Tristetraprolin-driven regulatory circuit controls quality and timing of mRNA decay in inflammation

For a successful yet controlled immune response, cells need to specifically destabilize inflammatory mRNAs but prevent premature removal of those still used. The regulatory circuits controlling quality and timing in the global inflammatory mRNA decay are not understood. Here, we show that the mRNA-d...

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Autores principales: Kratochvill, Franz, Machacek, Christian, Vogl, Claus, Ebner, Florian, Sedlyarov, Vitaly, Gruber, Andreas R, Hartweger, Harald, Vielnascher, Raimund, Karaghiosoff, Marina, Rülicke, Thomas, Müller, Mathias, Hofacker, Ivo, Lang, Roland, Kovarik, Pavel
Formato: Online Artículo Texto
Lenguaje:English
Publicado: European Molecular Biology Organization 2011
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3737733/
https://www.ncbi.nlm.nih.gov/pubmed/22186734
http://dx.doi.org/10.1038/msb.2011.93
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author Kratochvill, Franz
Machacek, Christian
Vogl, Claus
Ebner, Florian
Sedlyarov, Vitaly
Gruber, Andreas R
Hartweger, Harald
Vielnascher, Raimund
Karaghiosoff, Marina
Rülicke, Thomas
Müller, Mathias
Hofacker, Ivo
Lang, Roland
Kovarik, Pavel
author_facet Kratochvill, Franz
Machacek, Christian
Vogl, Claus
Ebner, Florian
Sedlyarov, Vitaly
Gruber, Andreas R
Hartweger, Harald
Vielnascher, Raimund
Karaghiosoff, Marina
Rülicke, Thomas
Müller, Mathias
Hofacker, Ivo
Lang, Roland
Kovarik, Pavel
author_sort Kratochvill, Franz
collection PubMed
description For a successful yet controlled immune response, cells need to specifically destabilize inflammatory mRNAs but prevent premature removal of those still used. The regulatory circuits controlling quality and timing in the global inflammatory mRNA decay are not understood. Here, we show that the mRNA-destabilizing function of the AU-rich element-binding protein tristetraprolin (TTP) is inversely regulated by the p38 MAPK activity profile such that after inflammatory stimulus the TTP-dependent decay is initially limited to few mRNAs. With time, the TTP-dependent decay gradually spreads resulting in cumulative elimination of one third of inflammation-induced unstable mRNAs in macrophages in vitro. We confirmed this sequential decay model in vivo since LPS-treated mice with myeloid TTP ablation exhibited similar cytokine dysregulation profile as macrophages. The mice were hypersensitive to LPS but otherwise healthy with no signs of hyperinflammation seen in conventional TTP knockout mice demonstrating the requirement for myeloid TTP in re-installment but not maintenance of immune homeostasis. These findings reveal a TTP- and p38 MAPK-dominated regulatory mechanism that is vital for balancing acute inflammation by a temporally and qualitatively controlled mRNA decay.
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spelling pubmed-37377332013-08-08 Tristetraprolin-driven regulatory circuit controls quality and timing of mRNA decay in inflammation Kratochvill, Franz Machacek, Christian Vogl, Claus Ebner, Florian Sedlyarov, Vitaly Gruber, Andreas R Hartweger, Harald Vielnascher, Raimund Karaghiosoff, Marina Rülicke, Thomas Müller, Mathias Hofacker, Ivo Lang, Roland Kovarik, Pavel Mol Syst Biol Article For a successful yet controlled immune response, cells need to specifically destabilize inflammatory mRNAs but prevent premature removal of those still used. The regulatory circuits controlling quality and timing in the global inflammatory mRNA decay are not understood. Here, we show that the mRNA-destabilizing function of the AU-rich element-binding protein tristetraprolin (TTP) is inversely regulated by the p38 MAPK activity profile such that after inflammatory stimulus the TTP-dependent decay is initially limited to few mRNAs. With time, the TTP-dependent decay gradually spreads resulting in cumulative elimination of one third of inflammation-induced unstable mRNAs in macrophages in vitro. We confirmed this sequential decay model in vivo since LPS-treated mice with myeloid TTP ablation exhibited similar cytokine dysregulation profile as macrophages. The mice were hypersensitive to LPS but otherwise healthy with no signs of hyperinflammation seen in conventional TTP knockout mice demonstrating the requirement for myeloid TTP in re-installment but not maintenance of immune homeostasis. These findings reveal a TTP- and p38 MAPK-dominated regulatory mechanism that is vital for balancing acute inflammation by a temporally and qualitatively controlled mRNA decay. European Molecular Biology Organization 2011-12-20 /pmc/articles/PMC3737733/ /pubmed/22186734 http://dx.doi.org/10.1038/msb.2011.93 Text en Copyright © 2011, EMBO and Macmillan Publishers Limited https://creativecommons.org/licenses/by-nc-sa/3.0/This is an open-access article distributed under the terms of the Creative Commons Attribution Noncommercial Share Alike 3.0 Unported License, which allows readers to alter, transform, or build upon the article and then distribute the resulting work under the same or similar license to this one. The work must be attributed back to the original author and commercial use is not permitted without specific permission.
spellingShingle Article
Kratochvill, Franz
Machacek, Christian
Vogl, Claus
Ebner, Florian
Sedlyarov, Vitaly
Gruber, Andreas R
Hartweger, Harald
Vielnascher, Raimund
Karaghiosoff, Marina
Rülicke, Thomas
Müller, Mathias
Hofacker, Ivo
Lang, Roland
Kovarik, Pavel
Tristetraprolin-driven regulatory circuit controls quality and timing of mRNA decay in inflammation
title Tristetraprolin-driven regulatory circuit controls quality and timing of mRNA decay in inflammation
title_full Tristetraprolin-driven regulatory circuit controls quality and timing of mRNA decay in inflammation
title_fullStr Tristetraprolin-driven regulatory circuit controls quality and timing of mRNA decay in inflammation
title_full_unstemmed Tristetraprolin-driven regulatory circuit controls quality and timing of mRNA decay in inflammation
title_short Tristetraprolin-driven regulatory circuit controls quality and timing of mRNA decay in inflammation
title_sort tristetraprolin-driven regulatory circuit controls quality and timing of mrna decay in inflammation
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3737733/
https://www.ncbi.nlm.nih.gov/pubmed/22186734
http://dx.doi.org/10.1038/msb.2011.93
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