Literature DB >> 21868357

Distinct phosphorylation sites on the β(2)-adrenergic receptor establish a barcode that encodes differential functions of β-arrestin.

Kelly N Nobles1, Kunhong Xiao, Seungkirl Ahn, Arun K Shukla, Christopher M Lam, Sudarshan Rajagopal, Ryan T Strachan, Teng-Yi Huang, Erin A Bressler, Makoto R Hara, Sudha K Shenoy, Steven P Gygi, Robert J Lefkowitz.   

Abstract

Phosphorylation of G protein-coupled receptors (GPCRs, which are also known as seven-transmembrane spanning receptors) by GPCR kinases (GRKs) plays essential roles in the regulation of receptor function by promoting interactions of the receptors with β-arrestins. These multifunctional adaptor proteins desensitize GPCRs, by reducing receptor coupling to G proteins and facilitating receptor internalization, and mediate GPCR signaling through β-arrestin-specific pathways. Detailed mapping of the phosphorylation sites on GPCRs targeted by individual GRKs and an understanding of how these sites regulate the specific functional consequences of β-arrestin engagement may aid in the discovery of therapeutic agents targeting individual β-arrestin functions. The β(2)-adrenergic receptor (β(2)AR) has many serine and threonine residues in the carboxyl-terminal tail and the intracellular loops, which are potential sites of phosphorylation. We monitored the phosphorylation of the β(2)AR at specific sites upon stimulation with an agonist that promotes signaling by both G protein-mediated and β-arrestin-mediated pathways or with a biased ligand that promotes signaling only through β-arrestin-mediated events in the presence of the full complement of GRKs or when either GRK2 or GRK6 was depleted. We correlated the specific and distinct patterns of receptor phosphorylation by individual GRKs with the functions of β-arrestins and propose that the distinct phosphorylation patterns established by different GRKs establish a "barcode" that imparts distinct conformations to the recruited β-arrestin, thus regulating its functional activities.

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Year:  2011        PMID: 21868357      PMCID: PMC3415961          DOI: 10.1126/scisignal.2001707

Source DB:  PubMed          Journal:  Sci Signal        ISSN: 1945-0877            Impact factor:   8.192


  44 in total

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Authors:  R J Lefkowitz; J Inglese; W J Koch; J Pitcher; H Attramadal; M G Caron
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3.  Functional specialization of beta-arrestin interactions revealed by proteomic analysis.

Authors:  Kunhong Xiao; Daniel B McClatchy; Arun K Shukla; Yang Zhao; Minyong Chen; Sudha K Shenoy; John R Yates; Robert J Lefkowitz
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4.  Phosphorylation sites on two domains of the beta 2-adrenergic receptor are involved in distinct pathways of receptor desensitization.

Authors:  W P Hausdorff; M Bouvier; B F O'Dowd; G P Irons; M G Caron; R J Lefkowitz
Journal:  J Biol Chem       Date:  1989-07-25       Impact factor: 5.157

5.  G-protein-coupled receptor kinase specificity for beta-arrestin recruitment to the beta2-adrenergic receptor revealed by fluorescence resonance energy transfer.

Authors:  Jonathan D Violin; Xiu-Rong Ren; Robert J Lefkowitz
Journal:  J Biol Chem       Date:  2006-05-10       Impact factor: 5.157

6.  beta-arrestin-dependent, G protein-independent ERK1/2 activation by the beta2 adrenergic receptor.

Authors:  Sudha K Shenoy; Matthew T Drake; Christopher D Nelson; Daniel A Houtz; Kunhong Xiao; Srinivasan Madabushi; Eric Reiter; Richard T Premont; Olivier Lichtarge; Robert J Lefkowitz
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7.  Localization of the sites mediating desensitization of the beta(2)-adrenergic receptor by the GRK pathway.

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9.  Role of the G protein-coupled receptor kinase site serine cluster in beta2-adrenergic receptor internalization, desensitization, and beta-arrestin translocation.

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  255 in total

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8.  Distinct Signaling Patterns of Allosteric Antagonism at the P2Y1 Receptor.

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9.  Structural and Functional Analysis of a β2-Adrenergic Receptor Complex with GRK5.

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Review 10.  G protein-coupled receptors--recent advances.

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