Insight into crystal structures and identification of potential styrylthieno[2,3- b ]pyridine-2-carboxamidederivatives against COVID-19 Mpro through structure-guided modeling and simulation approach.
Youness El BakriBasharat AhmadKandasamy SaravananIqrar Ahmad AnsariEtify A BakhiteOsama YounisSafiyyah A H Al-WaleedyOmaima F IbrahimAyman NafadyJoel T MagueShaaban K MohamedPublished in: Journal of biomolecular structure & dynamics (2023)
Anti-SARS-CoV-2 drugs are urgently needed to prevent the pandemic and for immunization. Their protease inhibitor treatment for COVID-19 has been used in clinical trials. In Calu-3 and THP1 cells, 3CL SARS-CoV-2 Mpro protease is required for viral expression, replication, and the activation of the cytokines IL-1, IL-6, and TNF-. The Mpro structure was chosen for this investigation because of its activity as a chymotrypsin-like enzyme and the presence of a cysteine-containing catalytic domain. Thienopyridine derivatives increase the release of nitric oxide from coronary endothelial cells, which is an important cell signaling molecule with antibacterial activity against bacteria, protozoa, and some viruses. Using DFT calculations, global descriptors are computed from HOMO-LUMO orbitals; the molecular reactivity sites are analyzed from an electrostatic potential map. NLO properties are calculated, and topological analysis is also part of the QTAIM studies. Both compounds 1 and 2 were designed from the precursor molecule pyrimidine and exhibited binding energies (-14.6708 kcal/mol and -16.4521 kcal/mol). The binding mechanisms of molecule 1 towards SARS-COV-2 3CL Mpro exhibited strong hydrogen bonding as well as Vdw interaction. In contrast, derivative 2 was bound to the active site protein's active studied that several residues and positions, including (His41, Cys44, Asp48, Met49, Pro52, Tyr54, Phe140, Leu141, Ser144, His163, Ser144, Cys145, His164, Met165, Glu166, Leu167, Asp187, Gln189, Thr190, and GLn192) are critical for the maintenance of inhibitors inside the active pocket. Molecular docking and 100 ns MD simulation analysis revealed that Both compounds 1 and 2 with higher binding affinity and stability toward the SARS-COV-2 3CL Mpro protein. Binding free energy calculations and other MD parameters support the finding.Communicated by Ramaswamy H. Sarma.
Keyphrases
- sars cov
- density functional theory
- molecular docking
- molecular dynamics simulations
- molecular dynamics
- binding protein
- respiratory syndrome coronavirus
- nitric oxide
- clinical trial
- endothelial cells
- dna binding
- poor prognosis
- magnetic resonance
- single cell
- coronary artery
- induced apoptosis
- coronavirus disease
- long non coding rna
- coronary artery disease
- heart failure
- oxidative stress
- protein protein
- drug induced
- randomized controlled trial
- zika virus
- small molecule
- cell death
- endoplasmic reticulum stress
- monte carlo
- risk assessment
- cell proliferation
- climate change
- combination therapy
- aortic stenosis
- silver nanoparticles
- water soluble
- fluorescent probe
- replacement therapy
- bone marrow