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首页> 外文期刊>Journal of molecular cell biology >Enabling systematic interrogation of protein-protein interactions in live cells with a versatile ultra-high-throughput biosensor platform.
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Enabling systematic interrogation of protein-protein interactions in live cells with a versatile ultra-high-throughput biosensor platform.

机译:借助多功能超高通量生物传感器平台,可以系统地研究活细胞中的蛋白质相互作用。

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摘要

Large-scale genomics studies have generated vast resources for in-depth understanding of vital biological and pathological processes. A rising challenge is to leverage such enormous information to rapidly decipher the intricate protein-protein interactions (PPIs) for functional characterization and therapeutic interventions. While a number of powerful technologies have been employed to detect PPIs, a singular PPI biosensor platform with both high sensitivity and robustness in a mammalian cell environment remains to be established. Here we describe the development and integration of a highly sensitive NanoLuc luciferase-based bioluminescence resonance energy transfer technology, termed BRET(n), which enables ultra-high-throughput (uHTS) PPI detection in live cells with streamlined co-expression of biosensors in a miniaturized format. We further demonstrate the application of BRET(n) in uHTS format in chemical biology research, including the discovery of chemical probes that disrupt PRAS40 dimerization and pathway connectivity profiling among core members of the Hippo signaling pathway. Such hippo pathway profiling not only confirmed previously reported PPIs, but also revealed two novel interactions, suggesting new mechanisms for regulation of Hippo signaling. Our BRET(n) biosensor platform with uHTS capability is expected to accelerate systematic PPI network mapping and PPI modulator-based drug discovery.
机译:大规模基因组学研究为深入了解重要的生物学和病理学过程提供了广阔的资源。一个日益严峻的挑战是利用如此巨大的信息来快速解密复杂的蛋白质-蛋白质相互作用(PPI),以进行功能表征和治疗干预。尽管已经采用了许多强大的技术来检测PPI,但是在哺乳动物细胞环境中具有高灵敏度和鲁棒性的单一PPI生物传感器平台仍有待建立。在这里,我们描述了一种称为BRET(n)的基于高灵敏度NanoLuc荧光素酶的生物发光共振能量转移技术的开发和集成,该技术可在活细胞中实现超高通量(uHTS)PPI检测,并简化了生物传感器的共表达。小型化的格式。我们进一步展示了uHTS格式的BRET(n)在化学生物学研究中的应用,包括发现破坏PRAS40二聚化和Hippo信号传导途径核心成员之间的途径连通性谱的化学探针。这种河马途径分析不仅证实了先前报道的PPI,而且还揭示了两个新颖的相互作用,提示了调控Hippo信号传导的新机制。我们具有uHTS功能的BRET(n)生物传感器平台有望加速系统化的PPI网络映射和基于PPI调节剂的药物发现。

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