PA-X is a virulence factor in avian H9N2 influenza virus

Gao, Huijie; Xu, Guanlong; Sun, Yipeng; Lu, Quan; Wang, Jinliang; Kong, Weili; Sun, Honglei; Pu, Juan; Chang, Kin-Chow; Liu, Jinhua

doi:10.1099/jgv.0.000232

Cited by 56 publications

(78 citation statements)

References 22 publications

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“…9 and Table 1). These data are consistent with previous findings describing that a pH1N1 WT virus showed a slightly increased virulence in mice compared to a virus expressing lower levels of the PA-X protein (21,35). Remarkably, by using our pH1N1 LAIV virus, we have observed greater differences in virus pathogenicity than those observed using pH1N1 WT, suggesting that the LAIV virus backbone is better suited to detect differences in pathogenicity than the WT backbone.…”

Section: Discussionsupporting

confidence: 82%

“…Similarly, Gao et al (43) and Hu et al (16) reported that loss of PA-X expression increased viral replication and pathogenicity of pH1N1 and H5N1 IAVs. In contrast, recent work has described that loss of PA-X in pH1N1 or H9N2 viruses leads to a reduction in viral pathogenicity (21,35). In addition, IAV strain-specific differences in the ability to block the cellular protein synthesis have also been reported (25,(31)(32)(33).…”

Section: Discussionmentioning

confidence: 75%

“…Multiple functions have been attributed to PA-X, including degradation of host mRNA that leads to inhibition of host protein synthesis and contributes to blocking the cellular antiviral responses (15)(16)(17)(18)(19). Moreover, the PA-X protein has been shown to be involved in modulating host inflammation, the immune response, and apoptosis (15,17,(20)(21)(22). Although PA and PA-X have the same N-terminal domain, PA-X has a much stronger endonucleolytic activity, indicating that the C-terminal region is responsible for the inhibition of the host protein expression (23).…”

mentioning

confidence: 99%

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Interplay of PA-X and NS1 Proteins in Replication and Pathogenesis of a Temperature-Sensitive 2009 Pandemic H1N1 Influenza A Virus

Nogales

Rodríguez

DeDiego

et al. 2017

J Virol

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Influenza A viruses (IAVs) cause seasonal epidemics and occasional pandemics, representing a serious public health concern. It has been described that one mechanism used by some IAV strains to escape the host innate immune responses and modulate virus pathogenicity involves the ability of the PA-X and NS1 proteins to inhibit the host protein synthesis in infected cells. It was reported that for the 2009 pandemic H1N1 IAV (pH1N1) only the PA-X protein had this inhibiting capability, while the NS1 protein did not. In this work, we have evaluated, for the first time, the combined effect of PA-X- and NS1-mediated inhibition of general gene expression on virus pathogenesis, using a temperature-sensitive, live-attenuated 2009 pandemic H1N1 IAV (pH1N1 LAIV). We found that viruses containing PA-X and NS1 proteins that simultaneously have (PA/NS1) or do not have (PA/NS1) the ability to block host gene expression showed reduced pathogenicity However, a virus where the ability to inhibit host protein expression was switched between PA-X and NS1 (PA/NS1) presented pathogenicity similar to that of a virus containing both wild-type proteins (PA/NS1). Our findings suggest that inhibition of host protein expression is subject to a strict balance, which can determine the successful progression of IAV infection. Importantly, knowledge obtained from our studies could be used for the development of new and more effective vaccine approaches against IAV. Influenza A viruses (IAVs) are one of the most common causes of respiratory infections in humans, resulting in thousands of deaths annually. Furthermore, IAVs can cause unpredictable pandemics of great consequence when viruses not previously circulating in humans are introduced into humans. The defense machinery provided by the host innate immune system limits IAV replication; however, to counteract host antiviral activities, IAVs have developed different inhibition mechanisms, including prevention of host gene expression mediated by the viral PA-X and NS1 proteins. Here, we provide evidence demonstrating that optimal control of host protein synthesis by IAV PA-X and/or NS1 proteins is required for efficient IAV replication in the host. Moreover, we demonstrate the feasibility of genetically controlling the ability of IAV PA-X and NS1 proteins to inhibit host immune responses, providing an approach to develop more effective vaccines to combat disease caused by this important respiratory pathogen.

