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Literature DB >> 32541966

Single-molecule analysis reveals agonist-specific dimer formation of µ-opioid receptors.

Jan Möller^1,2, Ali Isbilir^1,2, Titiwat Sungkaworn^2,3, Brendan Osberg^1,4, Christos Karathanasis⁵, Vikram Sunkara⁶, Eugene O Grushevskyi^1,2, Andreas Bock^1,2, Paolo Annibale^1,2, Mike Heilemann⁵, Christof Schütte^6,7, Martin J Lohse^8,9,10,11.

Abstract

G-protein-coupled receptors (GPCRs) are key signaling proteins that mostly function as monomers, but for several receptors constitutive dimer formation has been described and in some cases is essential for function. Using single-molecule microscopy combined with super-resolution techniques on intact cells, we describe here a dynamic monomer-dimer equilibrium of µ-opioid receptors (µORs), where dimer formation is driven by specific agonists. The agonist DAMGO, but not morphine, induces dimer formation in a process that correlates both temporally and in its agonist- and phosphorylation-dependence with β-arrestin2 binding to the receptors. This dimerization is independent from, but may precede, µOR internalization. These data suggest a new level of GPCR regulation that links dimer formation to specific agonists and their downstream signals.

Entities: Chemical

Mesh：

Substances：

Year: 2020 PMID： 32541966 DOI： 10.1038/s41589-020-0566-1

Source DB: PubMed Journal: Nat Chem Biol ISSN： 1552-4450 Impact factor: 16.174

51 in total

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Journal: Pharmacol Res Date: 2022-06-22 Impact factor: 10.334

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Journal: Biophys J Date: 2022-08-03 Impact factor: 3.699

5. Four-color single-molecule imaging with engineered tags resolves the molecular architecture of signaling complexes in the plasma membrane.

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6. Interface Prediction for GPCR Oligomerization Between Transmembrane Helices.

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Journal: Elife Date: 2021-04-21 Impact factor: 8.713

8. Determination of G-protein-coupled receptor oligomerization by molecular brightness analyses in single cells.

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Review 9. GRKs as Key Modulators of Opioid Receptor Function.

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10. Advanced fluorescence microscopy reveals disruption of dynamic CXCR4 dimerization by subpocket-specific inverse agonists.

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