Norovirus MLKL-like protein initiates cell death to induce viral egress

Guoxun Wang; Di Zhang; Robert C. Orchard; Dustin C. Hancks; Tiffany A. Reese

doi:10.1038/s41586-023-05851-w

Norovirus MLKL-like protein initiates cell death to induce viral egress

Guoxun Wang, Di Zhang, Robert C. Orchard, Dustin C. Hancks, Tiffany A. Reese

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

9 Scopus citations

Abstract

Non-enveloped viruses require cell lysis to release new virions from infected cells, suggesting that these viruses require mechanisms to induce cell death. Noroviruses are one such group of viruses, but there is no known mechanism that causes norovirus infection-triggered cell death and lysis^1–3. Here we identify a molecular mechanism of norovirus-induced cell death. We found that the norovirus-encoded NTPase NS3 contains an N-terminal four-helix bundle domain homologous to the membrane-disruption domain of the pseudokinase mixed lineage kinase domain-like (MLKL). NS3 has a mitochondrial localization signal and thus induces cell death by targeting mitochondria. Full-length NS3 and an N-terminal fragment of the protein bound the mitochondrial membrane lipid cardiolipin, permeabilized the mitochondrial membrane and induced mitochondrial dysfunction. Both the N-terminal region and the mitochondrial localization motif of NS3 were essential for cell death, viral egress from cells and viral replication in mice. These findings suggest that noroviruses have acquired a host MLKL-like pore-forming domain to facilitate viral egress by inducing mitochondrial dysfunction.

Original language	English (US)
Pages (from-to)	152-158
Number of pages	7
Journal	Nature
Volume	616
Issue number	7955
DOIs	https://doi.org/10.1038/s41586-023-05851-w
State	Published - Apr 6 2023

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title = "Norovirus MLKL-like protein initiates cell death to induce viral egress",

abstract = "Non-enveloped viruses require cell lysis to release new virions from infected cells, suggesting that these viruses require mechanisms to induce cell death. Noroviruses are one such group of viruses, but there is no known mechanism that causes norovirus infection-triggered cell death and lysis1–3. Here we identify a molecular mechanism of norovirus-induced cell death. We found that the norovirus-encoded NTPase NS3 contains an N-terminal four-helix bundle domain homologous to the membrane-disruption domain of the pseudokinase mixed lineage kinase domain-like (MLKL). NS3 has a mitochondrial localization signal and thus induces cell death by targeting mitochondria. Full-length NS3 and an N-terminal fragment of the protein bound the mitochondrial membrane lipid cardiolipin, permeabilized the mitochondrial membrane and induced mitochondrial dysfunction. Both the N-terminal region and the mitochondrial localization motif of NS3 were essential for cell death, viral egress from cells and viral replication in mice. These findings suggest that noroviruses have acquired a host MLKL-like pore-forming domain to facilitate viral egress by inducing mitochondrial dysfunction.",

author = "Guoxun Wang and Di Zhang and Orchard, {Robert C.} and Hancks, {Dustin C.} and Reese, {Tiffany A.}",

note = "Funding Information: The authors thank Z. G. Wang for providing the pLVX-TRE3G vector; J. Rizo-Rey, Z. G. Wang and K. Yang for helpful discussions and technical assistance; and members of the Reese laboratory for technical assistance. T.A.R. is supported by grants from the NIH (R01AI130020-01A1, U19AI142784), CPRIT (RP200118), and the Pew Scholars Program. D.C.H. is funded by a 1R35GM142689-01 and a Recruitment of First-Time, Tenure-Track Faculty from Cancer Prevention & Research Institute of Texas Award (RR 170047). Publisher Copyright: {\textcopyright} 2023, The Author(s), under exclusive licence to Springer Nature Limited.",

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AU - Reese, Tiffany A.

N1 - Funding Information: The authors thank Z. G. Wang for providing the pLVX-TRE3G vector; J. Rizo-Rey, Z. G. Wang and K. Yang for helpful discussions and technical assistance; and members of the Reese laboratory for technical assistance. T.A.R. is supported by grants from the NIH (R01AI130020-01A1, U19AI142784), CPRIT (RP200118), and the Pew Scholars Program. D.C.H. is funded by a 1R35GM142689-01 and a Recruitment of First-Time, Tenure-Track Faculty from Cancer Prevention & Research Institute of Texas Award (RR 170047). Publisher Copyright: © 2023, The Author(s), under exclusive licence to Springer Nature Limited.

PY - 2023/4/6

Y1 - 2023/4/6

N2 - Non-enveloped viruses require cell lysis to release new virions from infected cells, suggesting that these viruses require mechanisms to induce cell death. Noroviruses are one such group of viruses, but there is no known mechanism that causes norovirus infection-triggered cell death and lysis1–3. Here we identify a molecular mechanism of norovirus-induced cell death. We found that the norovirus-encoded NTPase NS3 contains an N-terminal four-helix bundle domain homologous to the membrane-disruption domain of the pseudokinase mixed lineage kinase domain-like (MLKL). NS3 has a mitochondrial localization signal and thus induces cell death by targeting mitochondria. Full-length NS3 and an N-terminal fragment of the protein bound the mitochondrial membrane lipid cardiolipin, permeabilized the mitochondrial membrane and induced mitochondrial dysfunction. Both the N-terminal region and the mitochondrial localization motif of NS3 were essential for cell death, viral egress from cells and viral replication in mice. These findings suggest that noroviruses have acquired a host MLKL-like pore-forming domain to facilitate viral egress by inducing mitochondrial dysfunction.

AB - Non-enveloped viruses require cell lysis to release new virions from infected cells, suggesting that these viruses require mechanisms to induce cell death. Noroviruses are one such group of viruses, but there is no known mechanism that causes norovirus infection-triggered cell death and lysis1–3. Here we identify a molecular mechanism of norovirus-induced cell death. We found that the norovirus-encoded NTPase NS3 contains an N-terminal four-helix bundle domain homologous to the membrane-disruption domain of the pseudokinase mixed lineage kinase domain-like (MLKL). NS3 has a mitochondrial localization signal and thus induces cell death by targeting mitochondria. Full-length NS3 and an N-terminal fragment of the protein bound the mitochondrial membrane lipid cardiolipin, permeabilized the mitochondrial membrane and induced mitochondrial dysfunction. Both the N-terminal region and the mitochondrial localization motif of NS3 were essential for cell death, viral egress from cells and viral replication in mice. These findings suggest that noroviruses have acquired a host MLKL-like pore-forming domain to facilitate viral egress by inducing mitochondrial dysfunction.

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Norovirus MLKL-like protein initiates cell death to induce viral egress

Abstract

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