Multi-model in silico characterization of 3-benzamidobenzoic acid derivatives as partial agonists of Farnesoid X receptor in the management of NAFLD

Soumya Mitra; Amit Kumar Halder; Nilanjan Ghosh; Subhash C Mandal; M Natália D S Cordeiro

doi:10.1016/j.compbiomed.2023.106789

Multi-model in silico characterization of 3-benzamidobenzoic acid derivatives as partial agonists of Farnesoid X receptor in the management of NAFLD

Comput Biol Med. 2023 May:157:106789. doi: 10.1016/j.compbiomed.2023.106789. Epub 2023 Mar 13.

Authors

Soumya Mitra¹, Amit Kumar Halder², Nilanjan Ghosh³, Subhash C Mandal³, M Natália D S Cordeiro⁴

Affiliations

¹ Dr. B.C. Roy College of Pharmacy & Allied Health Sciences, Durgapur, 713206, India.
² Dr. B.C. Roy College of Pharmacy & Allied Health Sciences, Durgapur, 713206, India; LAQV@REQUIMTE/Department of Chemistry and Biochemistry, Faculty of Sciences, University of Porto, 4169-007, Porto, Portugal.
³ Department of Pharmaceutical Technology, Jadavpur University, Kolkata, 700032, India.
⁴ LAQV@REQUIMTE/Department of Chemistry and Biochemistry, Faculty of Sciences, University of Porto, 4169-007, Porto, Portugal. Electronic address: ncordeir@fc.up.pt.

PMID: 36963353
DOI: 10.1016/j.compbiomed.2023.106789

Abstract

Non-alcoholic fatty liver disease (NAFLD) is a pathological condition which is strongly correlated with fat accumulation in the liver that has become a major health hazard globally. So far, limited treatment options are available for the management of NAFLD and partial agonism of Farnesoid X receptor (FXR) has proven to be one of the most promising strategies for treatment of NAFLD. In present work, a range of validated predictive cheminformatics and molecular modeling studies were performed with a series of 3-benzamidobenzoic acid derivatives in order to recognize their structural requirements for possessing higher potency towards FXR. 2D-QSAR models were able to extract the most significant structural attributes determining the higher activity towards the receptor. Ligand-based pharmacophore model was created with a novel and less-explored open access tool named QPhAR to acquire information regarding important 3D-pharmacophoric features that lead to higher agonistic potential towards the FXR. The alignment of the dataset compounds based on pharmacophore mapping led to 3D-QSAR models that pointed out the most crucial steric and electrostatic influence. Molecular dynamics (MD) simulation performed with the most potent and the least potent derivatives of the current dataset helped us to understand how to link the structural interpretations obtained from 2D-QSAR, 3D-QSAR and pharmacophore models with the involvement of specific amino acid residues in the FXR protein. The current study revealed that hydrogen bond interactions with carboxylate group of the ligands play an important role in the ligand receptor binding but higher stabilization of different helices close to the binding site of FXR (e.g., H5, H6 and H8) through aromatic scaffolds of the ligands should lead to higher activity for these ligands. The present work affords important guidelines towards designing novel FXR partial agonists for new therapeutic options in the management of NAFLD. Moreover, we relied mainly on open-access tools to develop the in-silico models in order to ensure their reproducibility as well as utilization.

Keywords: Farnesoid X receptor; Molecular dynamics; Non-alcoholic fatty liver disease; Pharmacophore mapping; QSAR.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Humans
Ligands
Molecular Docking Simulation
Molecular Dynamics Simulation
Non-alcoholic Fatty Liver Disease* / drug therapy
Quantitative Structure-Activity Relationship
RNA-Binding Proteins / antagonists & inhibitors
RNA-Binding Proteins / metabolism
Reproducibility of Results

Substances

Ligands
RNA-Binding Proteins