Norovirus regulation of the innate immune response and apoptosis occurs via the product of the alternative open reading frame 4

Nora McFadden; Dalan Bailey; Guia Carrara; Alicia Benson; Yasmin Chaudhry; Amita Shortland; Jonathan Heeney; Felix Yarovinsky; Peter Simmonds; Andrew Macdonald; Ian Goodfellow

doi:10.1371/journal.ppat.1002413

Norovirus regulation of the innate immune response and apoptosis occurs via the product of the alternative open reading frame 4

Nora McFadden, Dalan Bailey, Guia Carrara, Alicia Benson, Yasmin Chaudhry, Amita Shortland, Jonathan Heeney, Felix Yarovinsky, Peter Simmonds, Andrew Macdonald, Ian Goodfellow

Immunology and Immunotherapy

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

151 Citations (Scopus)

Abstract

Small RNA viruses have evolved many mechanisms to increase the capacity of their short genomes. Here we describe the identification and characterization of a novel open reading frame (ORF4) encoded by the murine norovirus (MNV) subgenomic RNA, in an alternative reading frame overlapping the VP1 coding region. ORF4 is translated during virus infection and the resultant protein localizes predominantly to the mitochondria. Using reverse genetics we demonstrated that expression of ORF4 is not required for virus replication in tissue culture but its loss results in a fitness cost since viruses lacking the ability to express ORF4 restore expression upon repeated passage in tissue culture. Functional analysis indicated that the protein produced from ORF4 antagonizes the innate immune response to infection by delaying the upregulation of a number of cellular genes activated by the innate pathway, including IFN-Beta. Apoptosis in the RAW264.7 macrophage cell line was also increased during virus infection in the absence of ORF4 expression. In vivo analysis of the WT and mutant virus lacking the ability to express ORF4 demonstrated an important role for ORF4 expression in infection and virulence. STAT1-/- mice infected with a virus lacking the ability to express ORF4 showed a delay in the onset of clinical signs when compared to mice infected with WT virus. Quantitative PCR and histopathological analysis of samples from these infected mice demonstrated that infection with a virus not expressing ORF4 results in a delayed infection in this system. In light of these findings we propose the name virulence factor 1, VF1 for this protein. The identification of VF1 represents the first characterization of an alternative open reading frame protein for the calicivirus family. The immune regulatory function of the MNV VF1 protein provide important perspectives for future research into norovirus biology and pathogenesis.

Original language	English
Pages (from-to)	e1002413
Journal	PLoS pathogens
Volume	7
Issue number	12
DOIs	https://doi.org/10.1371/journal.ppat.1002413
Publication status	Published - Dec 2011

Keywords

Amino Acid Sequence
Animals
Apoptosis
Blotting, Western
Caliciviridae Infections
Enzyme-Linked Immunosorbent Assay
Gene Expression Regulation
Immunity, Innate
Immunoprecipitation
Mice
Mice, Inbred C57BL
Mice, Knockout
Mitochondria
Molecular Sequence Data
Norovirus
Open Reading Frames
RNA, Viral
Real-Time Polymerase Chain Reaction
Reverse Genetics
Reverse Transcriptase Polymerase Chain Reaction
Viral Proteins
Virulence
Virulence Factors
Virus Replication

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10.1371/journal.ppat.1002413

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title = "Norovirus regulation of the innate immune response and apoptosis occurs via the product of the alternative open reading frame 4",

abstract = "Small RNA viruses have evolved many mechanisms to increase the capacity of their short genomes. Here we describe the identification and characterization of a novel open reading frame (ORF4) encoded by the murine norovirus (MNV) subgenomic RNA, in an alternative reading frame overlapping the VP1 coding region. ORF4 is translated during virus infection and the resultant protein localizes predominantly to the mitochondria. Using reverse genetics we demonstrated that expression of ORF4 is not required for virus replication in tissue culture but its loss results in a fitness cost since viruses lacking the ability to express ORF4 restore expression upon repeated passage in tissue culture. Functional analysis indicated that the protein produced from ORF4 antagonizes the innate immune response to infection by delaying the upregulation of a number of cellular genes activated by the innate pathway, including IFN-Beta. Apoptosis in the RAW264.7 macrophage cell line was also increased during virus infection in the absence of ORF4 expression. In vivo analysis of the WT and mutant virus lacking the ability to express ORF4 demonstrated an important role for ORF4 expression in infection and virulence. STAT1-/- mice infected with a virus lacking the ability to express ORF4 showed a delay in the onset of clinical signs when compared to mice infected with WT virus. Quantitative PCR and histopathological analysis of samples from these infected mice demonstrated that infection with a virus not expressing ORF4 results in a delayed infection in this system. In light of these findings we propose the name virulence factor 1, VF1 for this protein. The identification of VF1 represents the first characterization of an alternative open reading frame protein for the calicivirus family. The immune regulatory function of the MNV VF1 protein provide important perspectives for future research into norovirus biology and pathogenesis.",

