Identification of a Nuclear Receptor for Bile Acids

Makoto Makishima(Howard Hughes Medical Institute), Arthur Y. Okamoto(TiVo (United States)), Joyce J. Repa(Howard Hughes Medical Institute), Hua Tu(TiVo (United States)), R. Marc Learned(TiVo (United States)), Alvin Luk(TiVo (United States)), Mitchell Hull(TiVo (United States)), Kevin D. Lustig(TiVo (United States)), David J. Mangelsdorf(Howard Hughes Medical Institute), Bei Shan(TiVo (United States))
Science
May 21, 1999
10.1126/science.284.5418.1362
Cited by 2,672

Abstract

Bile acids are essential for the solubilization and transport of dietary lipids and are the major products of cholesterol catabolism. Results presented here show that bile acids are physiological ligands for the farnesoid X receptor (FXR), an orphan nuclear receptor. When bound to bile acids, FXR repressed transcription of the gene encoding cholesterol 7alpha-hydroxylase, which is the rate-limiting enzyme in bile acid synthesis, and activated the gene encoding intestinal bile acid-binding protein, which is a candidate bile acid transporter. These results demonstrate a mechanism by which bile acids transcriptionally regulate their biosynthesis and enterohepatic transport.

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