AutoDockFR: Advances in Protein-Ligand Docking with Explicitly Specified Binding Site Flexibility

Pradeep Anand Ravindranath, Stefano Forli, David S Goodsell, Arthur J Olson and Michel F Sanner

PLOS Computational Biology, 2015, vol. 11, issue 12, 1-28

Abstract: Automated docking of drug-like molecules into receptors is an essential tool in structure-based drug design. While modeling receptor flexibility is important for correctly predicting ligand binding, it still remains challenging. This work focuses on an approach in which receptor flexibility is modeled by explicitly specifying a set of receptor side-chains a-priori. The challenges of this approach include the: 1) exponential growth of the search space, demanding more efficient search methods; and 2) increased number of false positives, calling for scoring functions tailored for flexible receptor docking. We present AutoDockFR–AutoDock for Flexible Receptors (ADFR), a new docking engine based on the AutoDock4 scoring function, which addresses the aforementioned challenges with a new Genetic Algorithm (GA) and customized scoring function. We validate ADFR using the Astex Diverse Set, demonstrating an increase in efficiency and reliability of its GA over the one implemented in AutoDock4. We demonstrate greatly increased success rates when cross-docking ligands into apo receptors that require side-chain conformational changes for ligand binding. These cross-docking experiments are based on two datasets: 1) SEQ17 –a receptor diversity set containing 17 pairs of apo-holo structures; and 2) CDK2 –a ligand diversity set composed of one CDK2 apo structure and 52 known bound inhibitors. We show that, when cross-docking ligands into the apo conformation of the receptors with up to 14 flexible side-chains, ADFR reports more correctly cross-docked ligands than AutoDock Vina on both datasets with solutions found for 70.6% vs. 35.3% systems on SEQ17, and 76.9% vs. 61.5% on CDK2. ADFR also outperforms AutoDock Vina in number of top ranking solutions on both datasets. Furthermore, we show that correctly docked CDK2 complexes re-create on average 79.8% of all pairwise atomic interactions between the ligand and moving receptor atoms in the holo complexes. Finally, we show that down-weighting the receptor internal energy improves the ranking of correctly docked poses and that runtime for AutoDockFR scales linearly when side-chain flexibility is added.Author Summary: Docking programs are widely used to identify drug-like molecules interacting with a given receptor to inhibit its function. Although receptors are known to change conformation upon ligand binding, most docking programs model small molecules as flexible while modeling receptors as rigid, thus limiting the range of therapeutic targets for which docking can be applied. Here we introduce a new docking program, AutoDockFR, which simulates partial receptor flexibility by allowing a large number of explicitly specified receptor side-chains to explore their conformational space, while searching for energetically favorable binding poses for a given ligand. We show that we achieve higher docking success rates by including receptor flexibility in the binding site of receptor conformations that are experimentally determined without the ligand present (i.e. apo conformations). Previous approaches based on the a-priori and explicit specification of the part of the receptor to be considered flexible, have so far been limited to a small number of flexible protein side-chains (2–5), thus requiring prior knowledge of receptor side-chains undergoing conformational change upon binding of a given ligand. The demonstrated ability of AutoDockFR in identifying correct solutions for problems with up to 14 flexible receptor side-chains lessens this requirement.

Date: 2015
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Persistent link: https://EconPapers.repec.org/RePEc:plo:pcbi00:1004586

DOI: 10.1371/journal.pcbi.1004586

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