Conjugated bile acid replacement therapy for short-bowel syndrome

Although fat malabsorption in the short-bowel syndrome is caused in part by decreased bile acid secretion, bile acid replacement therapy is not used because of the belief that ingested bile acids would worsen diarrhea, outweighing the benefits of improved fat absorption. This study compared the effe...

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Published inGastroenterology (New York, N.Y. 1943) Vol. 116; no. 1; p. 15
Main Authors Gruy-Kapral, C, Little, K H, Fordtran, J S, Meziere, T L, Hagey, L R, Hofmann, A F
Format Journal Article
LanguageEnglish
Published United States 01.01.1999
Subjects
Animals
Aspartate Aminotransferases - blood
Bile Acids and Salts - adverse effects
Bile Acids and Salts - therapeutic use
Body Weight - drug effects
Cattle
Cholic Acids - adverse effects
Cholic Acids - therapeutic use
Diarrhea - drug therapy
Dietary Fats - metabolism
Energy Intake
Feces - chemistry
Female
Follow-Up Studies
Humans
Ileostomy
Intestinal Absorption
Middle Aged
Sarcosine - adverse effects
Sarcosine - analogs & derivatives
Sarcosine - therapeutic use
Short Bowel Syndrome - drug therapy
Short Bowel Syndrome - metabolism
Short Bowel Syndrome - physiopathology
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Summary:Although fat malabsorption in the short-bowel syndrome is caused in part by decreased bile acid secretion, bile acid replacement therapy is not used because of the belief that ingested bile acids would worsen diarrhea, outweighing the benefits of improved fat absorption. This study compared the effect of a natural conjugated bile acid mixture from ox bile with that of cholylsarcosine, a synthetic conjugated bile acid, on fat absorption and diarrhea in a patient with the short-bowel syndrome. Cholylsarcosine is resistant to bacterial metabolism and has no cathartic activity. Metabolic balance studies and a clinical trial were performed in an emaciated patient with the short-bowel syndrome and ileostomy in whom parenteral nutrition could not be used. In balance studies, conjugated bile acid replacement therapy with either preparation caused fat absorption to increase by approximately 40 g/day. Calcium absorption also increased. Neither bile acid product caused a clinically significant increase in ileostomy water output. During a 4-month outpatient trial, while the patient ingested 2 g/meal natural bile acids, her weight increased from 80 to 98 lb, without side effects. Conjugated bile acid replacement therapy should be part of the armamentarium for the treatment of selected patients with the short-bowel syndrome.
ISSN:0016-5085
DOI:10.1016/S0016-5085(99)70223-4