Protein synthesis inhibition and loss of homeostatic functions in astrocytes from an Alzheimer’s disease mouse model: a role for ER-mitochondria interaction

Deregulation of protein synthesis and ER stress/unfolded protein response (ER stress/UPR) have been reported in astrocytes. However, the relationships between protein synthesis deregulation and ER stress/UPR, as well as their role in the altered homeostatic support of Alzheimer’s disease (AD) astroc...

Descripción completa

Detalles Bibliográficos
Autores principales: Tapella, Laura, Dematteis, Giulia, Moro, Marianna, Pistolato, Beatrice, Tonelli, Elisa, Vanella, Virginia Vita, Giustina, Daniele, La Forgia, Aleida, Restelli, Elena, Barberis, Elettra, Cali, Tito, Brini, Marisa, Villani, Salvatore, Del Grosso, Erika, Grilli, Mariagrazia, Manfredi, Marcello, Corazzari, Marco, Grolla, Ambra A., Genazzani, Armando A., Lim, Dmitry
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group UK 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9579125/
https://www.ncbi.nlm.nih.gov/pubmed/36257957
http://dx.doi.org/10.1038/s41419-022-05324-4
_version_ 1784812117274132480
author Tapella, Laura
Dematteis, Giulia
Moro, Marianna
Pistolato, Beatrice
Tonelli, Elisa
Vanella, Virginia Vita
Giustina, Daniele
La Forgia, Aleida
Restelli, Elena
Barberis, Elettra
Cali, Tito
Brini, Marisa
Villani, Salvatore
Del Grosso, Erika
Grilli, Mariagrazia
Manfredi, Marcello
Corazzari, Marco
Grolla, Ambra A.
Genazzani, Armando A.
Lim, Dmitry
author_facet Tapella, Laura
Dematteis, Giulia
Moro, Marianna
Pistolato, Beatrice
Tonelli, Elisa
Vanella, Virginia Vita
Giustina, Daniele
La Forgia, Aleida
Restelli, Elena
Barberis, Elettra
Cali, Tito
Brini, Marisa
Villani, Salvatore
Del Grosso, Erika
Grilli, Mariagrazia
Manfredi, Marcello
Corazzari, Marco
Grolla, Ambra A.
Genazzani, Armando A.
Lim, Dmitry
author_sort Tapella, Laura
collection PubMed
description Deregulation of protein synthesis and ER stress/unfolded protein response (ER stress/UPR) have been reported in astrocytes. However, the relationships between protein synthesis deregulation and ER stress/UPR, as well as their role in the altered homeostatic support of Alzheimer’s disease (AD) astrocytes remain poorly understood. Previously, we reported that in astrocytic cell lines from 3xTg-AD mice (3Tg-iAstro) protein synthesis was impaired and ER-mitochondria distance was reduced. Here we show that impaired protein synthesis in 3Tg-iAstro is associated with an increase of p-eIF2α and downregulation of GADD34. Although mRNA levels of ER stress/UPR markers were increased two-three-fold, we found neither activation of PERK nor downstream induction of ATF4 protein. Strikingly, the overexpression of a synthetic ER-mitochondrial linker (EML) resulted in a reduced protein synthesis and augmented p-eIF2α without any effect on ER stress/UPR marker genes. In vivo, in hippocampi of 3xTg-AD mice, reduced protein synthesis, increased p-eIF2α and downregulated GADD34 protein were found, while no increase of p-PERK or ATF4 proteins was observed, suggesting that in AD astrocytes, both in vitro and in vivo, phosphorylation of eIF2α and impairment of protein synthesis are PERK-independent. Next, we investigated the ability of 3xTg-AD astrocytes to support metabolism and function of other cells of the central nervous system. Astrocyte-conditioned medium (ACM) from 3Tg-iAstro cells significantly reduced protein synthesis rate in primary hippocampal neurons. When added as a part of pericyte/endothelial cell (EC)/astrocyte 3D co-culture, 3Tg-iAstro, but not WT-iAstro, severely impaired formation and ramification of tubules, the effect, replicated by EML overexpression in WT-iAstro cells. Finally, a chemical chaperone 4-phenylbutyric acid (4-PBA) rescued protein synthesis, p-eIF2α levels in 3Tg-iAstro cells and tubulogenesis in pericyte/EC/3Tg-iAstro co-culture. Collectively, our results suggest that a PERK-independent, p-eIF2α-associated impairment of protein synthesis compromises astrocytic homeostatic functions, and this may be caused by the altered ER-mitochondria interaction.
format Online
Article
Text
id pubmed-9579125
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Nature Publishing Group UK
record_format MEDLINE/PubMed
spelling pubmed-95791252022-10-20 Protein synthesis inhibition and loss of homeostatic functions in astrocytes from an Alzheimer’s disease mouse model: a role for ER-mitochondria interaction Tapella, Laura Dematteis, Giulia Moro, Marianna Pistolato, Beatrice Tonelli, Elisa Vanella, Virginia Vita Giustina, Daniele La Forgia, Aleida Restelli, Elena Barberis, Elettra Cali, Tito Brini, Marisa Villani, Salvatore Del Grosso, Erika Grilli, Mariagrazia Manfredi, Marcello Corazzari, Marco Grolla, Ambra A. Genazzani, Armando A. Lim, Dmitry Cell Death Dis Article Deregulation of protein synthesis and ER stress/unfolded protein response (ER stress/UPR) have been reported in astrocytes. However, the relationships between protein synthesis deregulation and ER stress/UPR, as well as their role in the altered homeostatic support of Alzheimer’s disease (AD) astrocytes remain poorly understood. Previously, we reported that in astrocytic cell lines from 3xTg-AD mice (3Tg-iAstro) protein synthesis was impaired