Integrated Machine Learning and Chemoinformatics-Based Screening of Mycotic Compounds against Kinesin Spindle ProteinEg5 for Lung Cancer Therapy
Priyanka Maiti,
Priyanka Sharma,
Mahesha Nand,
Indra D. Bhatt,
Muthannan Andavar Ramakrishnan,
Shalini Mathpal,
Tushar Joshi,
Ragini Pant,
Shafi Mahmud,
Jesus Simal-Gandara,
Sultan Alshehri,
Mohammed M. Ghoneim,
Maha Alruwaily,
Ahmed Abdullah Al Awadh,
Mohammed Merae Alshahrani,
Subhash Chandra
Affiliations
Priyanka Maiti
Centre for Environmental Assessment and Climate Change, G.B. Pant National Institute of Himalayan Environment (GBP-NIHE), Kosi-Katarmal, Almora 263643, Uttarakhand, India
Priyanka Sharma
Department of Botany, DSB Campus, Kumaun University, Nainital 263002, Uttarakhand, India
Mahesha Nand
ENVIS Centre on Himalayan Ecology, G.B. Pant National Institute of Himalayan Environment (GBP-NIHE), Kosi-Katarmal, Almora 263643, Uttarakhand, India
Indra D. Bhatt
Centre for Biodiversity Conservation and Management, G.B. Pant National Institute of Himalayan Environment (GBP-NIHE), Kosi-Katarmal, Almora 263643, Uttarakhand, India
Muthannan Andavar Ramakrishnan
ICAR-Indian Veterinary Research Institute, Bengaluru 560024, Karnataka, India
Shalini Mathpal
Department of Biotechnology, Bhimtal Campus, Kumaun University, Nainital 263136, Uttarakhand, India
Tushar Joshi
Department of Biotechnology, Bhimtal Campus, Kumaun University, Nainital 263136, Uttarakhand, India
Ragini Pant
Department of Biotechnology, Bhimtal Campus, Kumaun University, Nainital 263136, Uttarakhand, India
Shafi Mahmud
Genetic Engineering and Biotechnology, University of Rajshahi, Rajshahi 6205, Bangladesh
Jesus Simal-Gandara
Nutrition and Bromatology Group, Department of Analytical Chemistry and Food Science, Faculty of Science, Universidade de Vigo, E-32004 Ourense, Spain
Sultan Alshehri
Department of Pharamaceutics, College of Pharmacy, King Saud University, Riyadh 11451, Saudi Arabia
Mohammed M. Ghoneim
Department of Pharmacy Practice, College of Pharamcy, AlMaarefa University, Ad Diriyah 13713, Saudi Arabia
Maha Alruwaily
Department of Pharmacy Practice, College of Pharamcy, AlMaarefa University, Ad Diriyah 13713, Saudi Arabia
Ahmed Abdullah Al Awadh
Department of Clinical Laboratory Science, Faculty of Applied Medical Science, Najran University, Najran 61441, Saudi Arabia
Mohammed Merae Alshahrani
Department of Clinical Laboratory Science, Faculty of Applied Medical Science, Najran University, Najran 61441, Saudi Arabia
Subhash Chandra
Department of Botany, Soban Singh Jeena University, Almora 263601, Uttarakhand, India
Among the various types of cancer, lung cancer is the second most-diagnosed cancer worldwide. The kinesin spindle protein, Eg5, is a vital protein behind bipolar mitotic spindle establishment and maintenance during mitosis. Eg5 has been reported to contribute to cancer cell migration and angiogenesis impairment and has no role in resting, non-dividing cells. Thus, it could be considered as a vital target against several cancers, such as renal cancer, lung cancer, urothelial carcinoma, prostate cancer, squamous cell carcinoma, etc. In recent years, fungal secondary metabolites from the Indian Himalayan Region (IHR) have been identified as an important lead source in the drug development pipeline. Therefore, the present study aims to identify potential mycotic secondary metabolites against the Eg5 protein by applying integrated machine learning, chemoinformatics based in silico-screening methods and molecular dynamic simulation targeting lung cancer. Initially, a library of 1830 mycotic secondary metabolites was screened by a predictive machine-learning model developed based on the random forest algorithm with high sensitivity (1) and an ROC area of 0.99. Further, 319 out of 1830 compounds screened with active potential by the model were evaluated for their drug-likeness properties by applying four filters simultaneously, viz., Lipinski’s rule, CMC-50 like rule, Veber rule, and Ghose filter. A total of 13 compounds passed from all the above filters were considered for molecular docking, functional group analysis, and cell line cytotoxicity prediction. Finally, four hit mycotic secondary metabolites found in fungi from the IHR were screened viz., (−)-Cochlactone-A, Phelligridin C, Sterenin E, and Cyathusal A. All compounds have efficient binding potential with Eg5, containing functional groups like aromatic rings, rings, carboxylic acid esters, and carbonyl and with cell line cytotoxicity against lung cancer cell lines, namely, MCF-7, NCI-H226, NCI-H522, A549, and NCI H187. Further, the molecular dynamics simulation study confirms the docked complex rigidity and stability by exploring root mean square deviations, root mean square fluctuations, and radius of gyration analysis from 100 ns simulation trajectories. The screened compounds could be used further to develop effective drugs against lung and other types of cancer.
