Early endonuclease-mediated evasion of RNA sensing ensures efficient coronavirus replication

Eveline Kindler; Cristina Gil-Cruz; Julia Spanier; Yize Li; Jochen Wilhelm; Huib H Rabouw; Roland Züst; Mihyun Hwang; Philip V'kovski; Hanspeter Stalder; Sabrina Marti; Matthias Habjan; Luisa Cervantes-Barragan; Ruth Elliot; Nadja Karl; Christina Gaughan; Frank J M van Kuppeveld; Robert H Silverman; Markus Keller; Burkhard Ludewig; Cornelia C Bergmann; John Ziebuhr; Susan R Weiss; Ulrich Kalinke; Volker Thiel

doi:10.1371/journal.ppat.1006195

Early endonuclease-mediated evasion of RNA sensing ensures efficient coronavirus replication

Eveline Kindler, Cristina Gil-Cruz, Julia Spanier, Yize Li, Jochen Wilhelm, Huib H Rabouw, Roland Züst, Mihyun Hwang, Philip V'kovski, Hanspeter Stalder, Sabrina Marti, Matthias Habjan, Luisa Cervantes-Barragan, Ruth Elliot, Nadja Karl, Christina Gaughan, Frank J M van Kuppeveld, Robert H Silverman, Markus Keller, Burkhard LudewigCornelia C Bergmann, John Ziebuhr, Susan R Weiss, Ulrich Kalinke, Volker Thiel

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

Abstract

Coronaviruses are of veterinary and medical importance and include highly pathogenic zoonotic viruses, such as SARS-CoV and MERS-CoV. They are known to efficiently evade early innate immune responses, manifesting in almost negligible expression of type-I interferons (IFN-I). This evasion strategy suggests an evolutionary conserved viral function that has evolved to prevent RNA-based sensing of infection in vertebrate hosts. Here we show that the coronavirus endonuclease (EndoU) activity is key to prevent early induction of double-stranded RNA (dsRNA) host cell responses. Replication of EndoU-deficient coronaviruses is greatly attenuated in vivo and severely restricted in primary cells even during the early phase of the infection. In macrophages we found immediate induction of IFN-I expression and RNase L-mediated breakdown of ribosomal RNA. Accordingly, EndoU-deficient viruses can retain replication only in cells that are deficient in IFN-I expression or sensing, and in cells lacking both RNase L and PKR. Collectively our results demonstrate that the coronavirus EndoU efficiently prevents simultaneous activation of host cell dsRNA sensors, such as Mda5, OAS and PKR. The localization of the EndoU activity at the site of viral RNA synthesis-within the replicase complex-suggests that coronaviruses have evolved a viral RNA decay pathway to evade early innate and intrinsic antiviral host cell responses.

Original language	English
Article number	e1006195
Journal	PLoS Pathogens
Volume	13
Issue number	2
DOIs	https://doi.org/10.1371/journal.ppat.1006195
Publication status	Published - 3 Feb 2017

Access to Document

10.1371/journal.ppat.1006195

kindlerFinal published version, 5.3 MB

Cite this

Kindler, E., Gil-Cruz, C., Spanier, J., Li, Y., Wilhelm, J., Rabouw, H. H., Züst, R., Hwang, M., V'kovski, P., Stalder, H., Marti, S., Habjan, M., Cervantes-Barragan, L., Elliot, R., Karl, N., Gaughan, C., van Kuppeveld, F. J. M., Silverman, R. H., Keller, M., ... Thiel, V. (2017). Early endonuclease-mediated evasion of RNA sensing ensures efficient coronavirus replication. PLoS Pathogens, 13(2), Article e1006195. https://doi.org/10.1371/journal.ppat.1006195

@article{3765e5240ac34655a48a9a10e631a06c,

title = "Early endonuclease-mediated evasion of RNA sensing ensures efficient coronavirus replication",

abstract = "Coronaviruses are of veterinary and medical importance and include highly pathogenic zoonotic viruses, such as SARS-CoV and MERS-CoV. They are known to efficiently evade early innate immune responses, manifesting in almost negligible expression of type-I interferons (IFN-I). This evasion strategy suggests an evolutionary conserved viral function that has evolved to prevent RNA-based sensing of infection in vertebrate hosts. Here we show that the coronavirus endonuclease (EndoU) activity is key to prevent early induction of double-stranded RNA (dsRNA) host cell responses. Replication of EndoU-deficient coronaviruses is greatly attenuated in vivo and severely restricted in primary cells even during the early phase of the infection. In macrophages we found immediate induction of IFN-I expression and RNase L-mediated breakdown of ribosomal RNA. Accordingly, EndoU-deficient viruses can retain replication only in cells that are deficient in IFN-I expression or sensing, and in cells lacking both RNase L and PKR. Collectively our results demonstrate that the coronavirus EndoU efficiently prevents simultaneous activation of host cell dsRNA sensors, such as Mda5, OAS and PKR. The localization of the EndoU activity at the site of viral RNA synthesis-within the replicase complex-suggests that coronaviruses have evolved a viral RNA decay pathway to evade early innate and intrinsic antiviral host cell responses.",

