Issue 10, 2018
From the journal:

MedChemComm

Discovery of new FXR agonists based on 6-ECDCA binding properties by virtual screening and molecular docking

Antonella Giancristofaro,a   Arménio J. M. Barbosa, ORCID logo b   Alessandra Ammazzalorso,a   Pasquale Amoia,a   Barbara De Filippis,a   Marialuigia Fantacuzzi,a   Letizia Giampietro,a   Cristina Maccallinia  and  Rosa Amoroso ORCID logo *a  

* Corresponding authors

a Department of Pharmacy, University of Chieti “G. d'Annunzio”, via dei vestini 31, 66100 Chieti, Italy
E-mail: rosa.amoroso@unich.it

b Chemistry Department, Faculdade de Ciências e Tecnologia, Universidade Nova de Lisboa, 2829-516 Caparica, Portugal

Abstract

FXR is a member of the nuclear receptor superfamily, which regulates the expression of various genes involved in bile acid, lipid and glucose metabolism. Targeting FXR with small molecules has been exploited to treat lipid-related disorders and diseases such as cholestasis, gallstones and hepatic disorders. In this work, we expand the existing pool of known FXR agonists using a fast hit-to-lead structure-based pharmacophore and docking screening protocol. A set of 25 molecules was selected after screening a large database of commercial chemicals, and experimental tests were carried out to demonstrate their ability to activate FXR. Three novel FXR agonists are reported, namely, one full agonist, more efficient than the endogenous ligand chenodeoxycholic acid, and two partial agonists.

Graphical abstract: Discovery of new FXR agonists based on 6-ECDCA binding properties by virtual screening and molecular docking

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Article information

DOI
https://doi.org/10.1039/C8MD00272J
Article type
Research Article
Submitted
28 May 2018
Accepted
28 Jun 2018
First published
04 Jul 2018

Med. Chem. Commun., 2018,9, 1630-1638

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Discovery of new FXR agonists based on 6-ECDCA binding properties by virtual screening and molecular docking

A. Giancristofaro, A. J. M. Barbosa, A. Ammazzalorso, P. Amoia, B. De Filippis, M. Fantacuzzi, L. Giampietro, C. Maccallini and R. Amoroso, Med. Chem. Commun., 2018, 9, 1630 DOI: 10.1039/C8MD00272J

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