G protein selectivity profile of GPR56/ADGRG1 and its effect on downstream effectors.

IF 6.2 2区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Raida Jallouli, Ana L Moreno-Salinas, Andréanne Laniel, Brian Holleran, Charlotte Avet, Joan Jacob, Trang Hoang, Christine Lavoie, Kendra S Carmon, Michel Bouvier, Richard Leduc
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Abstract

GPR56, an adhesion G-protein coupled receptor (aGPCRs) with constitutive and ligand-promoted activity, is involved in many physiological and pathological processes. Whether the receptor's constitutive or ligand-promoted activation occur through the same molecular mechanism, and whether different activation modes lead to functional selectivity between G proteins is unknown. Here we show that GPR56 constitutively activates both G12 and G13. Unlike constitutive activation and activation with 3-α-acetoxydihydrodeoxygedunin (3αDOG), stimulation with an antibody, 10C7, directed against GPR56's extracellular domain (ECD) led to an activation that favors G13 over G12. An autoproteolytically deficient mutant, GPR56-T383A, was also activated by 10C7 indicating that the tethered agonist (TA) exposed through autocatalytic cleavage, is not required for this activation modality. In contrast, this proteolysis-resistant mutant could not be activated by 3αDOG indicating different modes of activation by the two ligands. We show that an N-terminal truncated GPR56 construct (GPR56-Δ1-385) is devoid of constitutive activity but was activated by 3αDOG. Similarly to 3αDOG, 10C7 promoted the recruitment of β-arrestin-2 but GPR56 internalization was β-arrestin independent. Despite the slow activation mode of 10C7 that favors G13 over G12, it efficiently activated the downstream Rho pathway in BT-20 breast cancer cells. These data show that different GPR56 ligands have different modes of activation yielding differential G protein selectivity but converging on the activation of the Rho pathway both in heterologous expressions system and in cancer cells endogenously expressing the receptor. 10C7 is therefore an interesting tool to study both the processes underlying GPR56 activity and its role in cancer cells.

Abstract Image

GPR56/ADGRG1 的 G 蛋白选择性特征及其对下游效应物的影响。
GPR56 是一种粘附 G 蛋白偶联受体(aGPCRs),具有组成型和配体促进型活性,参与许多生理和病理过程。该受体的组成型激活和配体促进型激活是否通过相同的分子机制发生,以及不同的激活模式是否会导致 G 蛋白之间的功能选择性,目前尚不清楚。在这里,我们发现 GPR56 可构成性地激活 G12 和 G13。与组成型激活和用 3-α-acetoxydihydrodeoxygedunin (3αDOG) 激活不同,用针对 GPR56 细胞外结构域 (ECD) 的抗体 10C7 刺激 GPR56 会导致 G13 激活,而不是 G12 激活。自体蛋白水解缺陷突变体 GPR56-T383A 也能被 10C7 激活,这表明这种激活方式并不需要通过自体催化裂解暴露的系链激动剂(TA)。相反,这种蛋白水解抗性突变体不能被 3αDOG 激活,这表明两种配体的激活模式不同。我们发现一个 N 端截短的 GPR56 构建体(GPR56-Δ1-385)没有组成型活性,但能被 3αDOG 激活。与 3αDOG 类似,10C7 也促进了 β-restin-2 的招募,但 GPR56 的内化与 β-restin 无关。尽管 10C7 的激活模式较慢,更倾向于 G13 而不是 G12,但它还是有效地激活了 BT-20 乳腺癌细胞的下游 Rho 通路。这些数据表明,不同的 GPR56 配体具有不同的激活模式,从而产生不同的 G 蛋白选择性,但在异源表达系统和内源性表达受体的癌细胞中,它们都趋向于激活 Rho 通路。因此,10C7 是研究 GPR56 活性及其在癌细胞中作用的有趣工具。
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来源期刊
Cellular and Molecular Life Sciences
Cellular and Molecular Life Sciences 生物-生化与分子生物学
CiteScore
13.20
自引率
1.20%
发文量
546
审稿时长
1.0 months
期刊介绍: Journal Name: Cellular and Molecular Life Sciences (CMLS) Location: Basel, Switzerland Focus: Multidisciplinary journal Publishes research articles, reviews, multi-author reviews, and visions & reflections articles Coverage: Latest aspects of biological and biomedical research Areas include: Biochemistry and molecular biology Cell biology Molecular and cellular aspects of biomedicine Neuroscience Pharmacology Immunology Additional Features: Welcomes comments on any article published in CMLS Accepts suggestions for topics to be covered
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