评估G蛋白偶联受体(GPCRs)功能选择性的方法:在内源环境中评估G蛋白信号传导
Approaches to Assess Functional Selectivity in GPCRs: Evaluating G Protein Signaling in an Endogenous Environment.
作者信息
Bohn Laura M, Zhou Lei, Ho Jo-Hao
机构信息
Departments of Molecular Therapeutics and Neuroscience, The Scripps Research Institute, 130 Scripps Way #2A2, Jupiter, FL, 33458, USA,
出版信息
Methods Mol Biol. 2015;1335:177-89. doi: 10.1007/978-1-4939-2914-6_12.
Abstract
Ligand-directed signaling, biased agonism, and functional selectivity are terms that describe the propensity of a ligand to drive signaling toward one GPCR pathway over another. Most of the early examples demonstrated to date examine the divergence between GPCR signaling to G protein coupling and βarrestin2 recruitment. As biased agonists begin to become available based on cell-based screening criteria, a need arises to determine if G protein signaling biases will be maintained in the endogenous setting, wherein receptors are functioning to control relevant biological responses. This report presents our method and offers tips for evaluating G protein signaling in endogenous tissues. Predominately, brain tissues are discussed here; optimization points that can be applied to any tissues are highlighted.
摘要
配体导向信号传导、偏向性激动作用和功能选择性是描述配体驱动信号向一条GPCR途径而非另一条途径传导倾向的术语。迄今为止,大多数已证实的早期例子都研究了GPCR向G蛋白偶联信号传导与βarrestin2募集之间的差异。随着基于细胞筛选标准的偏向性激动剂开始出现,有必要确定G蛋白信号偏向性在内源性环境中是否会保持,在内源性环境中,受体发挥作用以控制相关生物学反应。本报告介绍了我们的方法,并提供了评估内源性组织中G蛋白信号传导的技巧。主要在此讨论脑组织;突出了可应用于任何组织的优化要点。
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