Abstract
Molecular docking algorithms are used to seek the most active compounds from a pool of ligands. In principle, molecular dynamics (MD) simulations with accurate physical potentials and sampling could yield better enrichments, but they are computationally expensive. Here, we describe a method called MELD-Bracket that utilizes biased replica exchange ladders in MD in order to compete different ligands against each other within a fast bracket style "binding tournament". MELD-Bracket finds best-binders rapidly when ligands are well separated in their binding affinities.
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