Cytosolic translational responses differ under conditions of severe short-term and long-term mitochondrial stress

Previous studies demonstrated that cells inhibit protein synthesis as a compensatory mechanism for mitochondrial dysfunction. Protein synthesis can be attenuated by 1) the inhibition of mTOR kinase, which results in a decrease in the phosphorylation of S6K1 and 4E-BP1 proteins, and 2) an increase in...

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Autores principales: Samluk, Lukasz, Urbanska, Malgorzata, Kisielewska, Katarzyna, Mohanraj, Karthik, Kim, Min-Ji, Machnicka, Katarzyna, Liszewska, Ewa, Jaworski, Jacek, Chacinska, Agnieszka
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The American Society for Cell Biology 2019
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Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6727742/
https://www.ncbi.nlm.nih.gov/pubmed/31116686
http://dx.doi.org/10.1091/mbc.E18-10-0628
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author Samluk, Lukasz
Urbanska, Malgorzata
Kisielewska, Katarzyna
Mohanraj, Karthik
Kim, Min-Ji
Machnicka, Katarzyna
Liszewska, Ewa
Jaworski, Jacek
Chacinska, Agnieszka
author_facet Samluk, Lukasz
Urbanska, Malgorzata
Kisielewska, Katarzyna
Mohanraj, Karthik
Kim, Min-Ji
Machnicka, Katarzyna
Liszewska, Ewa
Jaworski, Jacek
Chacinska, Agnieszka
author_sort Samluk, Lukasz
collection PubMed
description Previous studies demonstrated that cells inhibit protein synthesis as a compensatory mechanism for mitochondrial dysfunction. Protein synthesis can be attenuated by 1) the inhibition of mTOR kinase, which results in a decrease in the phosphorylation of S6K1 and 4E-BP1 proteins, and 2) an increase in the phosphorylation of eIF2α protein. The present study investigated both of these pathways under conditions of short-term acute and long-term mitochondrial stress. Short-term responses were triggered in mammalian cells by treatment with menadione, antimycin A, or CCCP. Long-term mitochondrial stress was induced by prolonged treatment with menadione or rotenone and expression of genetic alterations, such as knocking down the MIA40 oxidoreductase or knocking out NDUFA11 protein. Short-term menadione, antimycin A, or CCCP cell treatment led to the inhibition of protein synthesis, accompanied by a decrease in mTOR kinase activity, an increase in the phosphorylation of eIF2α (Ser51), and an increase in the level of ATF4 transcription factor. Conversely, long-term stress led to a decrease in eIF2α (Ser51) phosphorylation and ATF4 expression and to an increase in S6K1 (Thr389) phosphorylation. Thus, under long-term mitochondrial stress, cells trigger long-lasting adaptive responses for protection against excessive inhibition of protein synthesis.
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spelling pubmed-67277422019-09-30 Cytosolic translational responses differ under conditions of severe short-term and long-term mitochondrial stress Samluk, Lukasz Urbanska, Malgorzata Kisielewska, Katarzyna Mohanraj, Karthik Kim, Min-Ji Machnicka, Katarzyna Liszewska, Ewa Jaworski, Jacek Chacinska, Agnieszka Mol Biol Cell Articles Previous studies demonstrated that cells inhibit protein synthesis as a compensatory mechanism for mitochondrial dysfunction. Protein synthesis can be attenuated by 1) the inhibition of mTOR kinase, which results in a decrease in the phosphorylation of S6K1 and 4E-BP1 proteins, and 2) an increase in the phosphorylation of eIF2α protein. The present study investigated both of these pathways under conditions of short-term acute and long-term mitochondrial stress. Short-term responses were triggered in mammalian cells by treatment with menadione, antimycin A, or CCCP. Long-term mitochondrial stress was induced by prolonged treatment with menadione or rotenone and expression of genetic alterations, such as knocking down the MIA40 oxidoreductase or knocking out NDUFA11 protein. Short-term menadione, antimycin A, or CCCP cell treatment led to the inhibition of protein synthesis, accompanied by a decrease in mTOR kinase activity, an increase in the phosphorylation of eIF2α (Ser51), and an increase in the level of ATF4 transcription factor. Conversely, long-term stress led to a decrease in eIF2α (Ser51) phosphorylation and ATF4 expression and to an increase in S6K1 (Thr389) phosphorylation. Thus, under long-term mitochondrial stress, cells trigger long-lasting adaptive responses for protection against excessive inhibition of protein synthesis. The American Society for Cell Biology 2019-07-15 /pmc/articles/PMC6727742/ /pubmed/31116686 http://dx.doi.org/10.1091/mbc.E18-10-0628 Text en © 2019 Samluk et al. “ASCB®,” “The American Society for Cell Biology®,” and “Molecular Biology of the Cell®” are registered trademarks of The American Society for Cell Biology. http://creativecommons.org/licenses/by-nc-sa/3.0 This article is distributed by The American Society for Cell Biology under license from the author(s). Two months after publication it is available to the public under an Attribution–Noncommercial–Share Alike 3.0 Unported Creative Commons License.
spellingShingle Articles
Samluk, Lukasz
Urbanska, Malgorzata
Kisielewska, Katarzyna
Mohanraj, Karthik
Kim, Min-Ji
Machnicka, Katarzyna
Liszewska, Ewa
Jaworski, Jacek
Chacinska, Agnieszka
Cytosolic translational responses differ under conditions of severe short-term and long-term mitochondrial stress
title Cytosolic translational responses differ under conditions of severe short-term and long-term mitochondrial stress
title_full Cytosolic translational responses differ under conditions of severe short-term and long-term mitochondrial stress
title_fullStr Cytosolic translational responses differ under conditions of severe short-term and long-term mitochondrial stress
title_full_unstemmed Cytosolic translational responses differ under conditions of severe short-term and long-term mitochondrial stress
title_short Cytosolic translational responses differ under conditions of severe short-term and long-term mitochondrial stress
title_sort cytosolic translational responses differ under conditions of severe short-term and long-term mitochondrial stress
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6727742/
https://www.ncbi.nlm.nih.gov/pubmed/31116686
http://dx.doi.org/10.1091/mbc.E18-10-0628
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