Ero1α-Dependent ERp44 Dissociation From RyR2 Contributes to Cardiac Arrhythmia

Oxidative stress in cardiac disease promotes proarrhythmic disturbances in Ca(2+) homeostasis, impairing luminal Ca(2+) regulation of the sarcoplasmic reticulum (SR) Ca(2+) release channel, the RyR2 (ryanodine receptor), and increasing channel activity. However, exact mechanisms underlying redox-med...

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Autores principales: Hamilton, Shanna, Terentyeva, Radmila, Bogdanov, Vladimir, Kim, Tae Yun, Perger, Fruzsina, Yan, Jiajie, Ai, Xun, Carnes, Cynthia A., Belevych, Andriy E., George, Christopher H., Davis, Jonathan P., Gyorke, Sandor, Choi, Bum-Rak, Terentyev, Dmitry
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Lippincott Williams & Wilkins 2022
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8893133/
https://www.ncbi.nlm.nih.gov/pubmed/35086342
http://dx.doi.org/10.1161/CIRCRESAHA.121.320531
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author Hamilton, Shanna
Terentyeva, Radmila
Bogdanov, Vladimir
Kim, Tae Yun
Perger, Fruzsina
Yan, Jiajie
Ai, Xun
Carnes, Cynthia A.
Belevych, Andriy E.
George, Christopher H.
Davis, Jonathan P.
Gyorke, Sandor
Choi, Bum-Rak
Terentyev, Dmitry
author_facet Hamilton, Shanna
Terentyeva, Radmila
Bogdanov, Vladimir
Kim, Tae Yun
Perger, Fruzsina
Yan, Jiajie
Ai, Xun
Carnes, Cynthia A.
Belevych, Andriy E.
George, Christopher H.
Davis, Jonathan P.
Gyorke, Sandor
Choi, Bum-Rak
Terentyev, Dmitry
author_sort Hamilton, Shanna
collection PubMed
description Oxidative stress in cardiac disease promotes proarrhythmic disturbances in Ca(2+) homeostasis, impairing luminal Ca(2+) regulation of the sarcoplasmic reticulum (SR) Ca(2+) release channel, the RyR2 (ryanodine receptor), and increasing channel activity. However, exact mechanisms underlying redox-mediated increase of RyR2 function in cardiac disease remain elusive. We tested whether the oxidoreductase family of proteins that dynamically regulate the oxidative environment within the SR are involved in this process. METHODS: A rat model of hypertrophy induced by thoracic aortic banding (TAB) was used for ex vivo whole heart optical mapping and for Ca(2+) and reactive oxygen species imaging in isolated ventricular myocytes (VMs). RESULTS: The SR-targeted reactive oxygen species biosensor ERroGFP showed increased intra-SR oxidation in TAB VMs that was associated with increased expression of Ero1α (endoplasmic reticulum oxidoreductase 1 alpha). Pharmacological (EN460) or genetic Ero1α inhibition normalized SR redox state, increased Ca(2+) transient amplitude and SR Ca(2+) content, and reduced proarrhythmic spontaneous Ca(2+) waves in TAB VMs under β-adrenergic stimulation (isoproterenol). Ero1α overexpression in Sham VMs had opposite effects. Ero1α inhibition attenuated Ca(2+)-dependent ventricular tachyarrhythmias in TAB hearts challenged with isoproterenol. Experiments in TAB VMs and human embryonic kidney 293 cells expressing human RyR2 revealed that an Ero1α-mediated increase in SR Ca(2+)-channel activity involves dissociation of intraluminal protein ERp44 (endoplasmic reticulum protein 44) from the RyR2 complex. Site-directed mutagenesis and molecular dynamics simulations demonstrated a novel redox-sensitive association of ERp44 with RyR2 mediated by intraluminal cysteine 4806. ERp44-RyR2 association in TAB VMs was restored by Ero1α inhibition, but not by reducing agent dithiothreitol, as hypo-oxidation precludes formation of covalent bond between RyR2 and ERp44. CONCLUSIONS: A novel axis of intraluminal interaction between RyR2, ERp44, and Ero1α has been identified. Ero1α inhibition exhibits promising therapeutic potential by stabilizing RyR2-ERp44 complex, thereby reducing spontaneous Ca(2+) release and Ca(2+)-dependent tachyarrhythmias in hypertrophic hearts, without causing hypo-oxidative stress in the SR.
