Deletion of the Fission Yeast Homologue of Human Insulinase Reveals a TORC1-Dependent Pathway Mediating Resistance to Proteotoxic Stress

Insulin Degrading Enzyme (IDE) is a protease conserved through evolution with a role in diabetes and Alzheimer's disease. The reason underlying its ubiquitous expression including cells lacking identified IDE substrates remains unknown. Here we show that the fission yeast IDE homologue (Iph1) m...

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Autores principales: Beuzelin, Clémentine, Evnouchidou, Irini, Rigolet, Pascal, Cauvet-Burgevin, Anne, Girard, Pierre-Marie, Dardalhon, Delphine, Culina, Slobodan, Gdoura, Abdelaziz, van Endert, Peter, Francesconi, Stefania
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3691139/
https://www.ncbi.nlm.nih.gov/pubmed/23826334
http://dx.doi.org/10.1371/journal.pone.0067705
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author Beuzelin, Clémentine
Evnouchidou, Irini
Rigolet, Pascal
Cauvet-Burgevin, Anne
Girard, Pierre-Marie
Dardalhon, Delphine
Culina, Slobodan
Gdoura, Abdelaziz
van Endert, Peter
Francesconi, Stefania
author_facet Beuzelin, Clémentine
Evnouchidou, Irini
Rigolet, Pascal
Cauvet-Burgevin, Anne
Girard, Pierre-Marie
Dardalhon, Delphine
Culina, Slobodan
Gdoura, Abdelaziz
van Endert, Peter
Francesconi, Stefania
author_sort Beuzelin, Clémentine
collection PubMed
description Insulin Degrading Enzyme (IDE) is a protease conserved through evolution with a role in diabetes and Alzheimer's disease. The reason underlying its ubiquitous expression including cells lacking identified IDE substrates remains unknown. Here we show that the fission yeast IDE homologue (Iph1) modulates cellular sensitivity to endoplasmic reticulum (ER) stress in a manner dependent on TORC1 (Target of Rapamycin Complex 1). Reduced sensitivity to tunicamycin was associated with a smaller number of cells undergoing apoptosis. Wild type levels of tunicamycin sensitivity were restored in iph1 null cells when the TORC1 complex was inhibited by rapamycin or by heat inactivation of the Tor2 kinase. Although Iph1 cleaved hallmark IDE substrates including insulin efficiently, its role in the ER stress response was independent of its catalytic activity since expression of inactive Iph1 restored normal sensitivity. Importantly, wild type as well as inactive human IDE complemented gene-invalidated yeast cells when expressed at the genomic locus under the control of iph1(+) promoter. These results suggest that IDE has a previously unknown function unrelated to substrate cleavage, which links sensitivity to ER stress to a pro-survival role of the TORC1 pathway.
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spelling pubmed-36911392013-07-03 Deletion of the Fission Yeast Homologue of Human Insulinase Reveals a TORC1-Dependent Pathway Mediating Resistance to Proteotoxic Stress Beuzelin, Clémentine Evnouchidou, Irini Rigolet, Pascal Cauvet-Burgevin, Anne Girard, Pierre-Marie Dardalhon, Delphine Culina, Slobodan Gdoura, Abdelaziz van Endert, Peter Francesconi, Stefania PLoS One Research Article Insulin Degrading Enzyme (IDE) is a protease conserved through evolution with a role in diabetes and Alzheimer's disease. The reason underlying its ubiquitous expression including cells lacking identified IDE substrates remains unknown. Here we show that the fission yeast IDE homologue (Iph1) modulates cellular sensitivity to endoplasmic reticulum (ER) stress in a manner dependent on TORC1 (Target of Rapamycin Complex 1). Reduced sensitivity to tunicamycin was associated with a smaller number of cells undergoing apoptosis. Wild type levels of tunicamycin sensitivity were restored in iph1 null cells when the TORC1 complex was inhibited by rapamycin or by heat inactivation of the Tor2 kinase. Although Iph1 cleaved hallmark IDE substrates including insulin efficiently, its role in the ER stress response was independent of its catalytic activity since expression of inactive Iph1 restored normal sensitivity. Importantly, wild type as well as inactive human IDE complemented gene-invalidated yeast cells when expressed at the genomic locus under the control of iph1(+) promoter. These results suggest that IDE has a previously unknown function unrelated to substrate cleavage, which links sensitivity to ER stress to a pro-survival role of the TORC1 pathway. Public Library of Science 2013-06-24 /pmc/articles/PMC3691139/ /pubmed/23826334 http://dx.doi.org/10.1371/journal.pone.0067705 Text en © 2013 Beuzelin et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Beuzelin, Clémentine
Evnouchidou, Irini
Rigolet, Pascal
Cauvet-Burgevin, Anne
Girard, Pierre-Marie
Dardalhon, Delphine
Culina, Slobodan
Gdoura, Abdelaziz
van Endert, Peter
Francesconi, Stefania
Deletion of the Fission Yeast Homologue of Human Insulinase Reveals a TORC1-Dependent Pathway Mediating Resistance to Proteotoxic Stress
title Deletion of the Fission Yeast Homologue of Human Insulinase Reveals a TORC1-Dependent Pathway Mediating Resistance to Proteotoxic Stress
title_full Deletion of the Fission Yeast Homologue of Human Insulinase Reveals a TORC1-Dependent Pathway Mediating Resistance to Proteotoxic Stress
title_fullStr Deletion of the Fission Yeast Homologue of Human Insulinase Reveals a TORC1-Dependent Pathway Mediating Resistance to Proteotoxic Stress
title_full_unstemmed Deletion of the Fission Yeast Homologue of Human Insulinase Reveals a TORC1-Dependent Pathway Mediating Resistance to Proteotoxic Stress
title_short Deletion of the Fission Yeast Homologue of Human Insulinase Reveals a TORC1-Dependent Pathway Mediating Resistance to Proteotoxic Stress
title_sort deletion of the fission yeast homologue of human insulinase reveals a torc1-dependent pathway mediating resistance to proteotoxic stress
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3691139/
https://www.ncbi.nlm.nih.gov/pubmed/23826334
http://dx.doi.org/10.1371/journal.pone.0067705
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