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首页> 外文期刊>Journal of Medicinal Chemistry >Discovery of 4,7-Diamino-5-(4-phenoxyphenyl)-6-methylene-pyrinnido5,4-bpyrrolizines as Novel Bruton's Tyrosine Kinase Inhibitors
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Discovery of 4,7-Diamino-5-(4-phenoxyphenyl)-6-methylene-pyrinnido5,4-bpyrrolizines as Novel Bruton's Tyrosine Kinase Inhibitors

机译:4,7-二氨基-5-(4-苯氧基苯基)-6-亚甲基吡啶并5,4-b吡咯嗪作为新型布鲁顿酪氨酸激酶抑制剂的发现

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摘要

An alternative medicinal chemistry approach was conducted on Bruton's tyrosine kinase (BTK) inhibitor 1 (ibrutinib) by merging the pyrazolo3,4-dpyrimidine component into a tricyclic skeleton. Two types of compounds were prepared, and their biochemical activities on BTK as well as stereochemistry effects were determined. Structural optimization focusing on the reactive binding group to BTK Cys481 and on the metabolic site guided by metabolic study were conducted. 7S was identified as the most potent showing an IC50 value of 0.4 nM against BTK and 16 nM against BTK-dependent TMD8 cells. Compared to 1, 7S was slightly more selective with strong inhibition on the B-cell receptor signaling pathway. In a TMD8 cell derived animal xenograft model, 7S showed a relative tumor volume of 5.3 at 15 mg/kg QD dosage that was more efficacious than 1 (RTV 6.6) at a higher dose of 25 mg/kg QD. All these results suggest 7S as a new BTK inhibitor worthy of further profiling.
机译:通过将吡唑并[3,4-d]嘧啶组分合并到三环骨架中,对布鲁顿酪氨酸激酶 (BTK) 抑制剂 1 (伊布替尼)进行了另一种药物化学方法。制备了2种化合物,并确定了它们对BTK的生化活性和立体化学效应。在代谢研究的指导下,对BTK Cys481的反应性结合基团和代谢位点进行了结构优化。7S 被确定为最有效的,对 BTK 的 IC50 值为 0.4 nM,对 BTK 依赖性 TMD8 细胞的 IC50 值为 16 nM。与1相比,7S的选择性略高,对B细胞受体信号通路有较强的抑制作用。在 TMD8 细胞衍生的动物异种移植模型中,7S 在 15 mg/kg QD 剂量下显示相对肿瘤体积为 5.3,比 25 mg/kg QD 较高剂量下的 1 (RTV 6.6) 更有效。所有这些结果都表明,7S是一种新的BTK抑制剂,值得进一步分析。

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