PRO_SELECT: Combining Structure-Based Drug Design and Array-Based Chemistry for Rapid Lead Discovery. 2. The Development of a Series of Highly Potent and Selective Factor Xa Inhibitors - Concepedia

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PRO_SELECT: Combining Structure-Based Drug Design and Array-Based Chemistry for Rapid Lead Discovery. 2. The Development of a Series of Highly Potent and Selective Factor Xa Inhibitors

DOI Full Paper Access

85

Citations

17

References

2002

Year

John W. Liebeschuetz, Stuart Jones, Phillip J. Morgan, Christopher W. Murray, Andrew D. Rimmer, Jonathan M. E. Roscoe, Bohdan Waszkowycz, Pauline M. Welsh, William A. Wylie, Stephen Young,

Journal of Medicinal Chemistry

Drug TargetHit IdentificationBiomolecular Structure PredictionMolecular BiologyLead IdentificationChemical BiologyMedicinal ChemistryRapid Lead DiscoveryDrug DesignHighly PotentOther Serine ProteasesProteomicsTargeted LibraryVirtual ScreeningBiochemistryArray-based ChemistryProtein ModelingProtein Structure PredictionDrug DevelopmentPharmacologyMolecular ModelingProtein Active SiteNatural SciencesRational Drug DesignProtein EngineeringMedicineDrug Discovery

Abstract

In silico screening of combinatorial libraries prior to synthesis promises to be a valuable aid to lead discovery. PRO_SELECT, a tool for the virtual screening of libraries for fit to a protein active site, has been used to find novel leads against the serine protease factor Xa. A small seed template was built upon using three iterations of library design, virtual screening, synthesis, and biological testing. Highly potent molecules with selectivity for factor Xa over other serine proteases were rapidly obtained.

References

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