concentration (25 nM). Neither GLP-I-(1–37) nor GLP-II showed any effect on glucagon and insulin release. Although several gastrointestinal hormones have been nominated as incretins, none of them may suppress the glucagon secretion. A truncated form of GLP-I, GLP-I-(7–36)-amide thus seems to be a unique incretin that exerts glucagonostatic action.

Publisher

American Diabetes Association

Subject

Endocrinology, Diabetes and Metabolism,Internal Medicine

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