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  4. The bile acid membrane receptor TGR5: a valuable metabolic target
 
research article

The bile acid membrane receptor TGR5: a valuable metabolic target

Pols, Thijs W. H.  
•
Noriega, Lilia G.  
•
Nomura, Mitsunori  
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2011
Digestive diseases (Basel, Switzerland)

Bile acids (BAs) are amphipathic molecules that facilitate the uptake of lipids, and their levels fluctuate in the intestines as well as in the circulation depending on food intake. Besides their role in dietary lipid absorption, BAs function as signaling molecules that activate specific BA receptors and trigger downstream signaling cascades. The BA receptors and the signaling pathways they control are not only important in the regulation of BA synthesis and their metabolism, but they also regulate glucose homeostasis, lipid metabolism and energy expenditure - processes relevant in the context of the metabolic syndrome. In addition to the function of the nuclear receptor FXRα in regulating local effects of BAs in the organs of the enterohepatic axis, increasing evidence points to a crucial role of the G-protein-coupled receptor TGR5 in mediating systemic actions of BAs. Here we review the current knowledge on BA receptors, with a strong focus on the cell membrane receptor TGR5, which has emerged as a promising target for intervention in metabolic diseases.

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Type
research article
DOI
10.1159/000324126
Web of Science ID

WOS:000291783600006

Author(s)
Pols, Thijs W. H.  
•
Noriega, Lilia G.  
•
Nomura, Mitsunori  
•
Auwerx, Johan  
•
Schoonjans, Kristina  
Date Issued

2011

Published in
Digestive diseases (Basel, Switzerland)
Volume

29

Issue

1

Start page

37

End page

44

Subjects

Metabolism

•

Bile acids

•

Nuclear receptors

•

Tgr5

•

G-protein-coupled receptor

•

Activated Protein-Kinases

•

Glucagon-Like Peptide-1

•

Pregnane-X-Receptor

•

Nuclear Receptor

•

Lithocholic Acid

•

Life-Span

•

Identification

•

Gpbar1

•

Cells

•

Hepatocytes

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
UPSCHOONJANS  
LISP  
Available on Infoscience
November 15, 2011
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/72614
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