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Visualization of arrestin recruitment by a G Protein-Coupled Receptor

G Protein Coupled Receptors (GPCRs) are critically regulated by β-arrestins (βarrs), which not only desensitize G protein signaling but also initiate a G protein independent wave of signaling(1-5). A recent surge of structural data on a number of GPCRs, including the β(2) adrenergic receptor (β(2)AR...

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Autores principales: Shukla, Arun K., Westfield, Gerwin H., Xiao, Kunhong, Reis, Rosana I., Huang, Li-Yin, Tripathi-Shukla, Prachi, Qian, Jiang, Li, Sheng, Blanc, Adi, Oleskie, Austin N., Dosey, Anne M., Su, Min, Liang, Cui-Rong, Gu, Ling-Ling, Shan, Jin-Ming, Chen, Xin, Hanna, Rachel, Choi, Minjung, Yao, Xiao Jie, Klink, Bjoern U., Kahsai, Alem W., Sidhu, Sachdev S., Koide, Shohei, Penczek, Pawel A., Kossiakoff, Anthony A., Jr, Virgil L. Woods, Kobilka, Brian K., Skiniotis, Georgios, Lefkowitz, Robert J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4134437/
https://www.ncbi.nlm.nih.gov/pubmed/25043026
http://dx.doi.org/10.1038/nature13430
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author Shukla, Arun K.
Westfield, Gerwin H.
Xiao, Kunhong
Reis, Rosana I.
Huang, Li-Yin
Tripathi-Shukla, Prachi
Qian, Jiang
Li, Sheng
Blanc, Adi
Oleskie, Austin N.
Dosey, Anne M.
Su, Min
Liang, Cui-Rong
Gu, Ling-Ling
Shan, Jin-Ming
Chen, Xin
Hanna, Rachel
Choi, Minjung
Yao, Xiao Jie
Klink, Bjoern U.
Kahsai, Alem W.
Sidhu, Sachdev S.
Koide, Shohei
Penczek, Pawel A.
Kossiakoff, Anthony A.
Jr, Virgil L. Woods
Kobilka, Brian K.
Skiniotis, Georgios
Lefkowitz, Robert J.
author_facet Shukla, Arun K.
Westfield, Gerwin H.
Xiao, Kunhong
Reis, Rosana I.
Huang, Li-Yin
Tripathi-Shukla, Prachi
Qian, Jiang
Li, Sheng
Blanc, Adi
Oleskie, Austin N.
Dosey, Anne M.
Su, Min
Liang, Cui-Rong
Gu, Ling-Ling
Shan, Jin-Ming
Chen, Xin
Hanna, Rachel
Choi, Minjung
Yao, Xiao Jie
Klink, Bjoern U.
Kahsai, Alem W.
Sidhu, Sachdev S.
Koide, Shohei
Penczek, Pawel A.
Kossiakoff, Anthony A.
Jr, Virgil L. Woods
Kobilka, Brian K.
Skiniotis, Georgios
Lefkowitz, Robert J.
author_sort Shukla, Arun K.
collection PubMed
description G Protein Coupled Receptors (GPCRs) are critically regulated by β-arrestins (βarrs), which not only desensitize G protein signaling but also initiate a G protein independent wave of signaling(1-5). A recent surge of structural data on a number of GPCRs, including the β(2) adrenergic receptor (β(2)AR)-G protein complex, has provided novel insights into the structural basis of receptor activation(6-11). Lacking however has been complementary information on recruitment of βarrs to activated GPCRs primarily due to challenges in obtaining stable receptor-βarr complexes for structural studies. Here, we devised a strategy for forming and purifying a functional β(2)AR-βarr1 complex that allowed us to visualize its architecture by single particle negative stain electron microscopy (EM) and to characterize the interactions between β(2)AR and βarr1 using hydrogen-deuterium exchange mass spectrometry (HDXMS) and chemical cross-linking. EM 2D averages and 3D reconstructions reveal bimodal binding of βarr1 to the β(2)AR, involving two separate sets of interactions, one with the phosphorylated carboxy-terminus of the receptor and the other with its seven-transmembrane core. Areas of reduced HDX together with identification of cross-linked residues suggest engagement of the finger loop of βarr1 with the seven-transmembrane core of the receptor. In contrast, focal areas of increased HDX indicate regions of increased dynamics in both N and C domains of βarr1 when coupled to the β(2)AR. A molecular model of the β(2)AR-βarr signaling complex was made by docking activated βarr1 and β(2)AR crystal structures into the EM map densities with constraints provided by HDXMS and cross-linking, allowing us to obtain valuable insights into the overall architecture of a receptor-arrestin complex. The dynamic and structural information presented herein provides a framework for better understanding the basis of GPCR regulation by arrestins.
