1987
DOI: 10.1007/bf02774219
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Effect of synthetic trypsin inhibitor on plasma immunoreactive cholecystokinin in rats

Abstract: A sensitive and specific radioimmunoassay system for rat plasma cholecystokinin (CCK) was employed to study the effect of trypsin inhibitor on plasma CCK levels. Feeding the trypsin inhibitor, FOY-305 200 mg/kg, to rats for 10 days stimulated the pancreatic growth. However, there was no significant difference in fasting plasma concentrations and duodenal contents of CCK and secretin. On the other hand, acute ingestion of same dosage of FOY-305 caused a marked (20-fold) and sustained elevation of plasma CCK lev… Show more

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Cited by 11 publications
(13 citation statements)
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“…A new method of collecting and processing blood has been developed that yields similar recovery (80%) for all molecular forms of cholecystokinin that have been identified in blood (8,11,13,14) or intestinal extracts (3,25) of rat. Furthermore, unlike previous methods used to determine the endocrine form of cholecystokinin in rat (8,11,13,14), this new optimized method prevented degradation of radiolabeled CCK-8 or CCK-58.…”
Section: Discussionmentioning
confidence: 99%
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“…A new method of collecting and processing blood has been developed that yields similar recovery (80%) for all molecular forms of cholecystokinin that have been identified in blood (8,11,13,14) or intestinal extracts (3,25) of rat. Furthermore, unlike previous methods used to determine the endocrine form of cholecystokinin in rat (8,11,13,14), this new optimized method prevented degradation of radiolabeled CCK-8 or CCK-58.…”
Section: Discussionmentioning
confidence: 99%
“…These labels were also used as internal markers of recovery in all determinations of the molecular forms of cholecystokinin in fasted and stimulated rat blood and as markers to decide which fractions from SepPak should be pooled. Additionally, 125 I-Tyr 20 , 125 I-Tyr 52 -labeled CCK-58 was used to compare degradation of peptides by the method developed in this report to a method that simulates prior studies on the molecular forms of cholecystokinin in rats (8,11,13,14).…”
Section: Methodsmentioning
confidence: 99%
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