Literature DB >> 3562296

Fecal steroids and colorectal cancer.

R W Owen, M Dodo, M H Thompson, M J Hill.   

Abstract

The fecal steroid profiles of healthy subjects were compared with those of colorectal cancer (CRC) patients. The multicomponent profiles did not differ qualitatively in that CRC patients, like control subjects, had similar fecal steroids. The major bile acids detected in fecal extracts were lithocholic acid (LCA) and deoxycholic acid (DCA). The major sterol of animal origin was cholesterol and its bacterial metabolite coprostanol, whereas the major plant sterols were beta-sitosterol, stigmasterol, campesterol, and their corresponding bacterial metabolites. CRC patients excreted higher amounts of total major bile acids (LCA and DCA) than did the control group, but this difference was not significant. However, the LCA-to-DCA ratio was much higher in the CRC group [(1.43, p less than 0.01) compared with the control group (0.72)]. The control group excreted significantly higher amounts of total neutral sterols (p less than 0.001), sterols of animal origin (p less than 0.001), and plant sterols (p less than 0.001) compared with the CRC group; the plant sterols represented a much lower proportion of excreted total neutral sterols in the CRC group (p greater than 0.001) compared with the control group. We propose the following hypotheses. The LCA-to-DCA ratio may be an important discriminant market for CRC susceptibility. The fecal LCA-to-DCA ratio may depend on the differential hepatic synthesis of their respective precursors chenodeoxycholic acid (CDCA) and cholic acid. Hepatic synthesis of CDCA may be increased by more efficient conservation of dietary cholesterol because it has been shown that cholesterol of exogenous origin is the main precursor of this bile acid.(ABSTRACT TRUNCATED AT 250 WORDS)

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Year:  1987        PMID: 3562296     DOI: 10.1080/01635588709513914

Source DB:  PubMed          Journal:  Nutr Cancer        ISSN: 0163-5581            Impact factor:   2.900


  11 in total

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2.  Bile acid concentrations, cytotoxicity, and pH of fecal water from patients with colorectal adenomas.

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3.  Advances in Nutritional Metabolomics.

Authors:  Elizabeth P Ryan; Adam L Heuberger; Corey D Broeckling; Erica C Borresen; Cadie Tillotson; Jessica E Prenni
Journal:  Curr Metabolomics       Date:  2013

4.  Regulation of a xenobiotic sulfonation cascade by nuclear pregnane X receptor (PXR).

Authors:  Junichiro Sonoda; Wen Xie; John M Rosenfeld; Joyce L Barwick; Philip S Guzelian; Ronald M Evans
Journal:  Proc Natl Acad Sci U S A       Date:  2002-10-07       Impact factor: 11.205

5.  1H and 13C NMR characterization and stereochemical assignments of bile acids in aqueous media.

Authors:  Omkar B Ijare; B S Somashekar; Y Jadegoud; G A Nagana Gowda
Journal:  Lipids       Date:  2005-10       Impact factor: 1.880

6.  Contributions of bile acids to gastrointestinal physiology as receptor agonists and modifiers of ion channels.

Authors:  Stephen J Keely; Andreacarola Urso; Alexandr V Ilyaskin; Christoph Korbmacher; Nigel W Bunnett; Daniel P Poole; Simona E Carbone
Journal:  Am J Physiol Gastrointest Liver Physiol       Date:  2021-11-10       Impact factor: 4.052

7.  Fecal primary bile acids and serum cholesterol are associated with colorectal adenomas.

Authors:  Séverine Meance; Marie-Christine Boutron-Ruault; Anne Myara; Marie-France Gerhardt; Philippe Marteau; Anne Lavergne; Claire Franchisseur; Christine Bouley
Journal:  Dig Dis Sci       Date:  2003-09       Impact factor: 3.199

8.  Faecal unconjugated bile acids in patients with colorectal cancer or polyps.

Authors:  C H Imray; S Radley; A Davis; G Barker; C W Hendrickse; I A Donovan; A M Lawson; P R Baker; J P Neoptolemos
Journal:  Gut       Date:  1992-09       Impact factor: 23.059

9.  Role of bile acids and metabolic activity of colonic bacteria in increased risk of colon cancer after cholecystectomy.

Authors:  E Zuccato; M Venturi; G Di Leo; L Colombo; C Bertolo; S B Doldi; E Mussini
Journal:  Dig Dis Sci       Date:  1993-03       Impact factor: 3.199

10.  Lithocholic acid can carry out in vivo functions of vitamin D.

Authors:  Jamie A Nehring; Claudia Zierold; Hector F DeLuca
Journal:  Proc Natl Acad Sci U S A       Date:  2007-05-29       Impact factor: 11.205

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