AbstractStructure-based drug design requires the development of efficient computer programs for exploring the structural compatibility of various flexible ligands with a given receptor. While various algorithms are available for finding docked conformations, selecting a target function that can reliably score the conformations remains a serious problem. We show that the use of an empirical free energy evaluation method, originally developed to characterize protein-protein interactions, can substantially improve the efficacy of search algorithms. In addition to the molecular mechanics interaction energy, the function takes account of solvation and side chain conformational entropy, while remaining simple enough to replace the incomplete targ...
Binding affinity plays an important role in drug design. Accurate and fast prediction of binding fre...
Protein-ligand docking programs are widely used tools for computer-aided drug design. Many docking p...
The use of molecular simulation to estimate the strength of macromolecular binding free energies is ...
AbstractStructure-based drug design requires the development of efficient computer programs for expl...
AbstractBackground: An important prerequisite for computational structure-based drug design is predi...
Computational tools are useful for studying biological systems with an atomistic level of detail. Th...
A method is proposed for the estimation of absolute binding free energy of interaction between prote...
Structure-based drug design could benefit greatly from computational methodologies that accurately p...
Finding the orientation of a ligand (small molecule) with the lowest binding energy to the macromole...
Large-scale identification of native binding orientations is crucial for understanding the role of p...
Large-scale identification of native binding orientations is crucial for understanding the role of p...
<div><p>Large-scale identification of native binding orientations is crucial for understanding the r...
Copyright © 2015 Igor V. Oferkin et al.This is an open access article distributed under the Creative...
Finding the orientation of a ligand (small molecule) with the lowest binding energy to the macromole...
Molecular docking is a powerful tool used in drug discovery and structural biology for predicting th...
Binding affinity plays an important role in drug design. Accurate and fast prediction of binding fre...
Protein-ligand docking programs are widely used tools for computer-aided drug design. Many docking p...
The use of molecular simulation to estimate the strength of macromolecular binding free energies is ...
AbstractStructure-based drug design requires the development of efficient computer programs for expl...
AbstractBackground: An important prerequisite for computational structure-based drug design is predi...
Computational tools are useful for studying biological systems with an atomistic level of detail. Th...
A method is proposed for the estimation of absolute binding free energy of interaction between prote...
Structure-based drug design could benefit greatly from computational methodologies that accurately p...
Finding the orientation of a ligand (small molecule) with the lowest binding energy to the macromole...
Large-scale identification of native binding orientations is crucial for understanding the role of p...
Large-scale identification of native binding orientations is crucial for understanding the role of p...
<div><p>Large-scale identification of native binding orientations is crucial for understanding the r...
Copyright © 2015 Igor V. Oferkin et al.This is an open access article distributed under the Creative...
Finding the orientation of a ligand (small molecule) with the lowest binding energy to the macromole...
Molecular docking is a powerful tool used in drug discovery and structural biology for predicting th...
Binding affinity plays an important role in drug design. Accurate and fast prediction of binding fre...
Protein-ligand docking programs are widely used tools for computer-aided drug design. Many docking p...
The use of molecular simulation to estimate the strength of macromolecular binding free energies is ...