Abstract
We explore the ability of four quantum mechanical (QM)/molecular mechanical (MM) models to accurately identify the native pose of six HIV-1 protease inhibitors and compare them with the AMBER force field and ChemScore and GoldScore scoring functions. Three QM/MM scoring functions treated the ligand at the HF/6-31G*, AM1d, and PM3 levels; the fourth QM/MM function modeled the ligand and active site at the PM3-D level. For the discrimination of native from non-native poses, solvent-corrected HF/6-31G*: AMBER and AMBER functions exhibited the best overall performance. While the electrostatic component of the MM and QM/MM functions appears important for discriminating the native pose of the ligand, the polarization contribution in the QM/MM functions was relatively insensitive to a ligand's binding mode and, for one ligand, actually hindered discrimination. The inclusion of a desolvation penalty, here using a generalized Born solvent model, improved discrimination for the MM and QM/MM methods. There appeared to be no advantage to binding mode prediction by incorporating active site polarization at the PM3-D level. Finally, we found that choice of the protonation state of the aspartyl dyad in the HIV-1 protease active site influenced the ability of scoring methods to determine the native binding pose. © 2009 American Chemical Society.
Original language | English |
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Pages (from-to) | 913-924 |
Number of pages | 11 |
Journal | Journal of Chemical Information and Modeling |
Volume | 49 |
Issue number | 4 |
DOIs | |
Publication status | Published - 27 Apr 2009 |
Keywords
- generalized born model
- ligand interactions
- binding-affinity
- flexible docking
- md simulation
- active-site
- force-field
- inhibitors
- complexes
- proteins