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Tankyrase enzymes (TNKS) belonging to the poly(ADP-ribose) polymerase (PARP) superfamily are a promising target in the search for potential anti-cancer agents. Using the molecular docking and machine learning-based virtual screening techniques combined with the physico-chemical and ADMET profile prediction as well as molecular dynamics simulations, we have identified a number of candidate compounds in a subset of the ZINC database. Out of seven compounds biologically evaluated in vitro for their inhibition of the TNKS2 enzyme using immunochemical assay, one compound has shown good inhibitory activity with IC50 value less than 10 nM. Relatively simple scores based on molecular docking or MM-PBSA methods proved unsuitable for predicting the effect of structural modification or for accurate ranking of the compounds based on their binding energies. On the other hand, the molecular dynamics simulations and Free Energy Perturbation (FEP) calculations allowed us to further decipher the structure-activity relationships and retrospectively analyze the docking-based virtual screening performance. This approach can be applied at the subsequent lead optimization stages.
№ | Имя | Описание | Имя файла | Размер | Добавлен |
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1. | Полный текст | MedChemRussia2021_Radchenko70.pdf | 10,5 МБ | 27 января 2023 [genie@qsar.chem.msu.ru] |