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首页> 外文期刊>Journal of Medicinal Chemistry >Tricyclic series of heat shock protein 90 (HSP90) inhibitors part I: Discovery of tricyclic imidazo[4,5-c]pyridines as potent inhibitors of the hsp90 molecular chaperone
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Tricyclic series of heat shock protein 90 (HSP90) inhibitors part I: Discovery of tricyclic imidazo[4,5-c]pyridines as potent inhibitors of the hsp90 molecular chaperone

机译:三环系列热休克蛋白90(HSP90)抑制剂第I部分:发现三环咪唑并[4,5-c]吡啶类化合物作为hsp90分子伴侣的有效抑制剂

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摘要

A novel class of heat shock protein 90 (Hsp90) inhibitors was developed after a low throughput screen (LTS) of a focused library containing approximately 21K compounds selected by virtual screening. The initial [1-{3-H-imidazo[4-5-c]pyridin-2-yl}-3,4-dihydro-2H-pyrido[2,1-a]isoindole-6-one] (1) compound showed moderate activity (IC_(50) = 7.6 μM on Hsp82, the yeast homologue of Hsp90). A high-resolution X-ray structure shows that compound 1 binds into an "induced" hydrophobic pocket, 10-15 ? away from the ATP/resorcinol binding site. Iterative cycles of structure-based drug design (SBDD) and chemical synthesis led to the design and preparation of analogues with improved affinity. These optimized molecules make productive interactions within the ATP binding site as reported by other Hsp90 inhibitors. This resulted in compound 8, which is a highly potent inhibitor in biochemical and cellular assays (K_d = 0.35 nM on Hsp90; IC_(50) = 30 nM on SKBr3 mammary carcinoma cells) and in an in vivo leukemia model.
机译:在聚焦库的低通量筛选(LTS)之后,开发了一种新型的热休克蛋白90(Hsp90)抑制剂,该库包含通过虚拟筛选选择的约21K化合物。初始[1- {3-H-咪唑并[4-5-c]吡啶-2-基} -3,4-二氢-2H-吡啶[2,1-a]异吲哚-6-一](1)该化合物显示中等活性(对Hsp90的酵母同源物Hsp82的IC_(50)= 7.6μM)。高分辨率的X射线结构表明,化合物1结合在“诱导的”疏水口袋中10-15?远离ATP /间苯二酚结合位点。基于结构的药物设计(SBDD)和化学合成的反复循环导致设计和制备具有改进亲和力的类似物。如其他Hsp90抑制剂所报道的,这些优化的分子在ATP结合位点内产生了有效的相互作用。这产生了化合物8,其在生物化学和细胞测定中是高效抑制剂(在Hsp90上K_d = 0.35 nM;在SKBr3乳腺癌细胞上IC_(50)= 30 nM)和体内白血病模型中。

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