In silico and in vitro analysis of PPAR - α / γ dual agonists: Comparative evaluation of potential phytochemicals with anti-obesity drug orlistat

Sumit Kumar Mandal; Banoth Karan Kumar; Pankaj Kumar Sharma; Sankaranarayanan Murugesan; P R Deepa

doi:10.1016/j.compbiomed.2022.105796

In silico and in vitro analysis of PPAR - α / γ dual agonists: Comparative evaluation of potential phytochemicals with anti-obesity drug orlistat

Comput Biol Med. 2022 Aug:147:105796. doi: 10.1016/j.compbiomed.2022.105796. Epub 2022 Jun 28.

Authors

Sumit Kumar Mandal¹, Banoth Karan Kumar², Pankaj Kumar Sharma¹, Sankaranarayanan Murugesan², P R Deepa³

Affiliations

¹ Department of Biological Sciences, Birla Institute of Technology and Science Pilani, Pilani Campus, Pilani, 333 031, Rajasthan, India.
² Medicinal Chemistry Research Laboratory, Department of Pharmacy, Birla Institute of Technology and Science Pilani, Pilani Campus, Pilani, 333 031, Rajasthan, India.
³ Department of Biological Sciences, Birla Institute of Technology and Science Pilani, Pilani Campus, Pilani, 333 031, Rajasthan, India. Electronic address: deepa@pilani.bits-pilani.ac.in.

PMID: 35809408
DOI: 10.1016/j.compbiomed.2022.105796

Abstract

Obesity is an abnormal fat accumulation disorder in the metabolic syndrome constellation, and a risk factor for diabetes, cardiovascular disorders, non-alcoholic fatty liver disease (NAFLD), and cancer. Nuclear receptors (Peroxisome proliferator-activated receptor, PPAR) are implicated in metabolic syndrome and NAFLD, and have potential for therapeutic targeting. Nuclear receptors are ligand-dependent transcription factors that have diverse roles in metabolism, including regulating genes involved in lipid and glucose metabolism, modulating inflammatory genes, and are crucial for maintaining metabolic flexibility. PPAR activates adipose triglyceride lipase, which then releases fatty acids as ligands for PPAR, indicating the interdependency of nuclear receptors and lipases. Here, molecular docking was performed with selected phytochemical ligands that can bind with PPAR-α/γ (PDB ID: 2ZNN and 2ATH, respectively) using Glide module of Schrodinger software followed by molecular dynamics simulation study using Desmond module, and ADMET analysis. Interestingly, orlistat which is a well-known lipase and fatty acid synthase inhibitor also demonstrated favorable binding affinity with both PPAR-α/γ (-10.96 kcal/mol against PPARα and -10.26 kcal/mol against PPARγ). The highest docking scores were however shown by the flavonoids - rutin (-14.88 kcal/mol against PPARα and -13.64 kcal/mol against PPARγ), and its aglycone, quercetin (-10.08 kcal/mol in PPARα and -9.89 kcal/mol in PPARγ). The other phytochemicals (genistein, esculin, daidzin, naringenin, daidzein, dihydroxy coumarin, hydroquinone) showed lower binding affinity as dual agonists. The anti-obesity effects were experimentally validated in cultured adipocytes, which revealed better lipid inhibition by rutin and quercetin than orlistat (quercetin > rutin > orlistat) pointing to their strong potential in anti-obesity treatment.

Keywords: Molecular docking; Molecular dynamics; Obesity; Orlistat; Peroxisome proliferator activated receptor alpha/ gamma; Phytochemicals.

Publication types

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

MeSH terms

Anti-Obesity Agents* / pharmacology
Anti-Obesity Agents* / therapeutic use
Humans
Ligands
Lipids
Metabolic Syndrome*
Molecular Docking Simulation
Non-alcoholic Fatty Liver Disease*
Obesity / drug therapy
Orlistat / pharmacology
PPAR alpha / chemistry
PPAR alpha / metabolism
PPAR gamma / chemistry
PPAR gamma / metabolism
Phytochemicals / pharmacology
Quercetin
Rutin / pharmacology

Substances

Anti-Obesity Agents
Ligands
Lipids
PPAR alpha
PPAR gamma
Phytochemicals
Rutin
Orlistat
Quercetin