| Literature DB >> 31900622 |
Raise Ahmad1, Olivier Lahuna1, Anissa Sidibe1, Avais Daulat1, Qiang Zhang1, Marine Luka1, Jean-Luc Guillaume1, Sarah Gallet2, François Guillonneau1, Juliette Hamroune1, Sophie Polo3, Vincent Prévot2, Philippe Delagrange4, Julie Dam1, Ralf Jockers5.
Abstract
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.Entities:
Keywords: Calpain; GPCR; GPR50; Orphan; Proteolytic cleavage; Signal transduction
Mesh:
Substances:
Year: 2020 PMID: 31900622 DOI: 10.1007/s00018-019-03440-7
Source DB: PubMed Journal: Cell Mol Life Sci ISSN: 1420-682X Impact factor: 9.261