and ER-mitochondria distance was reduced. Here we show that impaired protein synthesis in 3Tg-iAstro is associated with an increase of p-eIF2α and downregulation of GADD34. Although mRNA levels of ER stress/UPR markers were increased two-three-fold, we found neither activation of PERK nor downstream induction of ATF4 protein. Strikingly, the overexpression of a synthetic ER-mitochondrial linker (EML) resulted in a reduced protein synthesis and augmented p-eIF2α without any effect on ER stress/UPR marker genes. In vivo, in hippocampi of 3xTg-AD mice, reduced protein synthesis, increased p-eIF2α and downregulated GADD34 protein were found, while no increase of p-PERK or ATF4 proteins was observed, suggesting that in AD astrocytes, both in vitro and in vivo, phosphorylation of eIF2α and impairment of protein synthesis are PERK-independent. Next, we investigated the ability of 3xTg-AD astrocytes to support metabolism and function of other cells of the central nervous system. Astrocyte-conditioned medium (ACM) from 3Tg-iAstro cells significantly reduced protein synthesis rate in primary hippocampal neurons. When added as a part of pericyte/endothelial cell (EC)/astrocyte 3D co-culture, 3Tg-iAstro, but not WT-iAstro, severely impaired formation and ramification of tubules, the effect, replicated by EML overexpression in WT-iAstro cells. Finally, a chemical chaperone 4-phenylbutyric acid (4-PBA) rescued protein synthesis, p-eIF2α levels in 3Tg-iAstro cells and tubulogenesis in pericyte/EC/3Tg-iAstro co-culture. Collectively, our results suggest that a PERK-independent, p-eIF2α-associated impairment of protein synthesis compromises astrocytic homeostatic functions, and this may be caused by the altered ER-mitochondria interaction. Nature Publishing Group UK 2022-10-18 /pmc/articles/PMC9579125/ /pubmed/36257957 http://dx.doi.org/10.1038/s41419-022-05324-4 Text en © The Author(s) 2022 https://creativecommons.org/licenses/by/4.0/Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Article
Tapella, Laura
Dematteis, Giulia
Moro, Marianna
Pistolato, Beatrice
Tonelli, Elisa
Vanella, Virginia Vita
Giustina, Daniele
La Forgia, Aleida
Restelli, Elena
Barberis, Elettra
Cali, Tito
Brini, Marisa
Villani, Salvatore
Del Grosso, Erika
Grilli, Mariagrazia
Manfredi, Marcello
Corazzari, Marco
Grolla, Ambra A.
Genazzani, Armando A.
Lim, Dmitry
Protein synthesis inhibition and loss of homeostatic functions in astrocytes from an Alzheimer’s disease mouse model: a role for ER-mitochondria interaction
title Protein synthesis inhibition and loss of homeostatic functions in astrocytes from an Alzheimer’s disease mouse model: a role for ER-mitochondria interaction
title_full Protein synthesis inhibition and loss of homeostatic functions in astrocytes from an Alzheimer’s disease mouse model: a role for ER-mitochondria interaction
title_fullStr Protein synthesis inhibition and loss of homeostatic functions in astrocytes from an Alzheimer’s disease mouse model: a role for ER-mitochondria interaction
title_full_unstemmed Protein synthesis inhibition and loss of homeostatic functions in astrocytes from an Alzheimer’s disease mouse model: a role for ER-mitochondria interaction
title_short Protein synthesis inhibition and loss of homeostatic functions in astrocytes from an Alzheimer’s disease mouse model: a role for ER-mitochondria interaction
title_sort protein synthesis inhibition and loss of homeostatic functions in astrocytes from an alzheimer’s disease mouse model: a role for er-mitochondria interaction
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9579125/
https://www.ncbi.nlm.nih.gov/pubmed/36257957
http://dx.doi.org/10.1038/s41419-022-05324-4
work_keys_str_mv AT tapellalaura proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT dematteisgiulia proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT moromarianna proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT pistolatobeatrice proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT tonellielisa proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT vanellavirginiavita proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT giustinadaniele proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT laforgiaaleida proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT restellielena proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT barberiselettra proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT calitito proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT brinimarisa proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT villanisalvatore proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT delgrossoerika proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT grillimariagrazia proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT manfredimarcello proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT corazzarimarco proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT grollaambraa proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT genazzaniarmandoa proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction
AT limdmitry proteinsynthesisinhibitionandlossofhomeostaticfunctionsinastrocytesfromanalzheimersdiseasemousemodelaroleforermitochondriainteraction

Ejemplares similares