Structure-based design of potent non-peptide MDM2 inhibitors |
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| Authors: | Ding Ke Lu Yipin Nikolovska-Coleska Zaneta Qiu Su Ding Yousong Gao Wei Stuckey Jeanne Krajewski Krzysztof Roller Peter P Tomita York Parrish Damon A Deschamps Jeffrey R Wang Shaomeng |
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| Affiliation: | Departments of Internal Medicine and Medicinal Chemistry and Comprehensive Cancer Center, and Life Sciences Institute, University of Michigan, 1500 East Medical Center Drive, Ann Arbor, Michigan 48109, USA. |
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| Abstract: | A successful structure-based design of a class of non-peptide small-molecule MDM2 inhibitors targeting the p53-MDM2 protein-protein interaction is reported. The most potent compound 1d binds to MDM2 protein with a Ki value of 86 nM and is 18 times more potent than a natural p53 peptide (residues 16-27). Compound 1d is potent in inhibition of cell growth in LNCaP prostate cancer cells with wild-type p53 and shows only a weak activity in PC-3 prostate cancer cells with a deleted p53. Importantly, 1d has a minimal toxicity to normal prostate epithelial cells. Our studies provide a convincing example that structure-based strategy can be employed to design highly potent, non-peptide, cell-permeable, small-molecule inhibitors to target protein-protein interaction, which remains a very challenging area in chemical biology and drug design. |
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