| Literature DB >> 32303636 |
Feng-Jie Wu1, Lisa M Williams2, Alaa Abdul-Ridha2, Avanka Gunatilaka2, Tasneem M Vaid1, Martina Kocan2, Alice R Whitehead2, Michael D W Griffin3, Ross A D Bathgate4, Daniel J Scott5, Paul R Gooley6.
Abstract
G protein-coupled receptors (GPCRs) use a series of conserved microswitches to transmit signals across the cell membrane via an allosteric network encompassing the ligand-binding site and the G protein-binding site. Crystal structures of GPCRs provide snapshots of their inactive and active states, but poorly describe the conformational dynamics of the allosteric network that underlies GPCR activation. Here, we analyzed the correlation between ligand binding and receptor conformation of the α1A-adrenoreceptor, a GPCR that stimulates smooth muscle contraction in response to binding noradrenaline. NMR of [13CϵH3]methionine-labeled α1A-adrenoreceptor variants, each exhibiting differing signaling capacities, revealed how different classes of ligands modulate the conformational equilibria of this receptor. [13CϵH3]Methionine residues near the microswitches exhibited distinct states that correlated with ligand efficacies, supporting a conformational selection mechanism. We propose that allosteric coupling among the microswitches controls the conformation of the α1A-adrenoreceptor and underlies the mechanism of ligand modulation of GPCR signaling in cells.Entities:
Keywords: G protein-coupled receptor (GPCR); adrenergic receptor; allosteric coupling; binding mechanism; conformational change; conformational equilibrium; ligand-binding protein; microswitch; nuclear magnetic resonance (NMR); solution structure
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Year: 2020 PMID: 32303636 PMCID: PMC7247315 DOI: 10.1074/jbc.RA120.012842
Source DB: PubMed Journal: J Biol Chem ISSN: 0021-9258 Impact factor: 5.157