Translational repression of pre-formed cytokine-encoding mRNA prevents chronic activation of memory T cells

Fiamma Salerno; Sander Engels; Maartje van den Biggelaar; Floris P. J. van Alphen; Aurelie Guislain; Wanqi Zhao; Deborah L. Hodge; Sarah E. Bell; Jan Paul Medema; Marieke von Lindern; Martin Turner; Howard A. Young; Monika C. Wolkers

doi:https://doi.org/10.1038/s41590-018-0155-6

Translational repression of pre-formed cytokine-encoding mRNA prevents chronic activation of memory T cells

Fiamma Salerno, Sander Engels, Maartje van den Biggelaar, Floris P. J. van Alphen, Aurelie Guislain, Wanqi Zhao, Deborah L. Hodge, Sarah E. Bell, Jan Paul Medema, Marieke von Lindern, Martin Turner, Howard A. Young, Monika C. Wolkers

Research output: Contribution to journal › Article › Academic › peer-review

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Abstract

Memory T cells are critical for the immune response to recurring infections. Their instantaneous reactivity to pathogens is empowered by the persistent expression of cytokine-encoding mRNAs. How the translation of proteins from pre-formed cytokine-encoding mRNAs is prevented in the absence of infection has remained unclear. Here we found that protein production in memory T cells was blocked via a 3′ untranslated region (3′ UTR)-mediated process. Germline deletion of AU-rich elements (AREs) in the Ifng-3′ UTR led to chronic cytokine production in memory T cells. This aberrant protein production did not result from increased expression and/or half-life of the mRNA. Instead, AREs blocked the recruitment of cytokine-encoding mRNA to ribosomes; this block depended on the ARE-binding protein ZFP36L2. Thus, AREs mediate repression of translation in mouse and human memory T cells by preventing undesirable protein production from pre-formed cytokine-encoding mRNAs in the absence of infection.

Original language	English
Pages (from-to)	828-837
Journal	Nature immunology
Volume	19
Issue number	8
DOIs	https://doi.org/10.1038/s41590-018-0155-6
Publication status	Published - 2018

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Salerno, F., Engels, S., van den Biggelaar, M., van Alphen, F. P. J., Guislain, A., Zhao, W., Hodge, D. L., Bell, S. E., Medema, J. P., von Lindern, M., Turner, M., Young, H. A., & Wolkers, M. C. (2018). Translational repression of pre-formed cytokine-encoding mRNA prevents chronic activation of memory T cells. Nature immunology, 19(8), 828-837. https://doi.org/10.1038/s41590-018-0155-6

@article{400383a38684436bad804357ef078149,

title = "Translational repression of pre-formed cytokine-encoding mRNA prevents chronic activation of memory T cells",

abstract = "Memory T cells are critical for the immune response to recurring infections. Their instantaneous reactivity to pathogens is empowered by the persistent expression of cytokine-encoding mRNAs. How the translation of proteins from pre-formed cytokine-encoding mRNAs is prevented in the absence of infection has remained unclear. Here we found that protein production in memory T cells was blocked via a 3′ untranslated region (3′ UTR)-mediated process. Germline deletion of AU-rich elements (AREs) in the Ifng-3′ UTR led to chronic cytokine production in memory T cells. This aberrant protein production did not result from increased expression and/or half-life of the mRNA. Instead, AREs blocked the recruitment of cytokine-encoding mRNA to ribosomes; this block depended on the ARE-binding protein ZFP36L2. Thus, AREs mediate repression of translation in mouse and human memory T cells by preventing undesirable protein production from pre-formed cytokine-encoding mRNAs in the absence of infection.",

author = "Fiamma Salerno and Sander Engels and {van den Biggelaar}, Maartje and {van Alphen}, {Floris P. J.} and Aurelie Guislain and Wanqi Zhao and Hodge, {Deborah L.} and Bell, {Sarah E.} and Medema, {Jan Paul} and {von Lindern}, Marieke and Martin Turner and Young, {Howard A.} and Wolkers, {Monika C.}",

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doi = "https://doi.org/10.1038/s41590-018-0155-6",

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Salerno, F, Engels, S, van den Biggelaar, M, van Alphen, FPJ, Guislain, A, Zhao, W, Hodge, DL, Bell, SE, Medema, JP , von Lindern, M, Turner, M, Young, HA & Wolkers, MC 2018, 'Translational repression of pre-formed cytokine-encoding mRNA prevents chronic activation of memory T cells', Nature immunology, vol. 19, no. 8, pp. 828-837. https://doi.org/10.1038/s41590-018-0155-6

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AU - Salerno, Fiamma

AU - Engels, Sander

AU - van den Biggelaar, Maartje

AU - van Alphen, Floris P. J.

AU - Guislain, Aurelie

AU - Zhao, Wanqi

AU - Hodge, Deborah L.

AU - Bell, Sarah E.

AU - Medema, Jan Paul

AU - von Lindern, Marieke

AU - Turner, Martin

AU - Young, Howard A.

AU - Wolkers, Monika C.

PY - 2018

Y1 - 2018

N2 - Memory T cells are critical for the immune response to recurring infections. Their instantaneous reactivity to pathogens is empowered by the persistent expression of cytokine-encoding mRNAs. How the translation of proteins from pre-formed cytokine-encoding mRNAs is prevented in the absence of infection has remained unclear. Here we found that protein production in memory T cells was blocked via a 3′ untranslated region (3′ UTR)-mediated process. Germline deletion of AU-rich elements (AREs) in the Ifng-3′ UTR led to chronic cytokine production in memory T cells. This aberrant protein production did not result from increased expression and/or half-life of the mRNA. Instead, AREs blocked the recruitment of cytokine-encoding mRNA to ribosomes; this block depended on the ARE-binding protein ZFP36L2. Thus, AREs mediate repression of translation in mouse and human memory T cells by preventing undesirable protein production from pre-formed cytokine-encoding mRNAs in the absence of infection.

AB - Memory T cells are critical for the immune response to recurring infections. Their instantaneous reactivity to pathogens is empowered by the persistent expression of cytokine-encoding mRNAs. How the translation of proteins from pre-formed cytokine-encoding mRNAs is prevented in the absence of infection has remained unclear. Here we found that protein production in memory T cells was blocked via a 3′ untranslated region (3′ UTR)-mediated process. Germline deletion of AU-rich elements (AREs) in the Ifng-3′ UTR led to chronic cytokine production in memory T cells. This aberrant protein production did not result from increased expression and/or half-life of the mRNA. Instead, AREs blocked the recruitment of cytokine-encoding mRNA to ribosomes; this block depended on the ARE-binding protein ZFP36L2. Thus, AREs mediate repression of translation in mouse and human memory T cells by preventing undesirable protein production from pre-formed cytokine-encoding mRNAs in the absence of infection.

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JO - Nature immunology

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Translational repression of pre-formed cytokine-encoding mRNA prevents chronic activation of memory T cells

Abstract

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