Small-molecule inhibitors of the PDZ domain of Dishevelled proteins interrupt Wnt signalling
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Published:2021-06-02
Issue:1
Volume:2
Page:355-374
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ISSN:2699-0016
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Container-title:Magnetic Resonance
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language:en
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Short-container-title:Magn. Reson.
Author:
Kamdem Nestor, Roske YvetteORCID, Kovalskyy DmytroORCID, Platonov Maxim O., Balinskyi Oleksii, Kreuchwig Annika, Saupe Jörn, Fang Liang, Diehl Anne, Schmieder Peter, Krause Gerd, Rademann Jörg, Heinemann UdoORCID, Birchmeier Walter, Oschkinat HartmutORCID
Abstract
Abstract. Dishevelled (Dvl) proteins are important regulators of the Wnt signalling
pathway, interacting through their PDZ domains with the Wnt receptor
Frizzled. Blocking the Dvl PDZ–Frizzled interaction represents a potential
approach for cancer treatment, which stimulated the identification of small-molecule inhibitors, among them the anti-inflammatory drug Sulindac and
Ky-02327. Aiming to develop tighter binding compounds without side effects,
we investigated structure–activity relationships of sulfonamides. X-ray
crystallography showed high complementarity of anthranilic acid derivatives
in the GLGF loop cavity and space for ligand growth towards the PDZ surface. Our best binding compound inhibits Wnt signalling in a dose-dependent manner as demonstrated by TOP-GFP assays (IC50∼50 µM) and Western blotting of β-catenin levels. Real-time PCR showed reduction in the expression of Wnt-specific genes. Our compound interacted with Dvl-1 PDZ (KD=2.4 µM) stronger than Ky-02327 and may be developed into a lead compound interfering with the Wnt pathway.
Funder
Horizon 2020 Deutsche Forschungsgemeinschaft
Publisher
Copernicus GmbH
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