CCK SATIETY IS DIFFERENTIALLY MEDIATED BY HIGH-AFFINITY AND LOW-AFFINITY CCK RECEPTORS IN MICE AND RATS

被引:51
|
作者
WEATHERFORD, SC
LAUGHTON, WB
SALABARRIA, J
DANHO, W
TILLEY, JW
NETTERVILLE, LA
SCHWARTZ, GJ
MORAN, TH
机构
[1] JOHNS HOPKINS UNIV, SCH MED,DEPT PSYCHIAT & BEHAV SCI,ROSS 618, 720 RUTLAND AVE, BALTIMORE, MD 21205 USA
[2] HOFFMANN LA ROCHE INC, DEPT MED CHEM 2, NUTLEY, NJ 07110 USA
[3] HOFFMANN LA ROCHE INC, DEPT NEUROBIOL & OBES RES, NUTLEY, NJ 07110 USA
[4] HOFFMANN LA ROCHE INC, DEPT PEPTIDE CHEM, NUTLEY, NJ 07110 USA
来源
AMERICAN JOURNAL OF PHYSIOLOGY | 1993年 / 264卷 / 02期
关键词
CHOLECYSTOKININ; FEEDING; CHOLECYSTOKININ-JMV-180; MK-329; CHOLECYSTOKININ ANTAGONIST; CHOLECYSTOKININ-A RECEPTOR; PANCREAS;
D O I
10.1152/ajpregu.1993.264.2.R244
中图分类号
Q4 [生理学];
学科分类号
071003 ;
摘要
Cholecystokinin-JMV-180 (JMV-180) is an analogue of cholecystokinin C-terminal octapeptide (CCK-8), which has been shown to be an agonist at the proposed CCK pancreatic high-affinity site and a functional antagonist at the pancreatic low-affinity site in rats and to have agonist activity at both high- and low-affinity sites in the mouse. In this study we used JMV-180 to evaluate the potential participation of these two CCK-A sites in the satiety effect of CCK-8 in rats and mice. When tested at doses that ranged from 0.01 to 9.2 mumol/kg, JMV-180 did not reliably affect food intake of solid or liquid test diets in rats. When combined with CCK-8 (3.2 or 8.5 nmol/kg) JMV-180 dose dependently reversed the satiety effect of CCK-8. In contrast to these results in the rat, both JMV-180 (3.7-14.8 mumol/kg) and CCK-8 (1.7-6.8 nmol/kg) dose dependently reduced the intake of 20% sucrose in mice. Both CCK-8- and JMV-180-induced suppression of food intake were attenuated by the CCK-A antagonist MK-329 (24.8 nmol/kg). The results of these studies suggest that agonist activity at sites pharmacologically similar to the CCK pancreatic high-affinity site is not sufficient for expression of CCK satiety, whereas agonist activity at low-affinity-like sites is necessary to reduce food intake. Thus the anorexic activity of CCK appears to be mediated through an interaction with a receptor site pharmacologically similar to the pancreatic low-affinity CCK receptor site.
引用
收藏
页码:R244 / R249
页数:6
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