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spelling pubmed-88931332022-03-10 Ero1α-Dependent ERp44 Dissociation From RyR2 Contributes to Cardiac Arrhythmia Hamilton, Shanna Terentyeva, Radmila Bogdanov, Vladimir Kim, Tae Yun Perger, Fruzsina Yan, Jiajie Ai, Xun Carnes, Cynthia A. Belevych, Andriy E. George, Christopher H. Davis, Jonathan P. Gyorke, Sandor Choi, Bum-Rak Terentyev, Dmitry Circ Res Original Research Oxidative stress in cardiac disease promotes proarrhythmic disturbances in Ca(2+) homeostasis, impairing luminal Ca(2+) regulation of the sarcoplasmic reticulum (SR) Ca(2+) release channel, the RyR2 (ryanodine receptor), and increasing channel activity. However, exact mechanisms underlying redox-mediated increase of RyR2 function in cardiac disease remain elusive. We tested whether the oxidoreductase family of proteins that dynamically regulate the oxidative environment within the SR are involved in this process. METHODS: A rat model of hypertrophy induced by thoracic aortic banding (TAB) was used for ex vivo whole heart optical mapping and for Ca(2+) and reactive oxygen species imaging in isolated ventricular myocytes (VMs). RESULTS: The SR-targeted reactive oxygen species biosensor ERroGFP showed increased intra-SR oxidation in TAB VMs that was associated with increased expression of Ero1α (endoplasmic reticulum oxidoreductase 1 alpha). Pharmacological (EN460) or genetic Ero1α inhibition normalized SR redox state, increased Ca(2+) transient amplitude and SR Ca(2+) content, and reduced proarrhythmic spontaneous Ca(2+) waves in TAB VMs under β-adrenergic stimulation (isoproterenol). Ero1α overexpression in Sham VMs had opposite effects. Ero1α inhibition attenuated Ca(2+)-dependent ventricular tachyarrhythmias in TAB hearts challenged with isoproterenol. Experiments in TAB VMs and human embryonic kidney 293 cells expressing human RyR2 revealed that an Ero1α-mediated increase in SR Ca(2+)-channel activity involves dissociation of intraluminal protein ERp44 (endoplasmic reticulum protein 44) from the RyR2 complex. Site-directed mutagenesis and molecular dynamics simulations demonstrated a novel redox-sensitive association of ERp44 with RyR2 mediated by intraluminal cysteine 4806. ERp44-RyR2 association in TAB VMs was restored by Ero1α inhibition, but not by reducing agent dithiothreitol, as hypo-oxidation precludes formation of covalent bond between RyR2 and ERp44. CONCLUSIONS: A novel axis of intraluminal interaction between RyR2, ERp44, and Ero1α has been identified. Ero1α inhibition exhibits promising therapeutic potential by stabilizing RyR2-ERp44 complex, thereby reducing spontaneous Ca(2+) release and Ca(2+)-dependent tachyarrhythmias in hypertrophic hearts, without causing hypo-oxidative stress in the SR. Lippincott Williams & Wilkins 2022-01-28 2022-03-04 /pmc/articles/PMC8893133/ /pubmed/35086342 http://dx.doi.org/10.1161/CIRCRESAHA.121.320531 Text en © 2022 The Authors. https://creativecommons.org/licenses/by-nc-nd/4.0/Circulation Research is published on behalf of the American Heart Association, Inc., by Wolters Kluwer Health, Inc. This is an open access article under the terms of the Creative Commons Attribution Non-Commercial-NoDerivs (https://creativecommons.org/licenses/by-nc-nd/4.0/) License, which permits use, distribution, and reproduction in any medium, provided that the original work is properly cited, the use is noncommercial, and no modifications or adaptations are made.
spellingShingle Original Research
Hamilton, Shanna
Terentyeva, Radmila
Bogdanov, Vladimir
Kim, Tae Yun
Perger, Fruzsina
Yan, Jiajie
Ai, Xun
Carnes, Cynthia A.
Belevych, Andriy E.
George, Christopher H.
Davis, Jonathan P.
Gyorke, Sandor
Choi, Bum-Rak
Terentyev, Dmitry
Ero1α-Dependent ERp44 Dissociation From RyR2 Contributes to Cardiac Arrhythmia
title Ero1α-Dependent ERp44 Dissociation From RyR2 Contributes to Cardiac Arrhythmia
title_full Ero1α-Dependent ERp44 Dissociation From RyR2 Contributes to Cardiac Arrhythmia
title_fullStr Ero1α-Dependent ERp44 Dissociation From RyR2 Contributes to Cardiac Arrhythmia
title_full_unstemmed Ero1α-Dependent ERp44 Dissociation From RyR2 Contributes to Cardiac Arrhythmia
title_short Ero1α-Dependent ERp44 Dissociation From RyR2 Contributes to Cardiac Arrhythmia
title_sort ero1α-dependent erp44 dissociation from ryr2 contributes to cardiac arrhythmia
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8893133/
https://www.ncbi.nlm.nih.gov/pubmed/35086342
http://dx.doi.org/10.1161/CIRCRESAHA.121.320531
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