Graphene oxide and flavonoids as potential inhibitors of the spike protein of SARS-CoV-2 variants and interaction between ligands: a parallel study of molecular docking and DFT.
Júlia Vaz SchultzMariana Zancan TonelMirkos Ortiz MartinsSolange Binotto FaganPublished in: Structural chemistry (2023)
Nanocarriers allow the connection between biomolecules and other structures to enhance the treatment efficacy, through the biomolecule's properties to an existing drug, or to allow a better and specific delivery. Apigenin and orientin are biomolecules with excellent therapeutic properties that are proposed in the fight against COVID-19. Besides that, graphene oxide is a nanomaterial that exhibits antiviral activity and is used as a nanocarrier of several drugs. We evaluated in this work, through molecular docking, the binding affinity between these structures to the receptor-binding domain of spike protein of two coronavirus variants, Delta and Omicron. The results indicate that all the structures exhibit affinity with the two protein targets, with binding affinity values of -11.88 to -6.65 kcal/mol for the Delta variant and values of -9.58 to -13.20 kcal/mol for the Omicron variant, which is a successful value as found in the literature as a potential inhibitor of SARS-CoV-2 infection. Also, through first-principles calculations based on Density Functional Theory, the interaction of graphene oxide with the biomolecules apigenin and orientin occurred. The results exhibit weak binding energy, which indicates that physical adsorption occurs, with better results when the biomolecule is set in parallel to the nanomaterial due to attractive π-π staking. These results are conducive to the development of a nanocarrier.
Keyphrases
- molecular docking
- sars cov
- density functional theory
- binding protein
- molecular dynamics simulations
- drug delivery
- respiratory syndrome coronavirus
- molecular dynamics
- high resolution
- coronavirus disease
- dna binding
- copy number
- systematic review
- physical activity
- mental health
- emergency department
- mass spectrometry
- human health
- capillary electrophoresis
- transcription factor
- aqueous solution
- drug release