Structure of the Ire1 autophosphorylation complex and implications for the unfolded protein response

Ire1 (Ern1) is an unusual transmembrane protein kinase essential for the endoplasmic reticulum (ER) unfolded protein response (UPR). Activation of Ire1 by association of its N-terminal ER luminal domains promotes autophosphorylation by its cytoplasmic kinase domain, leading to activation of the C-te...

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Autores principales: Ali, Maruf M U, Bagratuni, Tina, Davenport, Emma L, Nowak, Piotr R, Silva-Santisteban, M Cris, Hardcastle, Anthea, McAndrews, Craig, Rowlands, Martin G, Morgan, Gareth J, Aherne, Wynne, Collins, Ian, Davies, Faith E, Pearl, Laurence H
Formato: Texto
Lenguaje:English
Publicado: Nature Publishing Group 2011
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3049214/
https://www.ncbi.nlm.nih.gov/pubmed/21317875
http://dx.doi.org/10.1038/emboj.2011.18
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author Ali, Maruf M U
Bagratuni, Tina
Davenport, Emma L
Nowak, Piotr R
Silva-Santisteban, M Cris
Hardcastle, Anthea
McAndrews, Craig
Rowlands, Martin G
Morgan, Gareth J
Aherne, Wynne
Collins, Ian
Davies, Faith E
Pearl, Laurence H
author_facet Ali, Maruf M U
Bagratuni, Tina
Davenport, Emma L
Nowak, Piotr R
Silva-Santisteban, M Cris
Hardcastle, Anthea
McAndrews, Craig
Rowlands, Martin G
Morgan, Gareth J
Aherne, Wynne
Collins, Ian
Davies, Faith E
Pearl, Laurence H
author_sort Ali, Maruf M U
collection PubMed
description Ire1 (Ern1) is an unusual transmembrane protein kinase essential for the endoplasmic reticulum (ER) unfolded protein response (UPR). Activation of Ire1 by association of its N-terminal ER luminal domains promotes autophosphorylation by its cytoplasmic kinase domain, leading to activation of the C-terminal ribonuclease domain, which splices Xbp1 mRNA generating an active Xbp1s transcriptional activator. We have determined the crystal structure of the cytoplasmic portion of dephosphorylated human Ire1α bound to ADP, revealing the ‘phosphoryl-transfer' competent dimeric face-to-face complex, which precedes and is distinct from the back-to-back RNase ‘active' conformation described for yeast Ire1. We show that the Xbp1-specific ribonuclease activity depends on autophosphorylation, and that ATP-competitive inhibitors staurosporin and sunitinib, which inhibit autophosphorylation in vitro, also inhibit Xbp1 splicing in vivo. Furthermore, we demonstrate that activated Ire1α is a competent protein kinase, able to phosphorylate a heterologous peptide substrate. These studies identify human Ire1α as a target for development of ATP-competitive inhibitors that will modulate the UPR in human cells, which has particular relevance for myeloma and other secretory malignancies.
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spelling pubmed-30492142011-04-14 Structure of the Ire1 autophosphorylation complex and implications for the unfolded protein response Ali, Maruf M U Bagratuni, Tina Davenport, Emma L Nowak, Piotr R Silva-Santisteban, M Cris Hardcastle, Anthea McAndrews, Craig Rowlands, Martin G Morgan, Gareth J Aherne, Wynne Collins, Ian Davies, Faith E Pearl, Laurence H EMBO J Article Ire1 (Ern1) is an unusual transmembrane protein kinase essential for the endoplasmic reticulum (ER) unfolded protein response (UPR). Activation of Ire1 by association of its N-terminal ER luminal domains promotes autophosphorylation by its cytoplasmic kinase domain, leading to activation of the C-terminal ribonuclease domain, which splices Xbp1 mRNA generating an active Xbp1s transcriptional activator. We have determined the crystal structure of the cytoplasmic portion of dephosphorylated human Ire1α bound to ADP, revealing the ‘phosphoryl-transfer' competent dimeric face-to-face complex, which precedes and is distinct from the back-to-back RNase ‘active' conformation described for yeast Ire1. We show that the Xbp1-specific ribonuclease activity depends on autophosphorylation, and that ATP-competitive inhibitors staurosporin and sunitinib, which inhibit autophosphorylation in vitro, also inhibit Xbp1 splicing in vivo. Furthermore, we demonstrate that activated Ire1α is a competent protein kinase, able to phosphorylate a heterologous peptide substrate. These studies identify human Ire1α as a target for development of ATP-competitive inhibitors that will modulate the UPR in human cells, which has particular relevance for myeloma and other secretory malignancies. Nature Publishing Group 2011-03-02 2011-02-11 /pmc/articles/PMC3049214/ /pubmed/21317875 http://dx.doi.org/10.1038/emboj.2011.18 Text en Copyright © 2011, European Molecular Biology Organization http://creativecommons.org/licenses/by-nc-nd/3.0 This is an open-access article distributed under the terms of the Creative Commons Attribution Noncommercial No Derivative Works 3.0 Unported License, which permits distribution and reproduction in any medium, provided the original author and source are credited. This license does not permit commercial exploitation or the creation of derivative works without specific permission.
spellingShingle Article
Ali, Maruf M U
Bagratuni, Tina
Davenport, Emma L
Nowak, Piotr R
Silva-Santisteban, M Cris
Hardcastle, Anthea
McAndrews, Craig
Rowlands, Martin G
Morgan, Gareth J
Aherne, Wynne
Collins, Ian
Davies, Faith E
Pearl, Laurence H
Structure of the Ire1 autophosphorylation complex and implications for the unfolded protein response
title Structure of the Ire1 autophosphorylation complex and implications for the unfolded protein response
title_full Structure of the Ire1 autophosphorylation complex and implications for the unfolded protein response
title_fullStr Structure of the Ire1 autophosphorylation complex and implications for the unfolded protein response
title_full_unstemmed Structure of the Ire1 autophosphorylation complex and implications for the unfolded protein response
title_short Structure of the Ire1 autophosphorylation complex and implications for the unfolded protein response
title_sort structure of the ire1 autophosphorylation complex and implications for the unfolded protein response
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3049214/
https://www.ncbi.nlm.nih.gov/pubmed/21317875
http://dx.doi.org/10.1038/emboj.2011.18
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