| Literature DB >> 33669763 |
Serena Vittorio1, Rosaria Gitto1, Ilenia Adornato1, Emilio Russo2, Laura De Luca1.
Abstract
Computer aided drug-design methods proved to be powerful tools for the identification of new therapeutic agents. We employed a structure-based workflow to identify new inhibitors targeting mTOR kinase at rapamycin binding site. By combining molecular dynamics (MD) simulation and pharmacophore modelling, a simplified structure-based pharmacophore hypothesis was built starting from the FKBP12-rapamycin-FRB ternary complex retrieved from RCSB Protein Data Bank (PDB code 1FAP). Then, the obtained model was used as filter to screen the ZINC biogenic compounds library, containing molecules derived from natural sources or natural-inspired compounds. The resulting hits were clustered according to their similarity; moreover, compounds showing the highest pharmacophore fit-score were chosen from each cluster. The selected molecules were subjected to docking studies to clarify their putative binding mode. The binding free energy of the obtained complexes was calculated by MM/GBSA method and the hits characterized by the lowest ΔGbind values were identified as potential mTOR inhibitors. Furthermore, the stability of the resulting complexes was studied by means of MD simulation which revealed that the selected compounds were able to form a stable ternary complex with FKBP12 and FRB domain, thus underlining their potential ability to inhibit mTOR with a rapamycin-like mechanism.Entities:
Keywords: mTOR; molecular docking and structure-based virtual screening; molecular dynamics simulation; pharmacophore modeling; ternary complex FKBP12-rapamycin-FRB
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Year: 2021 PMID: 33669763 PMCID: PMC7922000 DOI: 10.3390/molecules26041103
Source DB: PubMed Journal: Molecules ISSN: 1420-3049 Impact factor: 4.411