In Silico Molecular Docking Analysis of Karanjin against Alzheimer's and Parkinson's Diseases as a Potential Natural Lead Molecule for New Drug Design, Development and Therapy

Charles Gnanaraj; Mahendran Sekar; Shivkanya Fuloria; Shasank S Swain; Siew Hua Gan; Kumarappan Chidambaram; Nur Najihah Izzati Mat Rani; Tavamani Balan; Sarah Stephenie; Pei Teng Lum; Srikanth Jeyabalan; M Yasmin Begum; Vivek Chandramohan; Lakshmi Thangavelu; Vetriselvan Subramaniyan; Neeraj Kumar Fuloria

doi:10.3390/molecules27092834

In Silico Molecular Docking Analysis of Karanjin against Alzheimer's and Parkinson's Diseases as a Potential Natural Lead Molecule for New Drug Design, Development and Therapy

Molecules. 2022 Apr 29;27(9):2834. doi: 10.3390/molecules27092834.

Authors

Charles Gnanaraj¹, Mahendran Sekar², Shivkanya Fuloria³, Shasank S Swain⁴, Siew Hua Gan⁵, Kumarappan Chidambaram⁶, Nur Najihah Izzati Mat Rani¹, Tavamani Balan¹, Sarah Stephenie⁷, Pei Teng Lum², Srikanth Jeyabalan⁸, M Yasmin Begum⁹, Vivek Chandramohan¹⁰, Lakshmi Thangavelu¹¹, Vetriselvan Subramaniyan¹², Neeraj Kumar Fuloria^{3

11}

Affiliations

¹ Faculty of Pharmacy and Health Sciences, Royal College of Medicine Perak, Universiti Kuala Lumpur, Ipoh 30450, Malaysia.
² Department of Pharmaceutical Chemistry, Faculty of Pharmacy and Health Sciences, Royal College of Medicine Perak, Universiti Kuala Lumpur, Ipoh 30450, Malaysia.
³ Faculty of Pharmacy, Centre of Excellence for Biomaterials Engineering, AIMST University, Bedong 08100, Malaysia.
⁴ Division of Microbiology and NCDs, ICMR-Regional Medical Research Centre, Bhubaneswar 751023, India.
⁵ School of Pharmacy, Monash University Malaysia, Bandar Sunway 47500, Malaysia.
⁶ Department of Pharmacology, College of Pharmacy, King Khalid University, Abha 62529, Saudi Arabia.
⁷ School of Biological Sciences, Faculty of Science and Technology, Quest International University Perak, Jalan Raja Permaisuri Bainun, Ipoh 30250, Malaysia.
⁸ Department of Pharmacology, Sri Ramachandra Faculty of Pharmacy, Sri Ramachandra Institute of Higher Education and Research (DU), Porur, Chennai 600116, India.
⁹ Department of Pharmaceutics, College of Pharmacy, King Khalid University, Abha 61421, Saudi Arabia.
¹⁰ Department of Biotechnology, Siddaganga Institute of Technology, Tumakuru 572103, India.
¹¹ Center for Transdisciplinary Research, Department of Pharmacology, Saveetha Dental College and Hospital, Saveetha Institute of Medical and Technical Sciences, Saveetha University, Chennai 600077, India.
¹² Faculty of Medicine, Bioscience and Nursing, MAHSA University, Jalan SP 2, Bandar Saujana Putra, Jenjarom 42610, Malaysia.

Abstract

Parkinson's disease (PD) and Alzheimer's disease (AD) are neurodegenerative disorders that have emerged as among the serious health problems of the 21st century. The medications currently available to treat AD and PD have limited efficacy and are associated with side effects. Natural products are one of the most vital and conservative sources of medicines for treating neurological problems. Karanjin is a furanoflavonoid, isolated mainly from Pongamia pinnata with several medicinal plants, and has been reported for numerous health benefits. However, the effect of karanjin on AD and PD has not yet been systematically investigated. To evaluate the neuroprotective effect of karanjin, extensive in silico studies starting with molecular docking against five putative targets for AD and four targets for PD were conducted. The findings were compared with three standard drugs using Auto Dock 4.1 and Molegro Virtual Docker software. Additionally, the physiochemical properties (Lipinski rule of five), drug-likeness and parameters including absorption, distribution, metabolism, elimination and toxicity (ADMET) profiles of karanjin were also studied. The molecular dynamics (MD) simulations were performed with two selective karanjin docking complexes to analyze the dynamic behaviors and binding free energy at 100 ns time scale. In addition, frontier molecular orbitals (FMOs) and density-functional theory (DFT) were also investigated from computational quantum mechanism perspectives using the Avogadro-ORCA 1.2.0 platform. Karanjin complies with all five of Lipinski's drug-likeness rules with suitable ADMET profiles for therapeutic use. The docking scores (kcal/mol) showed comparatively higher potency against AD and PD associated targets than currently used standard drugs. Overall, the potential binding affinity from molecular docking, static thermodynamics feature from MD-simulation and other multiparametric drug-ability profiles suggest that karanjin could be considered as a suitable therapeutic lead for AD and PD treatment. Furthermore, the present results were strongly correlated with the earlier study on karanjin in an Alzheimer's animal model. However, necessary in vivo studies, clinical trials, bioavailability, permeability and safe dose administration, etc. must be required to use karanjin as a potential drug against AD and PD treatment, where the in silico results are more helpful to accelerate the drug development.

Keywords: ADMET; Alzheimer’s disease; Lipinski’s rule; Parkinson’s disease; bioinformatics; drug-likeness; in silico; karanjin; molecular dynamics.

MeSH terms

Alzheimer Disease* / drug therapy
Animals
Benzopyrans
Drug Design
Molecular Docking Simulation
Molecular Dynamics Simulation
Parkinson Disease* / drug therapy

Substances

Benzopyrans
karanjin

Grants and funding

The authors would like to thank the Ministry of Higher Education (MOHE) Malaysia for the support provided via the Fundamental Research Grant Scheme [Ref: FRGS/1/2020/SKK06/UNIKL/03/2].