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spelling pubmed-41344372015-02-14 Visualization of arrestin recruitment by a G Protein-Coupled Receptor Shukla, Arun K. Westfield, Gerwin H. Xiao, Kunhong Reis, Rosana I. Huang, Li-Yin Tripathi-Shukla, Prachi Qian, Jiang Li, Sheng Blanc, Adi Oleskie, Austin N. Dosey, Anne M. Su, Min Liang, Cui-Rong Gu, Ling-Ling Shan, Jin-Ming Chen, Xin Hanna, Rachel Choi, Minjung Yao, Xiao Jie Klink, Bjoern U. Kahsai, Alem W. Sidhu, Sachdev S. Koide, Shohei Penczek, Pawel A. Kossiakoff, Anthony A. Jr, Virgil L. Woods Kobilka, Brian K. Skiniotis, Georgios Lefkowitz, Robert J. Nature Article G Protein Coupled Receptors (GPCRs) are critically regulated by β-arrestins (βarrs), which not only desensitize G protein signaling but also initiate a G protein independent wave of signaling(1-5). A recent surge of structural data on a number of GPCRs, including the β(2) adrenergic receptor (β(2)AR)-G protein complex, has provided novel insights into the structural basis of receptor activation(6-11). Lacking however has been complementary information on recruitment of βarrs to activated GPCRs primarily due to challenges in obtaining stable receptor-βarr complexes for structural studies. Here, we devised a strategy for forming and purifying a functional β(2)AR-βarr1 complex that allowed us to visualize its architecture by single particle negative stain electron microscopy (EM) and to characterize the interactions between β(2)AR and βarr1 using hydrogen-deuterium exchange mass spectrometry (HDXMS) and chemical cross-linking. EM 2D averages and 3D reconstructions reveal bimodal binding of βarr1 to the β(2)AR, involving two separate sets of interactions, one with the phosphorylated carboxy-terminus of the receptor and the other with its seven-transmembrane core. Areas of reduced HDX together with identification of cross-linked residues suggest engagement of the finger loop of βarr1 with the seven-transmembrane core of the receptor. In contrast, focal areas of increased HDX indicate regions of increased dynamics in both N and C domains of βarr1 when coupled to the β(2)AR. A molecular model of the β(2)AR-βarr signaling complex was made by docking activated βarr1 and β(2)AR crystal structures into the EM map densities with constraints provided by HDXMS and cross-linking, allowing us to obtain valuable insights into the overall architecture of a receptor-arrestin complex. The dynamic and structural information presented herein provides a framework for better understanding the basis of GPCR regulation by arrestins. 2014-06-22 2014-08-14 /pmc/articles/PMC4134437/ /pubmed/25043026 http://dx.doi.org/10.1038/nature13430 Text en http://www.nature.com/authors/editorial_policies/license.html#terms Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use:http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Shukla, Arun K.
Westfield, Gerwin H.
Xiao, Kunhong
Reis, Rosana I.
Huang, Li-Yin
Tripathi-Shukla, Prachi
Qian, Jiang
Li, Sheng
Blanc, Adi
Oleskie, Austin N.
Dosey, Anne M.
Su, Min
Liang, Cui-Rong
Gu, Ling-Ling
Shan, Jin-Ming
Chen, Xin
Hanna, Rachel
Choi, Minjung
Yao, Xiao Jie
Klink, Bjoern U.
Kahsai, Alem W.
Sidhu, Sachdev S.
Koide, Shohei
Penczek, Pawel A.
Kossiakoff, Anthony A.
Jr, Virgil L. Woods
Kobilka, Brian K.
Skiniotis, Georgios
Lefkowitz, Robert J.
Visualization of arrestin recruitment by a G Protein-Coupled Receptor
title Visualization of arrestin recruitment by a G Protein-Coupled Receptor
title_full Visualization of arrestin recruitment by a G Protein-Coupled Receptor
title_fullStr Visualization of arrestin recruitment by a G Protein-Coupled Receptor
title_full_unstemmed Visualization of arrestin recruitment by a G Protein-Coupled Receptor
title_short Visualization of arrestin recruitment by a G Protein-Coupled Receptor
title_sort visualization of arrestin recruitment by a g protein-coupled receptor
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4134437/
https://www.ncbi.nlm.nih.gov/pubmed/25043026
http://dx.doi.org/10.1038/nature13430
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