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Structures in G proteins important for subtype selective receptor binding and subsequent activation

Volker Jelinek, Nadja Mößlein, Moritz Bünemann

2021Communications Biology27 citationsDOIOpen Access PDF

Abstract

Abstract G protein-coupled receptors (GPCRs) selectively couple to specific heterotrimeric G proteins comprised of four subfamilies in order to induce appropriate physiological responses. However, structural determinants in Gα subunits responsible for selective recognition by approximately 800 human GPCRs have remained elusive. Here, we directly compare the influence of subtype-specific Gα structures on the stability of GPCR-G protein complexes and the activation by two Gq-coupled receptors. We used FRET-assays designed to distinguish multiple Go and Gq-based Gα chimeras in their ability to be selectively bound and activated by muscarinic M 3 and histaminic H 1 receptors. We identify the N-terminus including the αN/β1-hinge, the β2/β3-loop and the α5 helix of Gα to be key selectivity determinants which differ in their impact on selective binding to GPCRs and subsequent activation depending on the specific receptor. Altogether, these findings provide new insights into the molecular basis of G protein-coupling selectivity even beyond the Gα C-terminus.

Topics & Concepts

Heterotrimeric G proteinG protein-coupled receptorG proteinReceptorGq alpha subunitRhodopsin-like receptorsCell biologyFörster resonance energy transferBiologyChemistryBiochemistryAgonistMetabotropic receptorQuantum mechanicsPhysicsFluorescenceReceptor Mechanisms and SignalingProtein Kinase Regulation and GTPase SignalingNeuropeptides and Animal Physiology
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