Intestinal FXR-mediated FGF15 production contributes to diurnal control of hepatic bile acid synthesis in mice

Johanna H. M. Stroeve; Gemma Brufau; Frans Stellaard; Frank J. Gonzalez; Bart Staels; Folkert Kuipers

doi:10.1038/labinvest.2010.107

Intestinal FXR-mediated FGF15 production contributes to diurnal control of hepatic bile acid synthesis in mice

Johanna H. M. Stroeve^*
, Gemma Brufau
, Frans Stellaard
, Frank J. Gonzalez
, Bart Staels
, Folkert Kuipers

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

86 Citations (Scopus)

Abstract

Hepatic bile acid synthesis is subject to complex modes of transcriptional control, in which the bile acid-activated nuclear receptor farnesoid X receptor (FXR) in liver and intestine-derived, FXR-controlled fibroblast growth factor 15 (Fgf15) are involved. The Fgf15 pathway is assumed to contribute significantly to control of hepatic bile acid synthesis. However, scientific evidence supporting this assumption is primarily based on gene expression data. Using intestine-selective FXR knockout mice (iFXR-KO), we show that contribution of intestinal FXR-Fgf15 signalling in regulation of hepatic cholesterol 7a-hydroxylase (Cyp7A1) expression depends on time of the day with increased hepatic Cyp7A1 expression in iFXR-KO mice compared with controls exclusively during the dark phase. To assess the physiological relevance hereof, we determined effects of intestine-selective deletion of FXR on physiological parameters such as bile formation and kinetics of the enterohepatic circulation of bile acids. It appeared that intestinal FXR deficiency leads to a modest but significant increase in cholic acid pool size, without changes in fractional turnover rate. As a consequence, bile flow and biliary bile acid secretion rates were increased in iFXR-KO mice compared with controls. Feeding a bile acid-containing diet or treatment with a bile acid sequestrant similarly affected bile formation in iFXR-KO and control mice and induced similar changes in Cyp7A1 and Cyp8B1 expression patterns. In conclusion, this study is the first to demonstrate the physiological relevance of the contribution of the intestinal FXR-Fgf15 signalling pathway in control of hepatic bile acid synthesis. Fgf15 contributes to the regulation of hepatic bile acid synthesis in mice mainly during the dark phase. Expansion of the circulating bile acid pool as well as bile acid sequestration diminishes the contribution of intestinal FXR-Fgf15 signalling in control of hepatic bile acid synthesis and bile formation. Laboratory Investigation (2010) 90, 1457-1467; doi: 10.1038/labinvest.2010.107; published online 7 June 2010

Original language	English
Pages (from-to)	1457-1467
Number of pages	11
Journal	Laboratory Investigation
Volume	90
Issue number	10
DOIs	https://doi.org/10.1038/labinvest.2010.107
Publication status	Published - Oct-2010

Keywords

bile acids
circadian rhythm
Cyp7A1
enterohepatic circulation
Fgf15
Fxr
FARNESOID-X-RECEPTOR
NUCLEAR RECEPTOR
DEFICIENT MICE
CHOLESTEROL
METABOLISM
HOMEOSTASIS
LIVER
GENE
FIBROBLAST-GROWTH-FACTOR-19
TRANSCRIPTION

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@article{a0bf68bb93fa4031822fcf3d925f8e93,

title = "Intestinal FXR-mediated FGF15 production contributes to diurnal control of hepatic bile acid synthesis in mice",

abstract = "Hepatic bile acid synthesis is subject to complex modes of transcriptional control, in which the bile acid-activated nuclear receptor farnesoid X receptor (FXR) in liver and intestine-derived, FXR-controlled fibroblast growth factor 15 (Fgf15) are involved. The Fgf15 pathway is assumed to contribute significantly to control of hepatic bile acid synthesis. However, scientific evidence supporting this assumption is primarily based on gene expression data. Using intestine-selective FXR knockout mice (iFXR-KO), we show that contribution of intestinal FXR-Fgf15 signalling in regulation of hepatic cholesterol 7a-hydroxylase (Cyp7A1) expression depends on time of the day with increased hepatic Cyp7A1 expression in iFXR-KO mice compared with controls exclusively during the dark phase. To assess the physiological relevance hereof, we determined effects of intestine-selective deletion of FXR on physiological parameters such as bile formation and kinetics of the enterohepatic circulation of bile acids. It appeared that intestinal FXR deficiency leads to a modest but significant increase in cholic acid pool size, without changes in fractional turnover rate. As a consequence, bile flow and biliary bile acid secretion rates were increased in iFXR-KO mice compared with controls. Feeding a bile acid-containing diet or treatment with a bile acid sequestrant similarly affected bile formation in iFXR-KO and control mice and induced similar changes in Cyp7A1 and Cyp8B1 expression patterns. In conclusion, this study is the first to demonstrate the physiological relevance of the contribution of the intestinal FXR-Fgf15 signalling pathway in control of hepatic bile acid synthesis. Fgf15 contributes to the regulation of hepatic bile acid synthesis in mice mainly during the dark phase. Expansion of the circulating bile acid pool as well as bile acid sequestration diminishes the contribution of intestinal FXR-Fgf15 signalling in control of hepatic bile acid synthesis and bile formation. Laboratory Investigation (2010) 90, 1457-1467; doi: 10.1038/labinvest.2010.107; published online 7 June 2010",

keywords = "bile acids, circadian rhythm, Cyp7A1, enterohepatic circulation, Fgf15, Fxr, FARNESOID-X-RECEPTOR, NUCLEAR RECEPTOR, DEFICIENT MICE, CHOLESTEROL, METABOLISM, HOMEOSTASIS, LIVER, GENE, FIBROBLAST-GROWTH-FACTOR-19, TRANSCRIPTION",

author = "Stroeve, \{Johanna H. M.\} and Gemma Brufau and Frans Stellaard and Gonzalez, \{Frank J.\} and Bart Staels and Folkert Kuipers",

year = "2010",

month = oct,

doi = "10.1038/labinvest.2010.107",

language = "English",

volume = "90",

pages = "1457--1467",

journal = "Laboratory Investigation",

issn = "0023-6837",

publisher = "SPRINGERNATURE",

number = "10",

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TY - JOUR

T1 - Intestinal FXR-mediated FGF15 production contributes to diurnal control of hepatic bile acid synthesis in mice

AU - Stroeve, Johanna H. M.

