m                         6                         A modification controls the innate immune response to infection by targeting type I interferons

Roni Winkler; Ella Gillis; Lior Lasman; Modi Safra; Shay Geula; Clara Soyris; Aharon Nachshon; Julie Tai-Schmiedel; Nehemya Friedman; Vu Thuy Khanh Le-Trilling; Mirko Trilling; Michal Mandelboim; Jacob H. Hanna; Schraga Schwartz; Noam Stern-Ginossar

doi:10.1038/s41590-018-0275-z

m ⁶ A modification controls the innate immune response to infection by targeting type I interferons

Roni Winkler
, Ella Gillis
, Lior Lasman
, Modi Safra
, Shay Geula
, Clara Soyris
, Aharon Nachshon
, Julie Tai-Schmiedel
, Nehemya Friedman
, Vu Thuy Khanh Le-Trilling
, Mirko Trilling
, Michal Mandelboim
, Jacob H. Hanna
, Schraga Schwartz
, Noam Stern-Ginossar

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

384 Scopus citations

Abstract

N ⁶ -methyladenosine (m ⁶ A) is the most common mRNA modification. Recent studies have revealed that depletion of m ⁶ A machinery leads to alterations in the propagation of diverse viruses. These effects were proposed to be mediated through dysregulated methylation of viral RNA. Here we show that following viral infection or stimulation of cells with an inactivated virus, deletion of the m ⁶ A ‘writer’ METTL3 or ‘reader’ YTHDF2 led to an increase in the induction of interferon-stimulated genes. Consequently, propagation of different viruses was suppressed in an interferon-signaling-dependent manner. Significantly, the mRNA of IFNB, the gene encoding the main cytokine that drives the type I interferon response, was m ⁶ A modified and was stabilized following repression of METTL3 or YTHDF2. Furthermore, we show that m ⁶ A-mediated regulation of interferon genes was conserved in mice. Together, our findings uncover the role m ⁶ A serves as a negative regulator of interferon response by dictating the fast turnover of interferon mRNAs and consequently facilitating viral propagation.

Original language	English
Pages (from-to)	173-182
Number of pages	10
Journal	Nature Immunology
Volume	20
Issue number	2
DOIs	https://doi.org/10.1038/s41590-018-0275-z
State	Published - 1 Feb 2019
Externally published	Yes

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

ASJC Scopus subject areas

Immunology and Allergy
Immunology

Access to Document

10.1038/s41590-018-0275-z

Cite this

Winkler, R., Gillis, E., Lasman, L., Safra, M., Geula, S., Soyris, C., Nachshon, A., Tai-Schmiedel, J., Friedman, N., Le-Trilling, V. T. K., Trilling, M., Mandelboim, M., Hanna, J. H., Schwartz, S., & Stern-Ginossar, N. (2019). m ⁶ A modification controls the innate immune response to infection by targeting type I interferons Nature Immunology, 20(2), 173-182. https://doi.org/10.1038/s41590-018-0275-z

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title = " m 6 A modification controls the innate immune response to infection by targeting type I interferons ",

abstract = " N 6 -methyladenosine (m 6 A) is the most common mRNA modification. Recent studies have revealed that depletion of m 6 A machinery leads to alterations in the propagation of diverse viruses. These effects were proposed to be mediated through dysregulated methylation of viral RNA. Here we show that following viral infection or stimulation of cells with an inactivated virus, deletion of the m 6 A {\textquoteleft}writer{\textquoteright} METTL3 or {\textquoteleft}reader{\textquoteright} YTHDF2 led to an increase in the induction of interferon-stimulated genes. Consequently, propagation of different viruses was suppressed in an interferon-signaling-dependent manner. Significantly, the mRNA of IFNB, the gene encoding the main cytokine that drives the type I interferon response, was m 6 A modified and was stabilized following repression of METTL3 or YTHDF2. Furthermore, we show that m 6 A-mediated regulation of interferon genes was conserved in mice. Together, our findings uncover the role m 6 A serves as a negative regulator of interferon response by dictating the fast turnover of interferon mRNAs and consequently facilitating viral propagation.",

