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Summary form only given. Few methods use molecular dynamics simulations based on atomically detailed force fields to study the protein-ligand docking process because they are considered too time demanding despite their accuracy. We present a docking algorithm based on molecular dynamics simulations which has a highly flexible computational granularity. We compare the accuracy and the time required with well-known, commonly used docking methods like AutoDock, DOCK, FlexX, ICM, and GOLD. We show that our algorithm is accurate, fast and, because of its flexibility, applicable even to loosely coupled distributed systems like desktop grids for docking.
Date of Conference: 26-30 April 2004