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CaMello-XR enables visualization and optogenetic control of Gq/11 signals and receptor trafficking in GPCR-specific domains

机译:CaMello-XR可实现Gq / 11信号的可视化和光遗传学控制以及GPCR特定域中的受体运输

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摘要

The signal specificity of G protein-coupled receptors (GPCRs) including serotonin receptors (5-HT-R) depends on the trafficking and localization of the GPCR within its subcellular signaling domain. Visualizing traffic-dependent GPCR signals in neurons is difficult, but important to understand the contribution of GPCRs to synaptic plasticity. We engineered CaMello (Ca2+-melanopsin-local-sensor) and CaMello-5HT2A for visualization of traffic-dependent Ca2+ signals in 5-HT2A-R domains. These constructs consist of the light-activated Gq/11 coupled melanopsin, mCherry and GCaMP6m for visualization of Ca2+ signals and receptor trafficking, and the 5-HT2A C-terminus for targeting into 5-HT2A-R domains. We show that the specific localization of the GPCR to its receptor domain drastically alters the dynamics and localization of the intracellular Ca2+ signals in different neuronal populations in vitro and in vivo. The CaMello method may be extended to every GPCR coupling to the Gq/11 pathway to help unravel new receptor-specific functions in respect to synaptic plasticity and GPCR localization.
机译:G蛋白偶联受体(GPCR)包括5-羟色胺受体(5-HT-R)的信号特异性取决于GPCR在其亚细胞信号域内的运输和定位。可视化神经元中依赖交通的GPCR信号是困难的,但了解GPCR对突触可塑性的贡献很重要。我们设计了CaMello(Ca 2 + -黑皮素局部传感器)和CaMello-5HT2A,用于可视化5-HT2A-R域中依赖交通的Ca 2 + 信号。这些构建体由光激活的Gq / 11偶联的黑色素,mCherry和GCaMP6m组成,用于可视化Ca 2 + 信号和受体运输,以及用于靶向5-HT2A-的5-HT2A C端。 R域。我们发现,GPCR对其受体结构域的特异性定位在体外和体内显着改变了细胞内Ca 2 + 信号在不同神经元群体中的动力学和定位。 CaMello方法可以扩展到每个与Gq / 11途径偶联的GPCR,以帮助揭示有关突触可塑性和GPCR定位的新受体特异性功能。

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