Abstract

This application proposes a continuation of my neurobehavioral analysis of pancreatic glucagon's role in the control of postprandial satiety in the rat. The planned experiments are designed, first, to characterize further the behavioral and physiological contexts in which exogenous glucagon controls meal size and elicits postprandial satiety; second, to elucidate the peripheral and central neural mechanisms mediating these effects. The central goal of this project is to advance understanding of the physiological controls of feeding behavior. This is a major problem in behavioral neuroscience, and its solution is a prerequisite for the development of physiologically-based treatments of clinical disorders such as obesity, bulimia, and anorexia nervosa. The investigation of the satiety effect of exogenous pancreatic glucagon is especially relevant in this context because there is evidence that endogenous pancreatic glucagon is necessary for the normal control of meal size in the rat. The proposal has seven purposes: First, to determine the site of action and afferent path to the brain for the satiety effect of exogenous pancreatic glucagon. Second, to determine the sites of the terminals fields in the medulla of the hepatic vagal afferents mediating glucagon's satiety effect. Third, to test whether exogenous glucagon's effects on gastric distention or on rate of gastric emptying mediate glucagon's satiety effect. Fourth, to determine the behavioral characteristics and specificity of the inhibitory effect on feeding of exogenous epinephrine in order to evaluate the hypothesis that epinephrine and glucagon have functionallly identical satiety effects. Fifth, to test the hypothesis that the same peripheral innervation mediates the feeding effects of glucagon and epinephrine. Sixth, to test the hypothesis that hepatic glycogenolysis mediates glucagon's satiety effect by comparing glucagon's potencies to elicit satiety and to elicit glycogenolysis at different times of day. Seventh, to investigate the effect of the intensity of sweet taste on glucagon's satiety effect.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK032448-05
Application #
3230840
Study Section
Biopsychology Study Section (BPO)
Project Start
1982-09-01
Project End
1987-06-30
Budget Start
1986-07-01
Budget End
1987-06-30
Support Year
5
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
Columbia University (N.Y.)
Department
Type
Graduate Schools
DUNS #
064931884
City
New York
State
NY
Country
United States
Zip Code
10027

  Publications

Geary, N; Asarian, L (2001) Estradiol increases glucagon's satiating potency in ovariectomized rats. Am J Physiol Regul Integr Comp Physiol 281:R1290-4
Geary, N (1999) Effects of glucagon, insulin, amylin and CGRP on feeding. Neuropeptides 33:400-5
Geary, N (1996) Failure of pulsatile infusion to increase glucagon's satiating potency. Physiol Behav 59:613-6
Surina-Baumgartner, D M; Langhans, W; Geary, N (1995) Hepatic portal insulin antibody infusion increases, but insulin does not alter, spontaneous meal size in rats. Am J Physiol 269:R978-82
Geary, N; Trace, D; Smith, G P (1995) Estradiol interacts with gastric or postgastric food stimuli to decrease sucrose ingestion in ovariectomized rats. Physiol Behav 57:155-8
Geary, N; Trace, D; McEwen, B et al. (1994) Cyclic estradiol replacement increases the satiety effect of CCK-8 in ovariectomized rats. Physiol Behav 56:281-9
Le Sauter, J; Geary, N (1993) [Pancreatic glucagon: physiological signal of postprandial satiety] Ann Endocrinol (Paris) 54:149-61
Geary, N; Le Sauter, J; Noh, U (1993) Glucagon acts in the liver to control spontaneous meal size in rats. Am J Physiol 264:R116-22
Geary, N; Fudge, J; Le Sauter, J (1992) Scheduled running wheel activity indexes the specificity of pharmacological anorexia. Behav Neural Biol 58:1-7
Geary, N; Kissileff, H R; Pi-Sunyer, F X et al. (1992) Individual, but not simultaneous, glucagon and cholecystokinin infusions inhibit feeding in men. Am J Physiol 262:R975-80

Showing the most recent 10 out of 17 publications