Extracting binding energies and binding modes from biomolecular simulations of fragment binding to endothiapepsin

Abstract: Fragment‐based drug discovery (FBDD) aims to discover a set of small binding fragments that may be subsequently linked together. Therefore, in‐depth knowledge of the individual fragments' structural and energetic binding properties is essential. In addition to experimental techniques, the direct simulation of fragment binding by molecular dynamics (MD) simulations became popular to characterize fragment binding. However, former studies showed that long simulation times and high computational demands per fragme… Show more