Evidence for functional pre-coupled complexes of receptor heteromers and adenylyl cyclase.

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作者:Navarro Gemma, Cordomí Arnau, Casadó-Anguera Verónica, Moreno Estefanía, Cai Ning-Sheng, Cortés Antoni, Canela Enric I, Dessauer Carmen W, Casadó Vicent, Pardo Leonardo, Lluís Carme, Ferré Sergi
G protein-coupled receptors (GPCRs), G proteins and adenylyl cyclase (AC) comprise one of the most studied transmembrane cell signaling pathways. However, it is unknown whether the ligand-dependent interactions between these signaling molecules are based on random collisions or the rearrangement of pre-coupled elements in a macromolecular complex. Furthermore, it remains controversial whether a GPCR homodimer coupled to a single heterotrimeric G protein constitutes a common functional unit. Using a peptide-based approach, we here report evidence for the existence of functional pre-coupled complexes of heteromers of adenosine A(2A) receptor and dopamine D(2) receptor homodimers coupled to their cognate Gs and Gi proteins and to subtype 5 AC. We also demonstrate that this macromolecular complex provides the necessary frame for the canonical Gs-Gi interactions at the AC level, sustaining the ability of a Gi-coupled GPCR to counteract AC activation mediated by a Gs-coupled GPCR.

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