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Merck

Combined Proteomic and In Silico Target Identification Reveal a Role for 5-Lipoxygenase in Developmental Signaling Pathways.

Cell chemical biology (2018-09-27)
Silke Brand, Sayantani Roy, Peter Schröder, Bernd Rathmer, Jessica Roos, Shobhna Kapoor, Sumersing Patil, Claudia Pommerenke, Thorsten Maier, Petra Janning, Sonja Eberth, Dieter Steinhilber, Dennis Schade, Gisbert Schneider, Kamal Kumar, Slava Ziegler, Herbert Waldmann
ABSTRAKT

Identification and validation of the targets of bioactive small molecules identified in cell-based screening is challenging and often meets with failure, calling for the development of new methodology. We demonstrate that a combination of chemical proteomics with in silico target prediction employing the SPiDER method may provide efficient guidance for target candidate selection and prioritization for experimental in-depth evaluation. We identify 5-lipoxygenase (5-LO) as the target of the Wnt pathway inhibitor Lipoxygenin. Lipoxygenin is a non-redox 5-LO inhibitor, modulates the β-catenin-5-LO complex and induces reduction of both β-catenin and 5-LO levels in the nucleus. Lipoxygenin and the structurally unrelated 5-LO inhibitor CJ-13,610 promote cardiac differentiation of human induced pluripotent stem cells and inhibit Hedgehog, TGF-β, BMP, and Activin A signaling, suggesting an unexpected and yet unknown role of 5-LO in these developmental pathways.

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