Pharmacophore modeling and virtual screening studies for discovery of novel farnesoid X receptor (FXR) agonists

Shizhen Zhao; Wenjing Peng; Xinping Li; Le Wang; Wenbo Yin; Yan-Dong Wang; Ruifang Hou; Wei-Dong Chen

doi:10.1039/d0ra09320c

Pharmacophore modeling and virtual screening studies for discovery of novel farnesoid X receptor (FXR) agonists

RSC Adv. 2021 Jan 7;11(4):2158-2166. doi: 10.1039/d0ra09320c. eCollection 2021 Jan 6.

Authors

Shizhen Zhao¹, Wenjing Peng¹, Xinping Li¹, Le Wang¹, Wenbo Yin², Yan-Dong Wang³, Ruifang Hou¹, Wei-Dong Chen^{1

4}

Affiliations

¹ Key Laboratory of Receptors-Mediated Gene Regulation and Drug Discovery, People's Hospital of Hebi, School of Medicine, Henan University Henan China hrf8868@163.com wdchen666@163.com.
² Key Laboratory of Structure-Based Drug Design and Discovery, Ministry of Education, School of Pharmaceutical Engineering, Shenyang Pharmaceutical University 103 Wenhua Road, Shenhe District Shenyang 110016 PR China.
³ State Key Laboratory of Chemical Resource Engineering, College of Life Science and Technology, Beijing University of Chemical Technology Beijing China.
⁴ Key Laboratory of Molecular Pathology, School of Basic Medical Science, Inner Mongolia Medical University Hohhot China.

Abstract

Farnesoid X receptor (FXR) agonists would be considered as an important therapeutic strategy for several chronic liver and metabolic diseases. Here we have employed an integrated virtual screening by combining ligand-based pharmacophore mapping and molecular docking to identify novel nonsteroidal FXR agonists. Eighteen compounds were selected for in vitro FXR agonistic activity assay, and results showed five compounds exhibiting promising FXR agonistic activity. Among these compounds, compounds F4 and F17 were the most remarkable in vitro activity by using homogeneous time resolved fluorescence (HTRF) assay and the full-length FXR reporter gene assay in HepG2 cells. Real-time PCR assay was performed to measure the expression of FXR target genes. Compounds F4 and F17 increased small heterodimer partner (SHP), in turn, suppress mRNA levels of cholesterol 7-alpha-hydroxylase (CYP7A1). The obtained compounds F4 and F17 from this study may be potential leads for developing novel FXR agonists in the treatment of metabolic diseases.