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Literature DB >> 28651823

Novel Structural Insights into GPCR-β-Arrestin Interaction and Signaling.

Ravi Ranjan¹, Hemlata Dwivedi¹, Mithu Baidya¹, Mohit Kumar¹, Arun K Shukla².

Abstract

G protein-coupled receptors (GPCRs) are major signal recognition and transmission units in the plasma membrane. The interaction of activated and phosphorylated GPCRs with the multifunctional adaptor proteins β-arrestins (βarrs) is crucial for regulation of their signaling and functional outcomes. Over the past few years, a range of structural, biochemical, and cellular studies have revealed novel insights into GPCR-βarr interaction and signaling. Some of these findings have come as a surprise and therefore have the potential to significantly refine the conceptual framework of the GPCR-βarr system. Here we discuss these recent advances with particular emphasis on biphasic GPCR-βarr interaction, the formation of GPCR-G-protein-βarr supercomplexes, and receptor-specific conformational signatures in βarrs. We also underline the emerging research areas that are likely to be at the center stage of investigations in the coming years.

Keywords: GPCRs; biased agonism; cellular signaling; desensitization; endocytosis; β-arrestins

Mesh：

Substances：

Year: 2017 PMID： 28651823 DOI： 10.1016/j.tcb.2017.05.008

Source DB: PubMed Journal: Trends Cell Biol ISSN： 0962-8924 Impact factor: 20.808

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Cited

34 in total

Review 1. Emerging Paradigm of Intracellular Targeting of G Protein-Coupled Receptors.

Authors: Madhu Chaturvedi; Justin Schilling; Alexandre Beautrait; Michel Bouvier; Jeffrey L Benovic; Arun K Shukla
Journal: Trends Biochem Sci Date: 2018-05-04 Impact factor: 13.807

2. Conformational Sensors and Domain Swapping Reveal Structural and Functional Differences between β-Arrestin Isoforms.

Authors: Eshan Ghosh; Hemlata Dwivedi; Mithu Baidya; Ashish Srivastava; Punita Kumari; Tomek Stepniewski; Hee Ryung Kim; Mi-Hye Lee; Jaana van Gastel; Madhu Chaturvedi; Debarati Roy; Shubhi Pandey; Jagannath Maharana; Ramon Guixà-González; Louis M Luttrell; Ka Young Chung; Somnath Dutta; Jana Selent; Arun K Shukla
Journal: Cell Rep Date: 2019-09-24 Impact factor: 9.423

3. Ligand-induced activation of ERK1/2 signaling by constitutively active G_s-coupled 5-HT receptors.

Authors: Ping Liu; Yu-Ling Yin; Ting Wang; Li Hou; Xiao-Xi Wang; Man Wang; Guan-Guan Zhao; Yi Shi; H Eric Xu; Yi Jiang
Journal: Acta Pharmacol Sin Date: 2019-03-04 Impact factor: 6.150

4. Genetic code expansion and photocross-linking identify different β-arrestin binding modes to the angiotensin II type 1 receptor.

Authors: Laurence Gagnon; Yubo Cao; Aaron Cho; Dana Sedki; Thomas Huber; Thomas P Sakmar; Stéphane A Laporte
Journal: J Biol Chem Date: 2019-09-17 Impact factor: 5.157

Review 5. Many faces of the GPCR-arrestin interaction.

Authors: Kiae Kim; Ka Young Chung
Journal: Arch Pharm Res Date: 2020-08-14 Impact factor: 4.946

Review 6. GPCR drug discovery: integrating solution NMR data with crystal and cryo-EM structures.

Authors: Ichio Shimada; Takumi Ueda; Yutaka Kofuku; Matthew T Eddy; Kurt Wüthrich
Journal: Nat Rev Drug Discov Date: 2018-11-09 Impact factor: 84.694

7. Preferential Small Intestine Homing and Persistence of CD8 T Cells in Rhesus Macaques Achieved by Molecularly Engineered Expression of CCR9 and Reduced Ex Vivo Manipulation.

Authors: Matthew T Trivett; James D Burke; Claire Deleage; Lori V Coren; Brenna J Hill; Sumiti Jain; Eugene V Barsov; Matthew W Breed; Joshua A Kramer; Gregory Q Del Prete; Jeffrey D Lifson; Adrienne E Swanstrom; David E Ott
Journal: J Virol Date: 2019-10-15 Impact factor: 5.103

Novel Structural Insights into GPCR-β-Arrestin Interaction and Signaling.

Review 1. Emerging Paradigm of Intracellular Targeting of G Protein-Coupled Receptors.

2. Conformational Sensors and Domain Swapping Reveal Structural and Functional Differences between β-Arrestin Isoforms.

3. Ligand-induced activation of ERK1/2 signaling by constitutively active G_s-coupled 5-HT receptors.

4. Genetic code expansion and photocross-linking identify different β-arrestin binding modes to the angiotensin II type 1 receptor.

Review 5. Many faces of the GPCR-arrestin interaction.

Review 6. GPCR drug discovery: integrating solution NMR data with crystal and cryo-EM structures.

7. Preferential Small Intestine Homing and Persistence of CD8 T Cells in Rhesus Macaques Achieved by Molecularly Engineered Expression of CCR9 and Reduced Ex Vivo Manipulation.

Review 8. Metabotropic glutamate receptor trafficking.

9. Partial ligand-receptor engagement yields functional bias at the human complement receptor, C5aR1.

10. Reversible biotinylation of purified proteins for measuring protein-protein interactions.

Novel Structural Insights into GPCR-β-Arrestin Interaction and Signaling.

Review 1. Emerging Paradigm of Intracellular Targeting of G Protein-Coupled Receptors.

2. Conformational Sensors and Domain Swapping Reveal Structural and Functional Differences between β-Arrestin Isoforms.

3. Ligand-induced activation of ERK1/2 signaling by constitutively active Gs-coupled 5-HT receptors.

4. Genetic code expansion and photocross-linking identify different β-arrestin binding modes to the angiotensin II type 1 receptor.

Review 5. Many faces of the GPCR-arrestin interaction.

Review 6. GPCR drug discovery: integrating solution NMR data with crystal and cryo-EM structures.

7. Preferential Small Intestine Homing and Persistence of CD8 T Cells in Rhesus Macaques Achieved by Molecularly Engineered Expression of CCR9 and Reduced Ex Vivo Manipulation.

Review 8. Metabotropic glutamate receptor trafficking.

9. Partial ligand-receptor engagement yields functional bias at the human complement receptor, C5aR1.

10. Reversible biotinylation of purified proteins for measuring protein-protein interactions.

3. Ligand-induced activation of ERK1/2 signaling by constitutively active G_s-coupled 5-HT receptors.