Exploring the therapeutic mechanisms of millet in obesity through molecular docking, pharmacokinetics, and dynamic simulation

Komal G Lakhani; Rasmeih Hamid; Sheetal Gupta; Poojaben Prajapati; Ratna Prabha; Saumya Patel; Kirankumar P Suthar

doi:10.3389/fnut.2024.1453819

Exploring the therapeutic mechanisms of millet in obesity through molecular docking, pharmacokinetics, and dynamic simulation

Front Nutr. 2024 Oct 18:11:1453819. doi: 10.3389/fnut.2024.1453819. eCollection 2024.

Authors

Komal G Lakhani^#¹, Rasmeih Hamid^#², Sheetal Gupta³, Poojaben Prajapati⁴, Ratna Prabha⁵, Saumya Patel⁴, Kirankumar P Suthar¹

Affiliations

¹ Department of Plant Molecular Biology and Biotechnology, N. M. College of Agriculture, Navsari Agricultural University, Navsari, India.
² Department of Plant Breeding, Cotton Research Institute of Iran (CRII), Agricultural Research, Education, and Extension Organization (AREEO), Gorgan, Iran.
³ Department of Genetics and Plant Breeding, Navsari Agricultural University, Navsari, India.
⁴ Department of Botany, Bioinformatics, and Climate Change Impacts Management, School of Sciences, Gujarat University, Ahmedabad, India.
⁵ ICAR-Indian Agricultural Research Institute, New Delhi, India.

^# Contributed equally.

Abstract

Obesity, a prevalent global health concern, is characterized by excessive fat accumulation, which confers significant nutritional and health risks, including a shortened lifespan and diminished wellbeing. Central to the regulation of energy balance and food intake is the fat mass and obesity-associated (FTO) protein, which modulates the interplay between caloric consumption and energy expenditure. Given its pivotal role in obesity regulation, the identification of effective inhibitors targeting the FTO protein is imperative for developing therapeutic interventions. Currently available anti-obesity drugs are often plagued by undesirable side effects. In contrast, natural plant-derived bioactive compounds are gaining prominence in the pharmaceutical industry due to their efficacy and lower incidence of adverse effects. Little Millet, a traditional cereal known for its rich nutritional profile and high satiety index, was investigated in this study using molecular docking and dynamics simulation approach for its potential as an anti-obesity agent. Our research demonstrates that four bioactive compounds from Little Millet exhibit superior binding energies ranging from 7.22 to 8.83 kcal/mol, compared to the standard anti-obesity drug, orlistat, which has a binding energy of 5.96 kcal/mol. These compounds fulfilled all drug-like criteria, including the Lipinski, Ghose, Veber, Egan, and Muegge rules, and exhibited favorable profiles in terms of distribution, metabolism, and prolonged half-life without toxicity. Conversely, orlistat was associated with hepatotoxicity, a reduced half-life, and multiple violations of drug-likeness parameters, undermining its efficacy. Molecular dynamics simulations and Gibbs free energy assessments revealed that the four identified compounds maintain stable interactions with key residues in the FTO protein's active site. We propose further validation through extensive In vitro, In vivo, and clinical studies to ascertain the therapeutic potential of these compounds in combating obesity.

Keywords: ADMET; binding free energy; human fat mass and obesity associated protein (FTO); little millet; molecular docking and molecular dynamics (MD) simulation; obesity.

Grants and funding

The author(s) declare that financial support was received for the research, authorship, and/or publication of this article. Komal G. Lakhani gratefully acknowledges the support of the Science and Engineering Research Board (SERB), the Department of Science and Technology (DST), Government of India, and the Confederation of Indian Industry (CII) for the Prime Minister’s Fellowship. This study is the part of master’s student research work and, the university provided the funding from university’s research fund.