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In vivo modulation of hypoxia-inducible signaling by topographical helix mimetics

机译:地形螺旋模拟物对缺氧诱导信号的体内调节

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摘要

Development of small-molecule inhibitors of protein–protein interactions is a fundamental challenge at the interface of chemistry and cancer biology. Successful methods for design of protein–protein interaction inhibitors include computational and experimental high-throughput and fragment-based screening strategies to locate small-molecule fragments that bind protein surfaces. An alternative rational design approach seeks to mimic the orientation and disposition of critical binding residues at protein interfaces. We describe the design, synthesis, biochemical, and in vivo evaluation of a small-molecule scaffold that captures the topography of α-helices. We designed mimics of a key α-helical domain at the interface of hypoxia-inducible factor 1α and p300 to develop inhibitors of hypoxia-inducible signaling. The hypoxia-inducible factor/p300 interaction regulates the transcription of key genes, whose expression contributes to angiogenesis, metastasis, and altered energy metabolism in cancer. The designed compounds target the desired protein with high affinity and in a predetermined manner, with the optimal ligand providing effective reduction of tumor burden in experimental animal models.
机译:蛋白质与蛋白质相互作用的小分子抑制剂的开发是化学和癌症生物学界的一项基本挑战。设计蛋白质-蛋白质相互作用抑制剂的成功方法包括计算和实验高通量和基于片段的筛选策略,以定位结合蛋白质表面的小分子片段。另一种合理的设计方法试图模仿蛋白质界面上关键结合残基的方向和位置。我们描述了捕获α-螺旋形貌的小分子支架的设计,合成,生化和体内评估。我们设计了缺氧诱导因子1α和p300界面上的关键α-螺旋结构域的模拟物,以开发低氧诱导信号的抑制剂。缺氧诱导因子/ p300相互作用调节关键基因的转录,关键基因的表达有助于血管生成,转移和改变能量代谢的癌症。设计的化合物以预定的方式高亲和力靶向所需蛋白质,最佳配体可有效降低实验动物模型中的肿瘤负荷。

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