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Identification of Celastrol as a Novel YAP-TEAD Inhibitor for Cancer Therapy by High Throughput Screening with Ultrasensitive YAP/TAZ–TEAD Biosensors

机译:用超敏感的yap / Taz-tead生物传感器,鉴定Celastrol作为癌症治疗的新型YAP-Tead抑制剂

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摘要

The Hippo pathway has emerged as a key signaling pathway that regulates a broad range of biological functions, and dysregulation of the Hippo pathway is a feature of a variety of cancers. Given this, some have suggested that disrupting the interaction of the Hippo core component YAP and its paralog TAZ with transcriptional factor TEAD may be an effective strategy for cancer therapy. However, there are currently no clinically available drugs targeting the YAP/TAZ−TEAD interaction for cancer treatment. To facilitate screens for small molecule compounds that disrupt the YAP−TEAD interaction, we have developed the first ultra-bright NanoLuc biosensor to quantify YAP/TAZ−TEAD protein−protein interaction (PPI) both in living cells and also in vitro using biosensor fusion proteins purified from bacteria. Using this biosensor, we have performed an in vitro high throughput screen (HTS) of small molecule compounds and have identified and validated the drug Celastrol as a novel inhibitor of YAP/TAZ−TEAD interaction. We have also demonstrated that Celastrol can inhibit cancer cell proliferation, transformation, and cell migration. In this study, we describe a new inhibitor of the YAP/TAZ−TEAD interaction warranting further investigation and offer a novel biosensor tool for the discovery of other new Hippo-targeting drugs in future work.
机译:Hippo途径已成为调节广泛的生物功能的关键信号通路,河马途径的失调是各种癌症的特征。鉴于这一点,有些人建议破坏河马核心组分yap的相互作用及其对转录因子Tead的副古曲甙TAZ可能是癌症治疗的有效策略。然而,目前没有临床上可用的药物,旨在瞄准癌症治疗的YAP / TAZ-TEAD相互作用。为了促进破坏YAP-Tead相互作用的小分子化合物的屏幕,我们开发了第一个超亮纳米生物传感器,以定量活细胞和使用生物传感器融合的体外均在体外量化yap / taz-tab蛋白蛋白 - 蛋白 - 蛋白质相互作用(ppi)从细菌纯化的蛋白质。使用这种生物传感器,我们已经进行了小分子化合物的体外高通量筛网(HTS),并已鉴定并验证了药物Celastrol作为一种新的YAP / TAZ-TAD互动抑制剂。我们还表明Celastrol可以抑制癌细胞增殖,转化和细胞迁移。在这项研究中,我们描述了yap / taz-tead互动的新抑制剂保证进一步调查,并为未来的工作中发现其他新的河马靶向药物进行了新的生物传感器工具。

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