Cholecystokinin Increases Bile Acid Synthesis with Total Parenteral Nutrition but Does Not Prevent Stone Formation

Total parenteral nutrition (TPN) is associated with cholestasis and gallstones. Gallbladder stasis may be important in the development of gallstones, and cholecystokinin (CCK) to stimulate gallbadder contraction has been proposed as a treatment to prevent this complication. We studiedin vivobile aci...

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Bibliographic Details
Published in:The Journal of surgical research 1997-01, Vol.67 (1), p.84-89
Main Authors: Dawes, Lillian G., Muldoon, Joseph P., Greiner, Mary Anne, Bertolotti, Marco
Format: Article
Language:English
Subjects:
Anesthesia. Intensive care medicine. Transfusions. Cell therapy and gene therapy
Animals
Bile Acids and Salts - agonists
Bile Acids and Salts - biosynthesis
Bile Acids and Salts - chemistry
Biological and medical sciences
Cholecystokinin - pharmacology
Cholelithiasis - diet therapy
Cholelithiasis - prevention & control
Emergency and intensive care: metabolism and nutrition disorders. Enteral and parenteral nutrition
Intensive care medicine
Medical sciences
Parenteral Nutrition
Swine
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Summary:Total parenteral nutrition (TPN) is associated with cholestasis and gallstones. Gallbladder stasis may be important in the development of gallstones, and cholecystokinin (CCK) to stimulate gallbadder contraction has been proposed as a treatment to prevent this complication. We studiedin vivobile acid synthesis and bile acid output in miniswine on TPN to test whether daily CCK improves bile acid output and normalizes bile acid profiles with TPN. Nine miniswine were nutritionally maintained with TPN for 4 weeks; four pigs received CCK (0.1 mg/kg) iv daily.In vivobile acid synthesis was measured with injection of 7α-tritiated cholesterol. An increase in tritiated water reflects the activity of 7α-hydroxylation, the rate-limiting step in bile acid synthesis. At the end of 4 weeks, bile was collected and bile acid output and bile salt profiles were determined. One of five animals on TPN developed gallstones while two of four receiving daily CCK developed stones.In vivobile acid synthesis decreased with TPN (controls, 63 ± 9 mg/24 hr versus TPN, 13 ± 4 mg/24 hr) and increased in TPN animals with CCK treatment (TPN-CCK, 105 ± 35 mg/24 hr). Bile acid profiles are changed with TPN with more secondary bile acids, this was not improved with CCK. CCK improved bile acid synthesis and bile acid output but failed to prevent gallstone formation or normalize bile salt profiles. In addition to promoting gallbladder contraction, CCK may have a stimulatory effect on bile acid synthesis. CCK alone did not prevent gallstone formation.
ISSN:0022-4804
1095-8673
DOI:10.1006/jsre.1996.4953