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Research Article Free access | 10.1172/JCI110588

Effect of Diabetes Mellitus on the Regulation of Enzyme Secretion by Isolated Rat Pancreatic Acini

Makoto Otsuki and John A. Williams

Cell Biology Research Laboratory, Harold Brunn Institute, Mount Zion Hospital and Medical Center, San Francisco, California 94120

Department of Medicine, University of California, San Francisco, California 94143

Department of Physiology, University of California, San Francisco, California 94143

Find articles by Otsuki, M. in: JCI | PubMed | Google Scholar

Cell Biology Research Laboratory, Harold Brunn Institute, Mount Zion Hospital and Medical Center, San Francisco, California 94120

Department of Medicine, University of California, San Francisco, California 94143

Department of Physiology, University of California, San Francisco, California 94143

Find articles by Williams, J. in: JCI | PubMed | Google Scholar

Published July 1, 1982 - More info

Published in Volume 70, Issue 1 on July 1, 1982
J Clin Invest. 1982;70(1):148–156. https://doi.org/10.1172/JCI110588.
© 1982 The American Society for Clinical Investigation
Published July 1, 1982 - Version history
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Abstract

The nature and mechanism of the pancreatic exocrine dysfunction in diabetes mellitus were evaluated in vitro using isolated pancreatic acini prepared from streptozotocin-induced diabetic rats. The content of amylase and ribonuclease in diabetic acini was ∼0.5 and 50% of the normal content, respectively. Further, reduced amounts of both enzymes were secreted by diabetic acini in response to both cholecystokinin (CCK) and carbamylcholine. However, when enzyme secretion was normalized relative to initial acinar contents, both normal and diabetic acini released enzymes at a comparable maximal rate. The time course of the release of these enzymes, and newly synthesized protein were similar in both acini. In normal acini, the effect of CCK was maximal at a concentration of 100 pM; higher concentrations led to submaximal enzyme release. The dose-response curve in diabetic acini was similarly shaped, but shifted three-fold towards higher concentration. The mobilization of cellular Ca2+ in response to CCK was also shifted. In contrast to these results with CCK, the dose-response curve to carbamylcholine was unaltered by diabetes. The observed effects were confirmed to be due to insulin deficiency and not due to direct toxic effect of streptozotocin on acinar cells or malnutrition. Streptozotocin had no acute effect on acini when measured 24 h after administration, and alloxan, another beta cell toxin, induced similar changes in acinar enzyme content and secretory response. Moreover, the administration of exogenous insulin to diabetic rats returned the content of pancreatic amylase and the secretory response to CCK towards normal. Starvation for 48 h, although inducing a significant weight loss, did not mimic the effects of diabetes. The present studies demonstrate two major abnormalities in pancreatic exocrine secretion in the diabetic rat: (a) the content of certain digestive enzymes is markedly altered, leading to an altered amount of zymogen secretion, (b) the sensitivity to CCK is selectively reduced, most likely related to a defect in receptor activated transmembrane signaling.

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