Cyclohexane-1,3-dione Derivatives as Future Therapeutic Agents for NSCLC: QSAR Modeling, In Silico ADME-Tox Properties, and Structure-Based Drug Designing Approach.
Ossama DaouiSouad ElkhattabiMohamed BakhouchSalah BelaidiRichie R BhandareAfzal Basha ShaikSuraj Narayan MaliSamir ChtitaPublished in: ACS omega (2023)
The abnormal expression of the c-Met tyrosine kinase has been linked to the proliferation of several human cancer cell lines, including non-small-cell lung cancer (NSCLC). In this context, the identification of new c-Met inhibitors based on heterocyclic small molecules could pave the way for the development of a new cancer therapeutic pathway. Using multiple linear regression (MLR)-quantitative structure-activity relationship (QSAR) and artificial neural network (ANN)-QSAR modeling techniques, we look at the quantitative relationship between the biological inhibitory activity of 40 small molecules derived from cyclohexane-1,3-dione and their topological, physicochemical, and electronic properties against NSCLC cells. In this regard, screening methods based on QSAR modeling with density-functional theory (DFT) computations, in silico pharmacokinetic/pharmacodynamic (ADME-Tox) modeling, and molecular docking with molecular electrostatic potential (MEP) and molecular mechanics-generalized Born surface area (MM-GBSA) computations were used. Using physicochemical (stretch-bend, hydrogen bond acceptor, Connolly molecular area, polar surface area, total connectivity) and electronic (total energy, highest occupied molecular orbital (HOMO) and lowest unoccupied molecular orbital (LUMO) energy levels) molecular descriptors, compound 6d is identified as the optimal scaffold for drug design based on in silico screening tests. The computer-aided modeling developed in this study allowed us to design, optimize, and screen a new class of 36 small molecules based on cyclohexane-1,3-dione as potential c-Met inhibitors against NSCLC cell growth. The in silico rational drug design approach used in this study led to the identification of nine lead compounds for NSCLC therapy via c-Met protein targeting. Finally, the findings are validated using a 100 ns series of molecular dynamics simulations in an aqueous environment on c-Met free and complexed with samples of the proposed lead compounds and Foretinib drug.
Keyphrases
- molecular docking
- molecular dynamics simulations
- tyrosine kinase
- small cell lung cancer
- advanced non small cell lung cancer
- epidermal growth factor receptor
- density functional theory
- neural network
- endothelial cells
- papillary thyroid
- molecular dynamics
- squamous cell
- mesenchymal stem cells
- structure activity relationship
- squamous cell carcinoma
- ionic liquid
- human health
- brain metastases
- multiple sclerosis
- oxidative stress
- drug delivery
- bone marrow
- white matter
- drug induced
- signaling pathway
- cell death
- lymph node metastasis
- low birth weight
- pluripotent stem cells