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  4. Mechanistic Impact of Different Ligand Scaffolds on FXR Modulation Suggests Avenues to Selective Modulators
 
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2022
Journal Article
Title

Mechanistic Impact of Different Ligand Scaffolds on FXR Modulation Suggests Avenues to Selective Modulators

Abstract
The bile-acid sensing nuclear farnesoid X receptor (FXR) is an attractive target for the treatment of hepatic and metabolic diseases, but application of this chemotherapeutic concept remains limited due to adverse effects of FXR activation observed in clinical trials. To elucidate the mechanistic basis of FXR activation at the molecular level, we have systematically studied FXR co-regulator interactions and dimerization in response to seven chemically diverse FXR ligands. Different molecular effects on FXR activation mediated by different scaffolds were evident and aligned with characteristic structural changes within the ligand binding domain of FXR. A partial FXR agonist acted mainly through co-repressor displacement from FXR and caused an FXR-regulated gene expression pattern markedly differing from FXR agonist effects. These results suggest selective modulation of FXR dimerization and co-regulator interactions for different ligands, offering a potential avenue for the design of gene- or tissue-selective FXR modulators.
Author(s)
Heering, Jan
Fraunhofer-Institut für Translationale Medizin und Pharmakologie ITMP  
Jores, Nathalie
Kilu, Whitney
Schallmayer, Espen
Peelen, Evelyn
Muehler, Andreas R.
Kohlhof, Hella
Vitt, Daniel
Linhard, Verena L.
Gande, Santosh Lakshmi
Chaikuad, Apirat
Sreeramulu, Sridhar
Schwalbe, Harald J.
Merk, Daniel J.
Journal
ACS chemical biology  
DOI
10.1021/acschembio.2c00599
Language
English
Fraunhofer-Institut für Translationale Medizin und Pharmakologie ITMP  
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