Rational design and synthesis of 1,5-disubstituted tetrazoles as potent inhibitors of the MDM2-p53 interaction
- Surmiak, Ewa
- Neochoritis, Constantinos G
- Musielak, Bogdan
- Twarda-Clapa, Aleksandra
- Kurpiewska, Katarzyna
- Dubin, Grzegorz
- Camacho, Carlos
- Holak, Tad A
- Dömling, Alexander
DOIAbstract
Using the computational pharmacophore-based ANCHOR.QUERY platform a new scaffold was discovered. Potent compounds evolved inhibiting the protein-protein interaction p53-MDM2. An extensive SAR study was performed based on our four-point pharmacophore model, yielding derivatives with affinity to MDM2 in the nanomolar range. Their binding affinity with MDM2 was evaluated using both fluorescence polarization (FP) assay and 2D-NMR-HSQC experiments.</p
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