A family competition evolutionary algorithm for automated docking of flexible ligands to proteins

## Abstract An improved version of the fragment‐based flexible ligand docking approach SEED–FFLD is tested on inhibitors of human immunodeficiency virus type 1 protease, human α‐thrombin and the estrogen receptor β. The docking results indicate that it is possible to correctly reproduce the binding

We have developed a generic evolutionary method with an empirical scoring function for the protein-ligand docking, which is a problem of paramount importance in structure-based drug design. This approach, referred to as the GEMDOCK (Generic Evolutionary Method for molecular DOCKing), combines both c

## Abstract We have developed a new docking method to consider receptor flexibility, a hybrid method of molecular dynamics and harmonic dynamics. The global motions of the whole receptor were approximately introduced into those of the receptor in the docking simulation as harmonic dynamics. On the