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Literature DB >> 29632174

GHSR-D2R heteromerization modulates dopamine signaling through an effect on G protein conformation.

Marjorie Damian¹, Véronique Pons², Pedro Renault¹, Céline M'Kadmi¹, Bartholomé Delort¹, Lucie Hartmann³, Ali I Kaya⁴, Maxime Louet¹, Didier Gagne¹, Khoubaib Ben Haj Salah¹, Séverine Denoyelle¹, Gilles Ferry⁵, Jean A Boutin⁵, Renaud Wagner³, Jean-Alain Fehrentz¹, Jean Martinez¹, Jacky Marie¹, Nicolas Floquet¹, Céline Galès², Sophie Mary¹, Heidi E Hamm⁴, Jean-Louis Banères⁶.

Abstract

The growth hormone secretagogue receptor (GHSR) and dopamine receptor (D2R) have been shown to oligomerize in hypothalamic neurons with a significant effect on dopamine signaling, but the molecular processes underlying this effect are still obscure. We used here the purified GHSR and D2R to establish that these two receptors assemble in a lipid environment as a tetrameric complex composed of two each of the receptors. This complex further recruits G proteins to give rise to an assembly with only two G protein trimers bound to a receptor tetramer. We further demonstrate that receptor heteromerization directly impacts on dopamine-mediated Gi protein activation by modulating the conformation of its α-subunit. Indeed, association to the purified GHSR:D2R heteromer triggers a different active conformation of Gαi that is linked to a higher rate of GTP binding and a faster dissociation from the heteromeric receptor. This is an additional mechanism to expand the repertoire of GPCR signaling modulation that could have implications for the control of dopamine signaling in normal and physiopathological conditions.

Entities: Chemical Disease Gene

Keywords: G protein; GPCR; conformational dynamics; heteromer; signaling

Mesh：

Substances：

Year: 2018 PMID： 29632174 PMCID： PMC5924877 DOI： 10.1073/pnas.1712725115

Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN： 0027-8424 Impact factor: 11.205

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