AJP - Endocrinology and Metabolism, Vol 262, Issue 3 E338-E343, Copyright © 1992 by American Physiological Society
Insulin secretion from ob/ob mouse pancreatic islets: effects of neurotransmitters
T. M. Tassava, T. Okuda and D. R. Romsos
Department of Food Science and Human Nutrition, Michigan State University, East Lansing 48824-1224.
Effects of glucose, acetylcholine, and norepinephrine on insulin secretion
from pancreatic islets of 8- to 9-wk-old female genetically obese (ob/ob)
and lean mice were determined. The ob/ob islets were 60% larger in diameter
than lean mouse islets, secreted fourfold more insulin in response to
glucose, and secreted insulin at lower glucose concentrations than lean
islets. In the presence of 15 mM glucose, ob/ob islets showed an 8-fold
greater absolute increase in insulin secretion in response to acetylcholine
and a 12-fold greater absolute decrease in insulin secretion in response to
norepinephrine inhibition compared with lean islets. In the presence of 5
mM glucose, acetylcholine increased insulin secretion by threefold from
ob/ob islets with no effect on lean islets. When both ob/ob and lean islets
were stimulated by glucose to equivalent levels of insulin secretion,
acetylcholine potentiated glucose-induced insulin secretion equally in
ob/ob and lean islets. Enhanced glucose-induced responsiveness of ob/ob
islets thus can explain the greater acetylcholine potentiation of insulin
secretion and probably the greater norepinephrine inhibition of insulin
secretion in ob/ob islets compared with lean islets. These data are
consistent with the hypotheses that the major alteration in ob/ob mouse
islets is in glucose sensitivity and responsiveness, which subsequently
increases ob/ob islet susceptibility to neural regulation of insulin
secretion.
