GPR50-Ctail cleavage and nuclear translocation: a new signal transduction mode for G protein-coupled receptors

被引:0
|
作者
Raise Ahmad
Olivier Lahuna
Anissa Sidibe
Avais Daulat
Qiang Zhang
Marine Luka
Jean-Luc Guillaume
Sarah Gallet
François Guillonneau
Juliette Hamroune
Sophie Polo
Vincent Prévot
Philippe Delagrange
Julie Dam
Ralf Jockers
机构
[1] Université de Paris,Epigenetics and Cell Fate Centre
[2] Institut Cochin,undefined
[3] CNRS,undefined
[4] INSERM,undefined
[5] Jean-Pierre Aubert Research Center,undefined
[6] UMR7216,undefined
[7] CNRS,undefined
[8] Paris Diderot University,undefined
[9] Pôle D’Innovation Thérapeutique Neuropsychiatrie,undefined
[10] Institut de Recherches Servier,undefined
来源
Cellular and Molecular Life Sciences | 2020年 / 77卷
关键词
GPCR; Orphan; Calpain; GPR50; Proteolytic cleavage; Signal transduction;
D O I
暂无
中图分类号
学科分类号
摘要
Transmission of extracellular signals by G protein-coupled receptors typically relies on a cascade of intracellular events initiated by the activation of heterotrimeric G proteins or β-arrestins followed by effector activation/inhibition. Here, we report an alternative signal transduction mode used by the orphan GPR50 that relies on the nuclear translocation of its carboxyl-terminal domain (CTD). Activation of the calcium-dependent calpain protease cleaves off the CTD from the transmembrane-bound GPR50 core domain between Phe-408 and Ser-409 as determined by MALDI-TOF-mass spectrometry. The cytosolic CTD then translocates into the nucleus assisted by its ‘DPD’ motif, where it interacts with the general transcription factor TFII-I to regulate c-fos gene transcription. RNA-Seq analysis indicates a broad role of the CTD in modulating gene transcription with ~ 8000 differentially expressed genes. Our study describes a non-canonical, direct signaling mode of GPCRs to the nucleus with similarities to other receptor families such as the NOTCH receptor
引用
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页码:5189 / 5205
页数:16
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