Equilibrium and kinetic factors influencing bile sequestrant efficacy

In vitro bile salt binding equilibria and kinetic studies were performed with cholestyramine to determine how these factors influence bile sequestrant efficacy in vivo. Chloride ion at physiologic concentrations caused more than a twofold reduction in glycocholate (GCH) binding, compared to binding...

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Bibliographic Details
Published inPharmaceutical research Vol. 9; no. 5; p. 670
Main Authors Luner, P E, Amidon, G L
Format Journal Article
LanguageEnglish
Published United States 01.05.1992
Subjects
Anions - metabolism
Bile Acids and Salts - metabolism
Binding, Competitive - physiology
Chlorides - metabolism
Cholestyramine Resin - metabolism
Chromatography, High Pressure Liquid
Digestive System Physiological Phenomena
Humans
Intestinal Absorption - physiology
Kinetics
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Summary:In vitro bile salt binding equilibria and kinetic studies were performed with cholestyramine to determine how these factors influence bile sequestrant efficacy in vivo. Chloride ion at physiologic concentrations caused more than a twofold reduction in glycocholate (GCH) binding, compared to binding in the absence of salt, over a range of GCH concentrations and was also observed to displace bound GCH. In addition, chloride ion displaced from cholestyramine as a result of bile salt binding was measured using a chloride selective electrode, and the results show that bile salt binding is due to ion exchange. Comparison of the results of the equilibrium binding experiments to human data shows that the effect of anion binding competition alone cannot account for the lack of efficacy of cholestyramine. Consideration of other effects, such as additional binding competition or poor availability for binding, based on data from the literature, shows that adequate bile salt binding potential exists and that these interferences are not major factors influencing resin efficacy. In kinetic studies, both binding uptake of GCH and displacement of GCH from cholestyramine by chloride ion were relatively rapid, indicating that cholestyramine should equilibrate rapidly with bile salts in the GI tract. Based on these findings, it is suggested that the low efficacy of cholestyramine is a result mainly of its relatively poor ability to prevent bile salt reabsorption in the ileum.
ISSN:0724-8741
DOI:10.1023/A:1015862329303