Literature DB >> 16199535

Homo- and hetero-oligomerization of beta-arrestins in living cells.

Hélène Storez1, Mark G H Scott, Hassan Issafras, Anne Burtey, Alexandre Benmerah, Olivier Muntaner, Tristan Piolot, Marc Tramier, Maité Coppey-Moisan, Michel Bouvier, Catherine Labbé-Jullié, Stefano Marullo.   

Abstract

Arrestins are important proteins, which regulate the function of serpentine heptahelical receptors and contribute to multiple signaling pathways downstream of receptors. The ubiquitous beta-arrestins are believed to function exclusively as monomers, although self-association is assumed to control the activity of visual arrestin in the retina, where this isoform is particularly abundant. Here the oligomerization status of beta-arrestins was investigated using different approaches, including co-immunoprecipitation of epitope-tagged beta-arrestins and resonance energy transfer (BRET and FRET) in living cells. At steady state and at physiological concentrations, beta-arrestins constitutively form both homo- and hetero-oligomers. Co-expression of beta-arrestin2 and beta-arrestin1 prevented beta-arrestin1 accumulation into the nucleus, suggesting that hetero-oligomerization may have functional consequences. Our data clearly indicate that beta-arrestins can exist as homo- and hetero-oligomers in living cells and raise the hypothesis that the oligomeric state may regulate their subcellular distribution and functions.

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Year:  2005        PMID: 16199535     DOI: 10.1074/jbc.M508001200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  45 in total

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2.  The orphan GPR50 receptor specifically inhibits MT1 melatonin receptor function through heterodimerization.

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Review 4.  A day in the life of a G protein-coupled receptor: the contribution to function of G protein-coupled receptor dimerization.

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5.  Resonance energy transfer in cells: a new look at fixation effect and receptor aggregation on cell membrane.

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6.  Distinct conformational changes in beta-arrestin report biased agonism at seven-transmembrane receptors.

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8.  The 27-kDa heat shock protein confers cytoprotective effects through a beta 2-adrenergic receptor agonist-initiated complex with beta-arrestin.

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9.  S-Nitrosylation of β-Arrestins Biases Receptor Signaling and Confers Ligand Independence.

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Journal:  Mol Cell       Date:  2018-05-03       Impact factor: 17.970

10.  beta-arrestin 2 oligomerization controls the Mdm2-dependent inhibition of p53.

Authors:  Cédric Boularan; Mark G H Scott; Karima Bourougaa; Myriam Bellal; Emmanuel Esteve; Alain Thuret; Alexandre Benmerah; Marc Tramier; Maité Coppey-Moisan; Catherine Labbé-Jullié; Robin Fåhraeus; Stefano Marullo
Journal:  Proc Natl Acad Sci U S A       Date:  2007-11-05       Impact factor: 11.205

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