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Rapid and Efficient Hydrophilicity Tuning of p53/mdm2 Antagonists

机译:快速有效地调节p53 / mdm2拮抗剂的亲水性

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摘要

The protein-protein interaction of p53 and mdm2 is an important anticancer target. The interface, however, is very hydrophobic and naturally results in very hydrophobic antagonists. We used the Orru three component reaction (O-3CR) along with a rapid and efficient, recently discovered amidation reaction to dramatically improve the water solubility of our recently discovered low molecular weight p53/mdm2 antagonists. Arrays of amides were synthesized with improved hydrophilicity and retainment and/or improvement of p53/mdm2 inhibitory activity.
机译:p53和mdm2的蛋白-蛋白相互作用是重要的抗癌靶标。但是,该界面非常疏水,自然会产生非常疏水的拮抗剂。我们将Orru三组分反应(O-3CR)与最近发现的快速有效酰胺化反应一起使用,以显着提高我们最近发现的低分子量p53 / mdm2拮抗剂的水溶性。合成了具有改善的亲水性和p53 / mdm2抑制活性的保留和/或改善的酰胺阵列。

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