"FXR-Induced Secretion of FGF15/19 Inhibits CYP27 Expression in Cholang" by Dongju Jung, J. Philippe York et al.

ETSU Faculty Works

Title

FXR-Induced Secretion of FGF15/19 Inhibits CYP27 Expression in Cholangiocytes Through p38 Kinase Pathway

Creator(s)

Dongju Jung, Baylor College of Medicine
J. Philippe York, Weill Cornell Medicine
Li Wang, University of Utah School of Medicine
Chaofeng Yang, University of Texas Health Science Center at Houston
Aijun Zhang, Weill Cornell Medicine
Heather L. Francis, VA Medical Center
Paul Webb, Weill Cornell Medicine
Wallace L. McKeehan, University of Texas Health Science Center at Houston
Gianfranco Alpini, VA Medical Center
Gene D. LeSage, Quillen-Dishner College of Medicine
David D. Moore, Baylor College of Medicine
Xuefeng Xia, Weill Cornell Medicine

Document Type

Article

Publication Date

1-1-2014

Description

Cholangiocytes, bile duct lining cells, actively adjust the amount of cholesterol and bile acids in bile through expression of enzymes and channels involved in transportation and metabolism of the cholesterol and bile acids. Herein, we report molecular mechanisms regulating bile acid biosynthesis in cholangiocytes. Among the cytochrome p450 (Cyp) enzymes involved in bile acid biosynthesis, sterol 27-hydroxylase (Cyp27) that is the rate-limiting enzyme for the acidic pathway of bile acid biosynthesis expressed in cholangiocytes. Expression of other Cyp enzymes for the basic bile acid biosynthesis was hardly detected. The Cyp27 expression was negatively regulated by a hydrophobic bile acid through farnesoid X receptor (FXR), a nuclear receptor activated by bile acid ligands. Activated FXR exerted the negative effects by inducing an expression of fibroblast growth factor 15/19 (FGF15/19). Similar to its repressive function against cholesterol 7α-hydroxylase (Cyp7a1) expression in hepatocytes, secreted FGF15/19 triggered Cyp27 repression in cholangiocytes through interaction with its cognate receptor fibroblast growth factor receptor 4 (FGFR4). The involvements of FXR and FGFR4 for the bile acid-induced Cyp27 repression were confirmed in vivo using knockout mouse models. Different from the signaling in hepatocytes, wherein the FGF15/19-induced repression signaling is mediated by c-Jun N-terminal kinase (JNK), FGF15/19-induced Cyp27 repression in cholangiocytes was mediated by p38 kinase. Thus, the results collectively suggest that cholangiocytes may be able to actively regulate bile acid biosynthesis in cholangiocytes and even hepatocyte by secreting FGF15/19. We suggest the presence of cholangiocyte-mediated intrahepatic feedback loop in addition to the enterohepatic feedback loop against bile acid biosynthesis in the liver.

Citation Information

Jung, Dongju; York, J. Philippe; Wang, Li; Yang, Chaofeng; Zhang, Aijun; Francis, Heather L.; Webb, Paul; McKeehan, Wallace L.; Alpini, Gianfranco; LeSage, Gene D.; Moore, David D.; and Xia, Xuefeng. 2014. FXR-Induced Secretion of FGF15/19 Inhibits CYP27 Expression in Cholangiocytes Through p38 Kinase Pathway. Pflugers Archiv European Journal of Physiology. Vol.466(5). 1011-1019. https://doi.org/10.1007/s00424-013-1364-3 PMID: 24068255 ISSN: 0031-6768

Link to Full Text

Find in your library

COinS

Digital Commons @ East Tennessee State University

ETSU Faculty Works

Title

Creator(s)

Document Type

Publication Date

Description

Citation Information

Search

Browse All

Browse Faculty Works

Author Corner

Links