AU - Brufau, Gemma

AU - Stellaard, Frans

AU - Gonzalez, Frank J.

AU - Staels, Bart

AU - Kuipers, Folkert

PY - 2010/10

Y1 - 2010/10

N2 - Hepatic bile acid synthesis is subject to complex modes of transcriptional control, in which the bile acid-activated nuclear receptor farnesoid X receptor (FXR) in liver and intestine-derived, FXR-controlled fibroblast growth factor 15 (Fgf15) are involved. The Fgf15 pathway is assumed to contribute significantly to control of hepatic bile acid synthesis. However, scientific evidence supporting this assumption is primarily based on gene expression data. Using intestine-selective FXR knockout mice (iFXR-KO), we show that contribution of intestinal FXR-Fgf15 signalling in regulation of hepatic cholesterol 7a-hydroxylase (Cyp7A1) expression depends on time of the day with increased hepatic Cyp7A1 expression in iFXR-KO mice compared with controls exclusively during the dark phase. To assess the physiological relevance hereof, we determined effects of intestine-selective deletion of FXR on physiological parameters such as bile formation and kinetics of the enterohepatic circulation of bile acids. It appeared that intestinal FXR deficiency leads to a modest but significant increase in cholic acid pool size, without changes in fractional turnover rate. As a consequence, bile flow and biliary bile acid secretion rates were increased in iFXR-KO mice compared with controls. Feeding a bile acid-containing diet or treatment with a bile acid sequestrant similarly affected bile formation in iFXR-KO and control mice and induced similar changes in Cyp7A1 and Cyp8B1 expression patterns. In conclusion, this study is the first to demonstrate the physiological relevance of the contribution of the intestinal FXR-Fgf15 signalling pathway in control of hepatic bile acid synthesis. Fgf15 contributes to the regulation of hepatic bile acid synthesis in mice mainly during the dark phase. Expansion of the circulating bile acid pool as well as bile acid sequestration diminishes the contribution of intestinal FXR-Fgf15 signalling in control of hepatic bile acid synthesis and bile formation. Laboratory Investigation (2010) 90, 1457-1467; doi: 10.1038/labinvest.2010.107; published online 7 June 2010

AB - Hepatic bile acid synthesis is subject to complex modes of transcriptional control, in which the bile acid-activated nuclear receptor farnesoid X receptor (FXR) in liver and intestine-derived, FXR-controlled fibroblast growth factor 15 (Fgf15) are involved. The Fgf15 pathway is assumed to contribute significantly to control of hepatic bile acid synthesis. However, scientific evidence supporting this assumption is primarily based on gene expression data. Using intestine-selective FXR knockout mice (iFXR-KO), we show that contribution of intestinal FXR-Fgf15 signalling in regulation of hepatic cholesterol 7a-hydroxylase (Cyp7A1) expression depends on time of the day with increased hepatic Cyp7A1 expression in iFXR-KO mice compared with controls exclusively during the dark phase. To assess the physiological relevance hereof, we determined effects of intestine-selective deletion of FXR on physiological parameters such as bile formation and kinetics of the enterohepatic circulation of bile acids. It appeared that intestinal FXR deficiency leads to a modest but significant increase in cholic acid pool size, without changes in fractional turnover rate. As a consequence, bile flow and biliary bile acid secretion rates were increased in iFXR-KO mice compared with controls. Feeding a bile acid-containing diet or treatment with a bile acid sequestrant similarly affected bile formation in iFXR-KO and control mice and induced similar changes in Cyp7A1 and Cyp8B1 expression patterns. In conclusion, this study is the first to demonstrate the physiological relevance of the contribution of the intestinal FXR-Fgf15 signalling pathway in control of hepatic bile acid synthesis. Fgf15 contributes to the regulation of hepatic bile acid synthesis in mice mainly during the dark phase. Expansion of the circulating bile acid pool as well as bile acid sequestration diminishes the contribution of intestinal FXR-Fgf15 signalling in control of hepatic bile acid synthesis and bile formation. Laboratory Investigation (2010) 90, 1457-1467; doi: 10.1038/labinvest.2010.107; published online 7 June 2010

KW - bile acids

KW - circadian rhythm

KW - Cyp7A1

KW - enterohepatic circulation

KW - Fgf15

KW - Fxr

KW - FARNESOID-X-RECEPTOR

KW - NUCLEAR RECEPTOR

KW - DEFICIENT MICE

KW - CHOLESTEROL

KW - METABOLISM

KW - HOMEOSTASIS

KW - LIVER

KW - GENE

KW - FIBROBLAST-GROWTH-FACTOR-19

KW - TRANSCRIPTION

U2 - 10.1038/labinvest.2010.107

DO - 10.1038/labinvest.2010.107

M3 - Article

SN - 0023-6837

VL - 90

SP - 1457

EP - 1467

JO - Laboratory Investigation

JF - Laboratory Investigation

IS - 10

ER -

Intestinal FXR-mediated FGF15 production contributes to diurnal control of hepatic bile acid synthesis in mice

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