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首页> 外文期刊>Analytical Biochemistry: An International Journal of Analytical and Preparative Methods >Fluorescence polarization assay for the identification and evaluation of inhibitors at YAP-TEAD protein-protein interface 3
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Fluorescence polarization assay for the identification and evaluation of inhibitors at YAP-TEAD protein-protein interface 3

机译:荧光偏振测定用于鉴定和评估Yap-Tead蛋白蛋白界面3的抑制剂

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摘要

The Hippo signaling pathway controls cell-cell contact, cell proliferation, as well as organ size by integrating changes in the cellular microenvironment. In recent years, the pivotal role of Hippo signaling in cancers has been well recognized. Inhibition of the pathway promotes the translocation of the major Hippo pathway effectors, the yes-associated protein (YAP) and its paralog TAZ, to the nucleus, where they interact with the transcription factor family transcriptional enhancer associate domain (TEAD), thus coactivating the expression of downstream genes, leading to cell transformation, tissue overgrowth, and tumor development. Therefore, the interruption of the YAP-TEAD transcriptional complex represents a novel opportunity for the treatment of cancer. Here, we established a fluorescence polarization (FP)-based assay for the identification and evaluation of YAP-TEAD protein-protein interface (PPI) inhibitors at the YAP Omega-loop binding region of TEAD, which is also called interface 3 at the YAP-TEAD binding surface. Furthermore, a patented small molecule (Patent-22) was evaluated by the FP assay, which confirmed that it was a YAP-TEAD PPI inhibitor at interface 3. Possessing great application value, this FP method is reliable, robust, and economical for inhibitor assessment and drug discovery.
机译:利马信号通路通过整合细胞微环境的变化控制细胞 - 细胞接触,细胞增殖以及器官尺寸。近年来,河马信号在癌症中的关键作用得到了很好的认可。抑制该途径促进主要河马途径效应器,对核心的迁移,对核,核心,核心,它们与转录因子家族转录系列转录增强剂联系结构域(TEAD)相互作用,从而共同激活下游基因的表达,导致细胞转化,组织过度生长和肿瘤发育。因此,Yap-Tead转录复合物的中断代表了治疗癌症的新机会。在此,我们建立了基于荧光偏振(FP)的测定,用于鉴定和评估曲线的Yap Omega-Loop结合区域的Yap-Tead蛋白质 - 蛋白质界面(PPI)抑制剂,其在YAP的界面3也称为界面3 - 绑定表面。此外,通过FP测定法评估专利的小分子(专利-22),该FP测定法证实它是界面3中的yap-tead PPI抑制剂。该FP方法可靠,鲁棒,抑制剂经济评估和药物发现。

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