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author = "Nora McFadden and Dalan Bailey and Guia Carrara and Alicia Benson and Yasmin Chaudhry and Amita Shortland and Jonathan Heeney and Felix Yarovinsky and Peter Simmonds and Andrew Macdonald and Ian Goodfellow",

year = "2011",

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doi = "10.1371/journal.ppat.1002413",

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T1 - Norovirus regulation of the innate immune response and apoptosis occurs via the product of the alternative open reading frame 4

AU - McFadden, Nora

AU - Bailey, Dalan

AU - Carrara, Guia

AU - Benson, Alicia

AU - Chaudhry, Yasmin

AU - Shortland, Amita

AU - Heeney, Jonathan

AU - Yarovinsky, Felix

AU - Simmonds, Peter

AU - Macdonald, Andrew

AU - Goodfellow, Ian

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N2 - Small RNA viruses have evolved many mechanisms to increase the capacity of their short genomes. Here we describe the identification and characterization of a novel open reading frame (ORF4) encoded by the murine norovirus (MNV) subgenomic RNA, in an alternative reading frame overlapping the VP1 coding region. ORF4 is translated during virus infection and the resultant protein localizes predominantly to the mitochondria. Using reverse genetics we demonstrated that expression of ORF4 is not required for virus replication in tissue culture but its loss results in a fitness cost since viruses lacking the ability to express ORF4 restore expression upon repeated passage in tissue culture. Functional analysis indicated that the protein produced from ORF4 antagonizes the innate immune response to infection by delaying the upregulation of a number of cellular genes activated by the innate pathway, including IFN-Beta. Apoptosis in the RAW264.7 macrophage cell line was also increased during virus infection in the absence of ORF4 expression. In vivo analysis of the WT and mutant virus lacking the ability to express ORF4 demonstrated an important role for ORF4 expression in infection and virulence. STAT1-/- mice infected with a virus lacking the ability to express ORF4 showed a delay in the onset of clinical signs when compared to mice infected with WT virus. Quantitative PCR and histopathological analysis of samples from these infected mice demonstrated that infection with a virus not expressing ORF4 results in a delayed infection in this system. In light of these findings we propose the name virulence factor 1, VF1 for this protein. The identification of VF1 represents the first characterization of an alternative open reading frame protein for the calicivirus family. The immune regulatory function of the MNV VF1 protein provide important perspectives for future research into norovirus biology and pathogenesis.

AB - Small RNA viruses have evolved many mechanisms to increase the capacity of their short genomes. Here we describe the identification and characterization of a novel open reading frame (ORF4) encoded by the murine norovirus (MNV) subgenomic RNA, in an alternative reading frame overlapping the VP1 coding region. ORF4 is translated during virus infection and the resultant protein localizes predominantly to the mitochondria. Using reverse genetics we demonstrated that expression of ORF4 is not required for virus replication in tissue culture but its loss results in a fitness cost since viruses lacking the ability to express ORF4 restore expression upon repeated passage in tissue culture. Functional analysis indicated that the protein produced from ORF4 antagonizes the innate immune response to infection by delaying the upregulation of a number of cellular genes activated by the innate pathway, including IFN-Beta. Apoptosis in the RAW264.7 macrophage cell line was also increased during virus infection in the absence of ORF4 expression. In vivo analysis of the WT and mutant virus lacking the ability to express ORF4 demonstrated an important role for ORF4 expression in infection and virulence. STAT1-/- mice infected with a virus lacking the ability to express ORF4 showed a delay in the onset of clinical signs when compared to mice infected with WT virus. Quantitative PCR and histopathological analysis of samples from these infected mice demonstrated that infection with a virus not expressing ORF4 results in a delayed infection in this system. In light of these findings we propose the name virulence factor 1, VF1 for this protein. The identification of VF1 represents the first characterization of an alternative open reading frame protein for the calicivirus family. The immune regulatory function of the MNV VF1 protein provide important perspectives for future research into norovirus biology and pathogenesis.

KW - Amino Acid Sequence

KW - Animals

KW - Apoptosis

KW - Blotting, Western

KW - Caliciviridae Infections

KW - Enzyme-Linked Immunosorbent Assay

KW - Gene Expression Regulation

KW - Immunity, Innate

KW - Immunoprecipitation

KW - Mice

KW - Mice, Inbred C57BL

KW - Mice, Knockout

KW - Mitochondria

KW - Molecular Sequence Data

KW - Norovirus

KW - Open Reading Frames

KW - RNA, Viral

KW - Real-Time Polymerase Chain Reaction

KW - Reverse Genetics

KW - Reverse Transcriptase Polymerase Chain Reaction

KW - Viral Proteins

KW - Virulence

KW - Virulence Factors

KW - Virus Replication

U2 - 10.1371/journal.ppat.1002413

DO - 10.1371/journal.ppat.1002413

M3 - Article

C2 - 22174679

SN - 1553-7366

VL - 7

SP - e1002413

JO - PLoS pathogens

JF - PLoS pathogens

IS - 12

ER -

Norovirus regulation of the innate immune response and apoptosis occurs via the product of the alternative open reading frame 4

Abstract

Keywords

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