Neuroserpin polymers cause oxidative stress in a neuronal model of the dementia FENIB

The serpinopathies are human pathologies caused by mutations that promote polymerisation and intracellular deposition of proteins of the serpin superfamily, leading to a poorly understood cell toxicity. The dementia FENIB is caused by polymerisation of the neuronal serpin neuroserpin (NS) within the...

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Autores principales: Guadagno, Noemi A., Moriconi, Claudia, Licursi, Valerio, D'Acunto, Emanuela, Nisi, Paola S., Carucci, Nicoletta, De Jaco, Antonella, Cacci, Emanuele, Negri, Rodolfo, Lupo, Giuseppe, Miranda, Elena
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Academic Press 2017
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5439028/
https://www.ncbi.nlm.nih.gov/pubmed/28363799
http://dx.doi.org/10.1016/j.nbd.2017.03.010
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author Guadagno, Noemi A.
Moriconi, Claudia
Licursi, Valerio
D'Acunto, Emanuela
Nisi, Paola S.
Carucci, Nicoletta
De Jaco, Antonella
Cacci, Emanuele
Negri, Rodolfo
Lupo, Giuseppe
Miranda, Elena
author_facet Guadagno, Noemi A.
Moriconi, Claudia
Licursi, Valerio
D'Acunto, Emanuela
Nisi, Paola S.
Carucci, Nicoletta
De Jaco, Antonella
Cacci, Emanuele
Negri, Rodolfo
Lupo, Giuseppe
Miranda, Elena
author_sort Guadagno, Noemi A.
collection PubMed
description The serpinopathies are human pathologies caused by mutations that promote polymerisation and intracellular deposition of proteins of the serpin superfamily, leading to a poorly understood cell toxicity. The dementia FENIB is caused by polymerisation of the neuronal serpin neuroserpin (NS) within the endoplasmic reticulum (ER) of neurons. With the aim of understanding the toxicity due to intracellular accumulation of neuroserpin polymers, we have generated transgenic neural progenitor cell (NPC) cultures from mouse foetal cerebral cortex, stably expressing the control protein GFP (green fluorescent protein), or human wild type, G392E or delta NS. We have characterised these cell lines in the proliferative state and after differentiation to neurons. Our results show that G392E NS formed polymers that were mostly retained within the ER, while wild type NS was correctly secreted as a monomeric protein into the culture medium. Delta NS was absent at steady state due to its rapid degradation, but it was easily detected upon proteasomal block. Looking at their intracellular distribution, wild type NS was found in partial co-localisation with ER and Golgi markers, while G392E NS was localised within the ER only. Furthermore, polymers of NS were detected by ELISA and immunofluorescence in neurons expressing the mutant but not the wild type protein. We used control GFP and G392E NPCs differentiated to neurons to investigate which cellular pathways were modulated by intracellular polymers by performing RNA sequencing. We identified 747 genes with a significant upregulation (623) or downregulation (124) in G392E NS-expressing cells, and we focused our attention on several genes involved in the defence against oxidative stress that were up-regulated in cells expressing G392E NS (Aldh1b1, Apoe, Gpx1, Gstm1, Prdx6, Scara3, Sod2). Inhibition of intracellular anti-oxidants by specific pharmacological reagents uncovered the damaging effects of NS polymers. Our results support a role for oxidative stress in the cellular toxicity underlying the neurodegenerative dementia FENIB.
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spelling pubmed-54390282017-07-01 Neuroserpin polymers cause oxidative stress in a neuronal model of the dementia FENIB Guadagno, Noemi A. Moriconi, Claudia Licursi, Valerio D'Acunto, Emanuela Nisi, Paola S. Carucci, Nicoletta De Jaco, Antonella Cacci, Emanuele Negri, Rodolfo Lupo, Giuseppe Miranda, Elena Neurobiol Dis Article The serpinopathies are human pathologies caused by mutations that promote polymerisation and intracellular deposition of proteins of the serpin superfamily, leading to a poorly understood cell toxicity. The dementia FENIB is caused by polymerisation of the neuronal serpin neuroserpin (NS) within the endoplasmic reticulum (ER) of neurons. With the aim of understanding the toxicity due to intracellular accumulation of neuroserpin polymers, we have generated transgenic neural progenitor cell (NPC) cultures from mouse foetal cerebral cortex, stably expressing the control protein GFP (green fluorescent protein), or human wild type, G392E or delta NS. We have characterised these cell lines in the proliferative state and after differentiation to neurons. Our results show that G392E NS formed polymers that were mostly retained within the ER, while wild type NS was correctly secreted as a monomeric protein into the culture medium. Delta NS was absent at steady state due to its rapid degradation, but it was easily detected upon proteasomal block. Looking at their intracellular distribution, wild type NS was found in partial co-localisation with ER and Golgi markers, while G392E NS was localised within the ER only. Furthermore, polymers of NS were detected by ELISA and immunofluorescence in neurons expressing the mutant but not the wild type protein. We used control GFP and G392E NPCs differentiated to neurons to investigate which cellular pathways were modulated by intracellular polymers by performing RNA sequencing. We identified 747 genes with a significant upregulation (623) or downregulation (124) in G392E NS-expressing cells, and we focused our attention on several genes involved in the defence against oxidative stress that were up-regulated in cells expressing G392E NS (Aldh1b1, Apoe, Gpx1, Gstm1, Prdx6, Scara3, Sod2). Inhibition of intracellular anti-oxidants by specific pharmacological reagents uncovered the damaging effects of NS polymers. Our results support a role for oxidative stress in the cellular toxicity underlying the neurodegenerative dementia FENIB. Academic Press 2017-07 /pmc/articles/PMC5439028/ /pubmed/28363799 http://dx.doi.org/10.1016/j.nbd.2017.03.010 Text en © 2017 The Authors http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Article
Guadagno, Noemi A.
Moriconi, Claudia
Licursi, Valerio
D'Acunto, Emanuela
Nisi, Paola S.
Carucci, Nicoletta
De Jaco, Antonella
Cacci, Emanuele
Negri, Rodolfo
Lupo, Giuseppe
Miranda, Elena
Neuroserpin polymers cause oxidative stress in a neuronal model of the dementia FENIB
title Neuroserpin polymers cause oxidative stress in a neuronal model of the dementia FENIB
title_full Neuroserpin polymers cause oxidative stress in a neuronal model of the dementia FENIB
title_fullStr Neuroserpin polymers cause oxidative stress in a neuronal model of the dementia FENIB
title_full_unstemmed Neuroserpin polymers cause oxidative stress in a neuronal model of the dementia FENIB
title_short Neuroserpin polymers cause oxidative stress in a neuronal model of the dementia FENIB
title_sort neuroserpin polymers cause oxidative stress in a neuronal model of the dementia fenib
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5439028/
https://www.ncbi.nlm.nih.gov/pubmed/28363799
http://dx.doi.org/10.1016/j.nbd.2017.03.010
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