Endogenous cholecystokinin release responsible for pancreatic growth observed after pancreatic juice diversion

Endogenous cholecystokinin release responsible for pancreatic growth observed after pancreatic juice diversion

This study was undertaken to determine whether intermittent pancreatic juice diversion (PJD) from the intestine can induce pancreatic and duodenal growth. Concomitant infusions of SMS 201-995, a somatostatin analog, and L-364,718, a cholecystokinin (CCK) receptor antagonist, were used to establish t...

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Bibliographic Details
Published in:Endocrinology (Philadelphia) Vol. 129; no. 6; p. 2867
Main Authors: Rivard, N, Guan, D, Maouyo, D, Grondin, G, Bérubé, F L, Morisset, J
Format: Journal Article
Language:English
Published: United States 01-12-1991
Subjects:
Animals
Benzodiazepinones - pharmacology
Bile Ducts - surgery
Cholecystokinin - secretion
Devazepide
Duodenum - drug effects
Duodenum - growth & development
Duodenum - surgery
Male
Octreotide - pharmacology
Pancreas - drug effects
Pancreas - growth & development
Pancreas - secretion
Pancreatic Ducts - surgery
Pancreatic Juice - physiology
Rats
Rats, Inbred Strains
Receptors, Cholecystokinin - antagonists & inhibitors
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Summary:This study was undertaken to determine whether intermittent pancreatic juice diversion (PJD) from the intestine can induce pancreatic and duodenal growth. Concomitant infusions of SMS 201-995, a somatostatin analog, and L-364,718, a cholecystokinin (CCK) receptor antagonist, were used to establish the involvement of endogenous CCK. Fed rats equipped with biliary, duodenal, and pancreatic cannulae had their pancreatic juice diverted 8 h/day for 4 days and were infused or not with either SMS 201-995 (5 micrograms/kg.h) or L-364,718 (0.5 mg/kg.h) during diversion. After 4 days, rats were killed, and their pancreas and duodenum were excised for measurements of parameters indicative of growth. In normally fed rats with pancreatic juice returned, SMS 201-995 inhibited daily pancreatic secretions of volume and protein, whereas L-364,718 inhibited only protein output. These two inhibitors had no effect on normal pancreatic and duodenal growth. PJD was associated with increased volume and protein output, increased plasma CCK level, and pancreatic growth. All of these effects were completely blocked by SMS 201-995 and L-364,718, with the exception of plasma CCK level by the CCK antagonist. None of these treatments affected duodenal growth. These results suggest that intermittent infusions of these two inhibitors had no effect on normal pancreatic and duodenal growth, but were successful in preventing pancreatic growth induced by PJD. They also indicate that endogenous CCK is involved in PJD-induced pancreatic growth.
ISSN:0013-7227
DOI:10.1210/endo-129-6-2867