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PNAS Plus: Multimodular biosensors reveal a novel platform for activation of G proteins by growth factor receptors

机译:PNAS Plus:多模块生物传感器揭示了一种新的平台可通过生长因子受体激活G蛋白

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摘要

Environmental cues are transmitted to the interior of the cell via a complex network of signaling hubs. Receptor tyrosine kinases (RTKs) and trimeric G proteins are two such major signaling hubs in eukaryotes. Conventionally, canonical signal transduction via trimeric G proteins is thought to be triggered exclusively by G protein-coupled receptors. Here we used molecular engineering to develop modular fluorescent biosensors that exploit the remarkable specificity of bimolecular recognition, i.e., of both G proteins and RTKs, and reveal the workings of a novel platform for activation of G proteins by RTKs in single living cells. Comprised of the unique modular makeup of guanidine exchange factor Gα-interacting vesicle-associated protein (GIV)/girdin, a guanidine exchange factor that links G proteins to a variety of RTKs, these biosensors provide direct evidence that RTK–GIV–Gαi ternary complexes are formed in living cells and that Gαi is transactivated within minutes after growth factor stimulation at the plasma membrane. Thus, GIV-derived biosensors provide a versatile strategy for visualizing, monitoring, and manipulating the dynamic association of Gαi with RTKs for noncanonical transactivation of G proteins in cells and illuminate a fundamental signaling event regulated by GIV during diverse cellular processes and pathophysiologic states.
机译:环境提示通过复杂的信号集线器网络传输到单元内部。受体酪氨酸激酶(RTKs)和三聚体G蛋白是真核生物中的两个主要信号转导中心。常规上,认为经由三聚体G蛋白的规范信号转导仅由G蛋白偶联的受体触发。在这里,我们使用分子工程技术开发了模块化的荧光生物传感器,该传感器利用了双分子识别(即G蛋白和RTKs)的卓越特异性,并揭示了RTK在单个活细胞中激活G蛋白的新型平台的工作原理。包含与胍交换因子Gα相互作用的囊泡相关蛋白(GIV)/吉丁(一种将G蛋白与多种RTK连接的胍交换因子)的独特模块组成,这些生物传感器提供了直接证据,证明RTK–GIV–Gαi三元复合物它们在活细胞中形成,Gαi在质膜上的生长因子刺激后数分钟内被反式激活。因此,源自GIV的生物传感器提供了一种通用的策略,用于可视化,监控和操纵Gαi与RTK的动态关联,以实现细胞中G蛋白的非经典反式激活,并阐明了GIV在多种细胞过程和病理生理状态下调节的基本信号转导事件。

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