Dissecting the allosteric FXR modulation: a chemical biology approach using guggulsterone as a chemical tool

Daniela Passeri; Andrea Carotti; Jose M Ramos Pittol; Gianmario Ciaccioli; Roberto Pellicciari; Saskia W C van Mil; Antimo Gioiello

doi:10.1039/c9md00264b

Dissecting the allosteric FXR modulation: a chemical biology approach using guggulsterone as a chemical tool

Medchemcomm. 2019 Jun 24;10(8):1412-1419. doi: 10.1039/c9md00264b. eCollection 2019 Aug 1.

Authors

Daniela Passeri¹, Andrea Carotti², Jose M Ramos Pittol³, Gianmario Ciaccioli¹, Roberto Pellicciari¹, Saskia W C van Mil^{3

4}, Antimo Gioiello²

Affiliations

¹ TES Pharma , Corso Vannucci 47 , Perugia , Italy.
² Department of Pharmaceutical Sciences , University of Perugia , Perugia , Italy . Email: antimo.gioiello@unipg.it.
³ Center for Molecular Medicine , UMC Utrecht , Utrecht University , Utrecht , The Netherlands.
⁴ Tytgat Institute for Liver and Intestinal Research , Amsterdam UMC , Amsterdam , The Netherlands.

Abstract

Guggulsterone is a promiscuous ligand for endocrine and metabolic lipid receptors traditionally used to treat a number of diseases including diabesity, hyperlipidemia, atherosclerosis, and osteoarthritis. Although relatively weak, its activity at the farnesoid X receptor (FXR) is particularly intriguing as guggulsterone acts as an antagonist with a peculiar ability of gene selective modulation. We report here a chemical biology study with the aim to further characterize the biological action of guggulsterone at the FXR and to obtain further insights into the functional role played by noncanonical FXR binding pockets S2 and S3. Our results suggest that the FXR accessory pockets might act as potential targets for small molecules able to modulate the metabolic activation of the receptor without affecting the anti-inflammatory activity thus revealing a new approach for disclosing selective FXR modulators that might bypass potential side-effects from chronic treatments.