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Elucidating the Interactome of G Protein-Coupled Receptors and Receptor Activity-Modifying Proteins

机译:阐明 G 蛋白偶联受体和受体活性修饰蛋白的相互作用组

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摘要

G protein-coupled receptors (GPCRs) are known to interact with several other classes of integral membrane proteins that modulate their biology and pharmacology. However, the extent of these interactions and the mechanisms of their effects are not well understood. For example, one class of GPCR-interacting proteins, receptor activity-modifying proteins (RAMPs), comprise three related and ubiquitously expressed single-transmembrane span proteins. The RAMP family was discovered more than two decades ago, and since then GPCR–RAMP interactions and their functional consequences on receptor trafficking and ligand selectivity have been documented for several secretin (class B) GPCRs, most notably the calcitonin receptor-like receptor. Recent bioinformatics and multiplexed experimental studies suggest that GPCR–RAMP interactions might be much more widespread than previously anticipated. Recently, cryo-electron microscopy has provided high-resolution structures of GPCR–RAMP–ligand complexes, and drugs have been developed that target GPCR–RAMP complexes. In this review, we provide a summary of recent advances in techniques that allow the discovery of GPCR–RAMP interactions and their functional consequences and highlight prospects for future advances. We also provide an up-to-date list of reported GPCR–RAMP interactions based on a review of the current literature.
机译:已知 G 蛋白偶联受体 (GPCR) 与其他几类调节其生物学和药理学的整合膜蛋白相互作用。然而,这些相互作用的程度及其影响机制尚不清楚。例如,一类 GPCR 相互作用蛋白,受体活性修饰蛋白 (RAMP),包含三种相关且普遍表达的单跨膜跨度蛋白。RAMP 家族是在二十多年前发现的,从那时起,GPCR-RAMP 相互作用及其对受体运输和配体选择性的功能影响已被记录在几种促胰液素(B 类)GPCR 中,最值得注意的是降钙素受体样受体。最近的生物信息学和多重实验研究表明,GPCR-RAMP 相互作用可能比以前预期的要广泛得多。最近,冷冻电子显微镜提供了 GPCR-RAMP-配体复合物的高分辨率结构,并且已经开发了靶向 GPCR-RAMP 复合物的药物。在这篇综述中,我们总结了允许发现 GPCR-RAMP 相互作用及其功能后果的技术的最新进展,并强调了未来进展的前景。我们还根据对当前文献的回顾提供了已报道的 GPCR-RAMP 相互作用的最新列表。

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