author = "Eveline Kindler and Cristina Gil-Cruz and Julia Spanier and Yize Li and Jochen Wilhelm and Rabouw, {Huib H} and Roland Z{\"u}st and Mihyun Hwang and Philip V'kovski and Hanspeter Stalder and Sabrina Marti and Matthias Habjan and Luisa Cervantes-Barragan and Ruth Elliot and Nadja Karl and Christina Gaughan and {van Kuppeveld}, {Frank J M} and Silverman, {Robert H} and Markus Keller and Burkhard Ludewig and Bergmann, {Cornelia C} and John Ziebuhr and Weiss, {Susan R} and Ulrich Kalinke and Volker Thiel",

year = "2017",

month = feb,

day = "3",

doi = "10.1371/journal.ppat.1006195",

language = "English",

volume = "13",

journal = "PLoS Pathogens",

issn = "1553-7366",

publisher = "Public Library of Science",

number = "2",

}

Kindler, E, Gil-Cruz, C, Spanier, J, Li, Y, Wilhelm, J, Rabouw, HH, Züst, R, Hwang, M, V'kovski, P, Stalder, H, Marti, S, Habjan, M, Cervantes-Barragan, L, Elliot, R, Karl, N, Gaughan, C, van Kuppeveld, FJM, Silverman, RH, Keller, M, Ludewig, B, Bergmann, CC, Ziebuhr, J, Weiss, SR, Kalinke, U & Thiel, V 2017, 'Early endonuclease-mediated evasion of RNA sensing ensures efficient coronavirus replication', PLoS Pathogens, vol. 13, no. 2, e1006195. https://doi.org/10.1371/journal.ppat.1006195

TY - JOUR

T1 - Early endonuclease-mediated evasion of RNA sensing ensures efficient coronavirus replication

AU - Kindler, Eveline

AU - Gil-Cruz, Cristina

AU - Spanier, Julia

AU - Li, Yize

AU - Wilhelm, Jochen

AU - Rabouw, Huib H

AU - Züst, Roland

AU - Hwang, Mihyun

AU - V'kovski, Philip

AU - Stalder, Hanspeter

AU - Marti, Sabrina

AU - Habjan, Matthias

AU - Cervantes-Barragan, Luisa

AU - Elliot, Ruth

AU - Karl, Nadja

AU - Gaughan, Christina

AU - van Kuppeveld, Frank J M

AU - Silverman, Robert H

AU - Keller, Markus

AU - Ludewig, Burkhard

AU - Bergmann, Cornelia C

AU - Ziebuhr, John

AU - Weiss, Susan R

AU - Kalinke, Ulrich

AU - Thiel, Volker

PY - 2017/2/3

Y1 - 2017/2/3

N2 - Coronaviruses are of veterinary and medical importance and include highly pathogenic zoonotic viruses, such as SARS-CoV and MERS-CoV. They are known to efficiently evade early innate immune responses, manifesting in almost negligible expression of type-I interferons (IFN-I). This evasion strategy suggests an evolutionary conserved viral function that has evolved to prevent RNA-based sensing of infection in vertebrate hosts. Here we show that the coronavirus endonuclease (EndoU) activity is key to prevent early induction of double-stranded RNA (dsRNA) host cell responses. Replication of EndoU-deficient coronaviruses is greatly attenuated in vivo and severely restricted in primary cells even during the early phase of the infection. In macrophages we found immediate induction of IFN-I expression and RNase L-mediated breakdown of ribosomal RNA. Accordingly, EndoU-deficient viruses can retain replication only in cells that are deficient in IFN-I expression or sensing, and in cells lacking both RNase L and PKR. Collectively our results demonstrate that the coronavirus EndoU efficiently prevents simultaneous activation of host cell dsRNA sensors, such as Mda5, OAS and PKR. The localization of the EndoU activity at the site of viral RNA synthesis-within the replicase complex-suggests that coronaviruses have evolved a viral RNA decay pathway to evade early innate and intrinsic antiviral host cell responses.

AB - Coronaviruses are of veterinary and medical importance and include highly pathogenic zoonotic viruses, such as SARS-CoV and MERS-CoV. They are known to efficiently evade early innate immune responses, manifesting in almost negligible expression of type-I interferons (IFN-I). This evasion strategy suggests an evolutionary conserved viral function that has evolved to prevent RNA-based sensing of infection in vertebrate hosts. Here we show that the coronavirus endonuclease (EndoU) activity is key to prevent early induction of double-stranded RNA (dsRNA) host cell responses. Replication of EndoU-deficient coronaviruses is greatly attenuated in vivo and severely restricted in primary cells even during the early phase of the infection. In macrophages we found immediate induction of IFN-I expression and RNase L-mediated breakdown of ribosomal RNA. Accordingly, EndoU-deficient viruses can retain replication only in cells that are deficient in IFN-I expression or sensing, and in cells lacking both RNase L and PKR. Collectively our results demonstrate that the coronavirus EndoU efficiently prevents simultaneous activation of host cell dsRNA sensors, such as Mda5, OAS and PKR. The localization of the EndoU activity at the site of viral RNA synthesis-within the replicase complex-suggests that coronaviruses have evolved a viral RNA decay pathway to evade early innate and intrinsic antiviral host cell responses.

U2 - 10.1371/journal.ppat.1006195

DO - 10.1371/journal.ppat.1006195

M3 - Article

C2 - 28158275

SN - 1553-7366

VL - 13

JO - PLoS Pathogens

JF - PLoS Pathogens

IS - 2

M1 - e1006195

ER -

Early endonuclease-mediated evasion of RNA sensing ensures efficient coronavirus replication

Abstract

Access to Document

Fingerprint

Cite this