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Frontal Affinity Chromatography with MS Detection of EphB2 Tyrosine Kinase Receptor. 2. Identification of Small-Molecule Inhibitors via Coupling with Virtual Screening
Author(s) -
Leticia ToledoSherman,
Eugen Deretey,
Jacek J. SlonUsakiewicz,
William Ng,
JinRui Dai,
J. Estelle Foster,
Peter R. Redden,
Marni D. Uger,
Linda Liao,
Andrew Pasternak,
Neil Reid
Publication year - 2005
Publication title -
journal of medicinal chemistry
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.01
H-Index - 261
eISSN - 1520-4804
pISSN - 0022-2623
DOI - 10.1021/jm0492204
Subject(s) - pharmacophore , virtual screening , chemistry , drug discovery , docking (animal) , high throughput screening , computational biology , tyrosine kinase , receptor tyrosine kinase , small molecule , mass spectrometry , combinatorial chemistry , kinase , receptor , biochemistry , chromatography , medicine , nursing , biology
We have integrated two complementary methods, high-throughput virtual screening with a "high-content" wet screening technique based on frontal affinity chromatography with mass spectrometry detection (FAC-MS), for identification of hits against the erythropoietin-producing hepatocellular B2 (EphB2) receptor tyrosine kinase domain. Both an EphB2-directed virtual screen combining docking and scoring and a kinase-directed pharmacophore search strategy were used to identify a compound set enriched in bioactive compounds against EphB2. The coupling of virtual screening methodologies with FAC-MS is a unique hybrid approach that can be used to increase the efficacy of both hit discovery and optimization efforts in drug discovery and has successfully identified hits, in particular 19a (36% shift, IC(50) = 5.2 microM, K(d) = 3.3 microM), as inhibitors for EphB2, a potential cancer target.

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