Structure of the vasopressin hormone–V2 receptor–β-arrestin1 ternary complex

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Bous, Julien | Fouillen, Aurélien | Orcel, Hélène | Trapani, Stefano | Cong, Xiaojing | Fontanel, Simon | Saint-Paul, Julie | Lai-Kee-Him, Joséphine | Urbach, Serge | Sibille, Nathalie | Sounier, Rémy | Granier, Sébastien | Mouillac, Bernard | Bron, Patrick

Edité par CCSD ; American Association for the Advancement of Science (AAAS) -

International audience. Arrestins interact with G protein-coupled receptors (GPCRs) to stop G protein activation and to initiate key signaling pathways. Recent structural studies shed light on the molecular mechanisms involved in GPCR-arrestin coupling, but whether this process is conserved among GPCRs is poorly understood. Here, we report the cryo-electron microscopy active structure of the wild-type arginine-vasopressin V2 receptor (V2R) in complex with β-arrestin1. It reveals an atypical position of β-arrestin1 compared to previously described GPCR-arrestin assemblies, associated with an original V2R/β-arrestin1 interface involving all receptor intracellular loops. Phosphorylated sites of the V2R carboxyl terminus are clearly identified and interact extensively with the β-arrestin1 N-lobe, in agreement with structural data obtained with chimeric or synthetic systems. Overall, these findings highlight a notable structural variability among GPCR-arrestin signaling complexes.

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