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Characterization of novel checkpoint kinase 1 inhibitors by in vitro assays and in human cancer cells treated with topoisomerase inhibitors.

机译:通过体外测定和拓扑异构酶抑制剂处理的人类癌细胞中新型检查点激酶1抑制剂的表征。

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AIMS: We have developed biochemical and cell based assays to characterize small therapeutic molecules that inhibit the DNA damage checkpoint enzyme, Chk1 (Checkpoint kinase 1). MAIN METHODS: To prepare a screen of large chemical libraries, we purified the full-length and the catalytic domain versions of human Chk1. We characterized their properties and then selected full-length Chk1 as the variant most suitable for screening. We then identified and characterized structurally different Chk1 inhibitors in cell based-assays by measuring cytotoxicity and checkpoint bypass activity. KEY FINDINGS: We treated human cells with topoisomerase I inhibitors and demonstrated that at the time of Chk1 inhibitor addition, the cells have damaged DNA and activated Chk1. One Chk1 inhibitor, the indolocarbazole S27888, was active in the checkpoint bypass assay. SIGNIFICANCE: Knowing that the protein kinase inhibitory properties are different for each inhibitor, it seems that only a limited range of inhibitory activity is tolerated by cells. Chk1 has an essential role in determining how cancer cells respond to genotoxic treatments, therefore, inhibitors of this protein kinase are of great medical interest.
机译:目的:我们已经开发出基于生物化学和细胞的检测方法,以鉴定抑制DNA损伤检查点酶Chk1(检查点激酶1)的小型治疗性分子。主要方法:为了准备大型化学文库的筛选,我们纯化了人类Chk1的全长和催化结构域版本。我们表征了它们的特性,然后选择全长Chk1作为最适合筛选的变异体。然后,我们通过测量细胞毒性和检查点旁路活性,在基于细胞的分析中鉴定并表征了结构不同的Chk1抑制剂。主要发现:我们用拓扑异构酶I抑制剂处理了人类细胞,并证明在加入Chk1抑制剂时,这些细胞已经破坏了DNA,并激活了Chk1。一种Chk1抑制剂,吲哚咔唑S27888在检查点旁路测定中具有活性。意义:知道每种抑制剂的蛋白激酶抑制特性是不同的,似乎细胞只能耐受有限范围的抑制活性。 Chk1在确定癌细胞对遗传毒性治疗的反应中起着至关重要的作用,因此,这种蛋白激酶的抑制剂具有重要的医学意义。

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