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Literature DB >> 28461104

Differential manipulation of arrestin-3 binding to basal and agonist-activated G protein-coupled receptors.

Susanne Prokop¹, Nicole A Perry², Sergey A Vishnivetskiy², Andras D Toth¹, Asuka Inoue³, Graeme Milligan⁴, Tina M Iverson², Laszlo Hunyady¹, Vsevolod V Gurevich⁵.

Abstract

Non-visual arrestins interact with hundreds of different G protein-coupled receptors (GPCRs). Here we show that by introducing mutations into elements that directly bind receptors, the specificity of arrestin-3 can be altered. Several mutations in the two parts of the central "crest" of the arrestin molecule, middle-loop and C-loop, enhanced or reduced arrestin-3 interactions with several GPCRs in receptor subtype and functional state-specific manner. For example, the Lys139Ile substitution in the middle-loop dramatically enhanced the binding to inactive M2 muscarinic receptor, so that agonist activation of the M2 did not further increase arrestin-3 binding. Thus, the Lys139Ile mutation made arrestin-3 essentially an activation-independent binding partner of M2, whereas its interactions with other receptors, including the β2-adrenergic receptor and the D1 and D2 dopamine receptors, retained normal activation dependence. In contrast, the Ala248Val mutation enhanced agonist-induced arrestin-3 binding to the β2-adrenergic and D2 dopamine receptors, while reducing its interaction with the D1 dopamine receptor. These mutations represent the first example of altering arrestin specificity via enhancement of the arrestin-receptor interactions rather than selective reduction of the binding to certain subtypes.

Entities: CellLine Chemical Disease Gene Mutation Species

Keywords: Arrestin; GPCRs; Protein engineering; Protein-protein interactions; Receptor specificity

Mesh：

Substances：

Year: 2017 PMID： 28461104 PMCID： PMC5797668 DOI： 10.1016/j.cellsig.2017.04.021

Source DB: PubMed Journal: Cell Signal ISSN： 0898-6568 Impact factor: 4.315

81 in total

1. The differential engagement of arrestin surface charges by the various functional forms of the receptor.

Authors: Susan M Hanson; Vsevolod V Gurevich
Journal: J Biol Chem Date: 2005-12-08 Impact factor: 5.157

2. Phosphodiesterase activation by photoexcited rhodopsin is quenched when rhodopsin is phosphorylated and binds the intrinsic 48-kDa protein of rod outer segments.

Authors: U Wilden; S W Hall; H Kühn
Journal: Proc Natl Acad Sci U S A Date: 1986-03 Impact factor: 11.205

3. How does arrestin respond to the phosphorylated state of rhodopsin?

Authors: S A Vishnivetskiy; C L Paz; C Schubert; J A Hirsch; P B Sigler; V V Gurevich
Journal: J Biol Chem Date: 1999-04-23 Impact factor: 5.157

4. Manipulation of very few receptor discriminator residues greatly enhances receptor specificity of non-visual arrestins.

Authors: Luis E Gimenez; Sergey A Vishnivetskiy; Faiza Baameur; Vsevolod V Gurevich
Journal: J Biol Chem Date: 2012-07-11 Impact factor: 5.157

5. Targeted construction of phosphorylation-independent beta-arrestin mutants with constitutive activity in cells.

Authors: A Kovoor; J Celver; R I Abdryashitov; C Chavkin; V V Gurevich
Journal: J Biol Chem Date: 1999-03-12 Impact factor: 5.157

6. Topographic study of arrestin using differential chemical modifications and hydrogen/deuterium exchange.

Authors: H Ohguro; K Palczewski; K A Walsh; R S Johnson
Journal: Protein Sci Date: 1994-12 Impact factor: 6.725

7. The G-protein-coupled receptors in the human genome form five main families. Phylogenetic analysis, paralogon groups, and fingerprints.

Authors: Robert Fredriksson; Malin C Lagerström; Lars-Gustav Lundin; Helgi B Schiöth
Journal: Mol Pharmacol Date: 2003-06 Impact factor: 4.436

8. Enhanced arrestin facilitates recovery and protects rods lacking rhodopsin phosphorylation.

Authors: Xiufeng Song; Sergey A Vishnivetskiy; Owen P Gross; Katrina Emelianoff; Ana Mendez; Jeannie Chen; Eugenia V Gurevich; Marie E Burns; Vsevolod V Gurevich
Journal: Curr Biol Date: 2009-04-09 Impact factor: 10.834

9. Rapid diversification of cell signaling phenotypes by modular domain recombination.

Authors: Sergio G Peisajovich; Joan E Garbarino; Ping Wei; Wendell A Lim
Journal: Science Date: 2010-04-16 Impact factor: 47.728

10. Targeted Elimination of G Proteins and Arrestins Defines Their Specific Contributions to Both Intensity and Duration of G Protein-coupled Receptor Signaling.

Authors: Elisa Alvarez-Curto; Asuka Inoue; Laura Jenkins; Sheikh Zahir Raihan; Rudi Prihandoko; Andrew B Tobin; Graeme Milligan
Journal: J Biol Chem Date: 2016-11-16 Impact factor: 5.157

9 in total

Review 1. Plethora of functions packed into 45 kDa arrestins: biological implications and possible therapeutic strategies.

Authors: Vsevolod V Gurevich; Eugenia V Gurevich
Journal: Cell Mol Life Sci Date: 2019-08-17 Impact factor: 9.261

Differential manipulation of arrestin-3 binding to basal and agonist-activated G protein-coupled receptors.

1. The differential engagement of arrestin surface charges by the various functional forms of the receptor.

2. Phosphodiesterase activation by photoexcited rhodopsin is quenched when rhodopsin is phosphorylated and binds the intrinsic 48-kDa protein of rod outer segments.

3. How does arrestin respond to the phosphorylated state of rhodopsin?

4. Manipulation of very few receptor discriminator residues greatly enhances receptor specificity of non-visual arrestins.

5. Targeted construction of phosphorylation-independent beta-arrestin mutants with constitutive activity in cells.

6. Topographic study of arrestin using differential chemical modifications and hydrogen/deuterium exchange.

7. The G-protein-coupled receptors in the human genome form five main families. Phylogenetic analysis, paralogon groups, and fingerprints.

8. Enhanced arrestin facilitates recovery and protects rods lacking rhodopsin phosphorylation.

9. Rapid diversification of cell signaling phenotypes by modular domain recombination.

10. Targeted Elimination of G Proteins and Arrestins Defines Their Specific Contributions to Both Intensity and Duration of G Protein-coupled Receptor Signaling.

Review 1. Plethora of functions packed into 45 kDa arrestins: biological implications and possible therapeutic strategies.

Review 2. Arrestin mutations: Some cause diseases, others promise cure.

Review 3. Structure and dynamics of GPCR signaling complexes.

Review 4. Arrestins: Introducing Signaling Bias Into Multifunctional Proteins.

Review 5. The structural basis of the arrestin binding to GPCRs.

6. Lysine in the lariat loop of arrestins does not serve as phosphate sensor.

Review 7. Molecular Mechanisms of GPCR Signaling: A Structural Perspective.

8. Critical role of the finger loop in arrestin binding to the receptors.

Review 9. GPCR Signaling Regulation: The Role of GRKs and Arrestins.