摘要
The success of a structure-based drug is highly dependent on a known binding pose of the protein-ligand system. However, this is not always available. In this study, we set out to explore the applicability of the popular and easy-to-use MD-based MM/GBSA method to determine the binding poses of known FGFR inhibitors. It was found that MM/GBSA combined with 100 ns of MD simulation significantly improved the success rate of docking methods from 30-40% to 70%. This work demonstrates a way that the MM/GBSA method can be more accurate than it is in ligand ranking, filling a gap in structure-based drug discovery when the binding pose is unknown.
原文 | English |
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頁(從 - 到) | 9656-9663 |
頁數 | 8 |
期刊 | Physical Chemistry Chemical Physics |
卷 | 22 |
發行號 | 17 |
DOIs | |
出版狀態 | Published - 7 5月 2020 |