In recent years, protein-ligand docking has become a powerful tool for drug development. Although several approaches suitable for high throughput screening are available, there is a need for methods able to identify binding modes with high accuracy. This accuracy is essential to reliably compute the binding free energy of the ligand. Such methods are needed when the binding mode of lead compounds is not determined experimentally but is needed for structure-based lead optimization. We present here a new docking software, called EADock, that aims at this goal. It uses an hybrid evolutionary algorithm with two fitness functions, in combination with a sophisticated management of the diversity. EADock is interfaced with the CHARMM package for en...
Abstract: The prediction of binding modes (BMs) occurring between a small molecule and a target prot...
Protein-ligand docking is to predict the location and orientation of a ligand with respect to a prot...
The prediction of a protein-ligand interaction when the interaction site is known is a relatively si...
Abstract: We have developed a generic evolutionary method with an empirical scoring function for the...
Molecular docking softwares are one of the important tools of modern drug development pipelines. The...
ABSTRACT We have developed an evolution-ary approach for flexible ligand docking. This ap-proval, GE...
Ligand docking is the computational prediction of the bound conformation of a small molecule in a co...
We have developed a new docking method, Pose-Sensitive Inclined (PSI)-DOCK, for flexible ligand dock...
Molecular docking is a computational approach for predicting the most probable position of ligands i...
Structure-based molecular docking and ligand-based similarity search are two commonly used computati...
Protein-ligand docking programs are widely used tools for computer-aided drug design. Many docking p...
AbstractBackground: Molecular docking seeks to predict the geometry and affinity of the binding of a...
AbstractBackground: An important prerequisite for computational structure-based drug design is predi...
Ligand-protein docking is an optimization problem based on predicting the position of a ligand with ...
Recent years have witnessed rapid developments of computer-aided drug design methods, which have rea...
Abstract: The prediction of binding modes (BMs) occurring between a small molecule and a target prot...
Protein-ligand docking is to predict the location and orientation of a ligand with respect to a prot...
The prediction of a protein-ligand interaction when the interaction site is known is a relatively si...
Abstract: We have developed a generic evolutionary method with an empirical scoring function for the...
Molecular docking softwares are one of the important tools of modern drug development pipelines. The...
ABSTRACT We have developed an evolution-ary approach for flexible ligand docking. This ap-proval, GE...
Ligand docking is the computational prediction of the bound conformation of a small molecule in a co...
We have developed a new docking method, Pose-Sensitive Inclined (PSI)-DOCK, for flexible ligand dock...
Molecular docking is a computational approach for predicting the most probable position of ligands i...
Structure-based molecular docking and ligand-based similarity search are two commonly used computati...
Protein-ligand docking programs are widely used tools for computer-aided drug design. Many docking p...
AbstractBackground: Molecular docking seeks to predict the geometry and affinity of the binding of a...
AbstractBackground: An important prerequisite for computational structure-based drug design is predi...
Ligand-protein docking is an optimization problem based on predicting the position of a ligand with ...
Recent years have witnessed rapid developments of computer-aided drug design methods, which have rea...
Abstract: The prediction of binding modes (BMs) occurring between a small molecule and a target prot...
Protein-ligand docking is to predict the location and orientation of a ligand with respect to a prot...
The prediction of a protein-ligand interaction when the interaction site is known is a relatively si...