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  4. Novel potent and selective bile acid derivatives as TGR5 agonists: biological screening, structure-activity relationships, and molecular modeling studies
 
research article

Novel potent and selective bile acid derivatives as TGR5 agonists: biological screening, structure-activity relationships, and molecular modeling studies

Sato, Hiroyuki
•
Macchiarulo, Antonio
•
Thomas, Charles
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2008
Journal of medicinal chemistry

TGR5, a metabotropic receptor that is G-protein-coupled to the induction of adenylate cyclase, has been recognized as the molecular link connecting bile acids to the control of energy and glucose homeostasis. With the aim of disclosing novel selective modulators of this receptor and at the same time clarifying the molecular basis of TGR5 activation, we report herein the biological screening of a collection of natural occurring bile acids, bile acid derivatives, and some steroid hormones, which has resulted in the discovery of new potent and selective TGR5 ligands. Biological results of the tested collection of compounds were used to extend the structure-activity relationships of TGR5 agonists and to develop a binary classification model of TGR5 activity. This model in particular could unveil some hidden properties shared by the molecular shape of bile acids and steroid hormones that are relevant to TGR5 activation and may hence be used to address the design of novel selective and potent TGR5 agonists.

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Type
research article
DOI
10.1021/jm7015864
PubMed ID

18307294

Author(s)
Sato, Hiroyuki
Macchiarulo, Antonio
Thomas, Charles
Gioiello, Antimo
Une, Mizuho
Hofmann, Alan F.
Saladin, Régis
Schoonjans, Kristina  
Pellicciari, Roberto
Auwerx, Johan  
Date Issued

2008

Published in
Journal of medicinal chemistry
Volume

51

Issue

6

Start page

1831

End page

41

Editorial or Peer reviewed

REVIEWED

Written at

OTHER

EPFL units
LISP  
UPSCHOONJANS  
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/36724
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