author = "Roni Winkler and Ella Gillis and Lior Lasman and Modi Safra and Shay Geula and Clara Soyris and Aharon Nachshon and Julie Tai-Schmiedel and Nehemya Friedman and Le-Trilling, \{Vu Thuy Khanh\} and Mirko Trilling and Michal Mandelboim and Hanna, \{Jacob H.\} and Schraga Schwartz and Noam Stern-Ginossar",

note = "Publisher Copyright: {\textcopyright} 2018, The Author(s), under exclusive licence to Springer Nature America, Inc.",

year = "2019",

month = feb,

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doi = "10.1038/s41590-018-0275-z",

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Winkler, R, Gillis, E, Lasman, L, Safra, M, Geula, S, Soyris, C, Nachshon, A, Tai-Schmiedel, J, Friedman, N, Le-Trilling, VTK, Trilling, M, Mandelboim, M, Hanna, JH, Schwartz, S & Stern-Ginossar, N 2019, ' m ⁶ A modification controls the innate immune response to infection by targeting type I interferons ', Nature Immunology, vol. 20, no. 2, pp. 173-182. https://doi.org/10.1038/s41590-018-0275-z

m ⁶ A modification controls the innate immune response to infection by targeting type I interferons . / Winkler, Roni; Gillis, Ella; Lasman, Lior et al.
In: Nature Immunology, Vol. 20, No. 2, 01.02.2019, p. 173-182.

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

TY - JOUR

T1 - m 6 A modification controls the innate immune response to infection by targeting type I interferons

AU - Winkler, Roni

AU - Gillis, Ella

AU - Lasman, Lior

AU - Safra, Modi

AU - Geula, Shay

AU - Soyris, Clara

AU - Nachshon, Aharon

AU - Tai-Schmiedel, Julie

AU - Friedman, Nehemya

AU - Le-Trilling, Vu Thuy Khanh

AU - Trilling, Mirko

AU - Mandelboim, Michal

AU - Hanna, Jacob H.

AU - Schwartz, Schraga

AU - Stern-Ginossar, Noam

PY - 2019/2/1

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N2 - N 6 -methyladenosine (m 6 A) is the most common mRNA modification. Recent studies have revealed that depletion of m 6 A machinery leads to alterations in the propagation of diverse viruses. These effects were proposed to be mediated through dysregulated methylation of viral RNA. Here we show that following viral infection or stimulation of cells with an inactivated virus, deletion of the m 6 A ‘writer’ METTL3 or ‘reader’ YTHDF2 led to an increase in the induction of interferon-stimulated genes. Consequently, propagation of different viruses was suppressed in an interferon-signaling-dependent manner. Significantly, the mRNA of IFNB, the gene encoding the main cytokine that drives the type I interferon response, was m 6 A modified and was stabilized following repression of METTL3 or YTHDF2. Furthermore, we show that m 6 A-mediated regulation of interferon genes was conserved in mice. Together, our findings uncover the role m 6 A serves as a negative regulator of interferon response by dictating the fast turnover of interferon mRNAs and consequently facilitating viral propagation.

AB - N 6 -methyladenosine (m 6 A) is the most common mRNA modification. Recent studies have revealed that depletion of m 6 A machinery leads to alterations in the propagation of diverse viruses. These effects were proposed to be mediated through dysregulated methylation of viral RNA. Here we show that following viral infection or stimulation of cells with an inactivated virus, deletion of the m 6 A ‘writer’ METTL3 or ‘reader’ YTHDF2 led to an increase in the induction of interferon-stimulated genes. Consequently, propagation of different viruses was suppressed in an interferon-signaling-dependent manner. Significantly, the mRNA of IFNB, the gene encoding the main cytokine that drives the type I interferon response, was m 6 A modified and was stabilized following repression of METTL3 or YTHDF2. Furthermore, we show that m 6 A-mediated regulation of interferon genes was conserved in mice. Together, our findings uncover the role m 6 A serves as a negative regulator of interferon response by dictating the fast turnover of interferon mRNAs and consequently facilitating viral propagation.

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