Flaviviral protease inhibitors identified by fragment-based library docking into a structure generated by molecular dynamics

Dariusz Ekonomiuk, Xun Cheng Su, Kiyoshi Ozawa, Christophe Bodenreider, Pheng Lim Siew, Gottfried Otting, Danzhi Huang*, Amedeo Caflisch

*Corresponding author for this work

    Research output: Contribution to journalArticlepeer-review

    69 Citations (Scopus)

    Abstract

    Fragment-based docking was used to select a conformation for virtual screening from a molecular dynamics trajectory of the West Nile virus nonstructural 3 protease. This conformation was chosen from an ensemble of 100 molecular dynamics snapshots because it optimally accommodates benzene, the most common ring in known drugs, and two positively charged fragments (methylguanidinium and 2-phenylimidazoline). The latter fragments were used as probes because of the large number of hydrogen bond acceptors in the substrate binding site of the protease. Upon high-throughput docking of a diversity set of 18 694 molecules and pose filtering, only five compounds were chosen for experimental validation, and two of them are active in the low micromolar range in an enzymatic assay and a tryptophan fluorescence quenching assay. Evidence for specific binding to the protease active site is provided by nuclear magnetic resonance spectroscopy. The two inhibitors have different scaffolds (diphenylurea and diphenyl ester) and are promising lead candidates because they have amolecular weight of about 300 Da.

    Original languageEnglish
    Pages (from-to)4860-4868
    Number of pages9
    JournalJournal of Medicinal Chemistry
    Volume52
    Issue number15
    DOIs
    Publication statusPublished - 13 Aug 2009

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