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Section: Discussionsupporting

confidence: 82%

Section: Discussionmentioning

confidence: 75%

mentioning

confidence: 99%

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Interplay of PA-X and NS1 Proteins in Replication and Pathogenesis of a Temperature-Sensitive 2009 Pandemic H1N1 Influenza A Virus

Nogales

Rodríguez

DeDiego

et al. 2017

J Virol

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“…Several previous reports have examined the effects of PA-X on host response by comparing wild type and mutant virus infections, and shown that PA-X was important for modulating various immune responses (2, 6–8, 12, 14). To further elucidate PA-X’s effects on the host, we transfected plasmids expressing only PA-X into cell cultures and used RNA-seq to analyze the transcripts.…”

Section: Discussionmentioning

confidence: 99%

“…This ribonuclease domain has been attributed to the N terminal region, although several recent publications have shown that the C-terminal region may also be important in regulating ribonuclease activity (10, 12, 13). Interestingly, PA-X has also been shown to modulate other virus-host interactions such as preventing stress granule formation (and thereby preventing translational arrest), increasing the accumulation of poly(A)-binding proteins within the nucleus, and exhibiting anti-apoptotic activity (5, 6, 14). …”

Section: Introductionmentioning

confidence: 99%

Comparing the functions of equine and canine influenza H3N8 virus PA-X proteins: Suppression of reporter gene expression and modulation of global host gene expression

et al. 2016

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The influenza PA-X protein is translated from the PA open reading frame from frameshifting and suppresses cellular gene expression due to its ribonuclease activity. We further defined the functional roles of PA-X by comparing PA-X proteins from two related viruses – equine influenza (EIV) and canine influenza (CIV) H3N8 – that differ in a C-terminal truncation and internal mutations. In vitro reporter gene assays revealed that both proteins were able to suppress gene expression. Interestingly, EIV PA-X demonstrated ~50% greater activity compared to CIV PA-X, and we identified the mutations that caused this difference. We used RNA-seq to evaluate the effects of PA-X on host gene expression after transfection into cultured cells. There were no significant differences in this property between EIV and CIV PA-X proteins, but expression of either resulted in the up-regulation of genes when compared to controls, most notably immunity-related proteins, trafficking proteins, and transcription factors.

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PA-X-associated early alleviation of the acute lung injury contributes to the attenuation of a highly pathogenic H5N1 avian influenza virus in mice

Zhao

et al. 2016

Med Microbiol Immunol

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PA-X is a novel discovered accessory protein encoded by the PA mRNA. Our previous study demonstrated that PA-X decreases the virulence of a highly pathogenic H5N1 strain A/Chicken/Jiangsu/k0402/2010 in mice. However, the underlying mechanism of virulence attenuation associated with PA-X is still unknown. In this study, we compared two PA-X-deficient mutant viruses and the parental virus in terms of induction of pathology and manipulation of host response in the mouse lung, stimulation of cell death and PA nuclear accumulation. We first found that down-regulated PA-X expression markedly aggravated the acute lung injury of the infected mice early on day 1 post-infection (p.i.). We then determined that loss of PA-X expression induced higher levels of cytokines, chemokines and complement-derived peptides (C3a and C5a) in the lung, especially at early time point's p.i. In addition, in vitro assays showed that the PA-X-deficient viruses enhanced cell death and increased expression of reactive oxygen species (ROS) in mammalian cells. Moreover, we also found that PA nuclear accumulation of the PA-X-null viruses accelerated in MDCK cells. These results demonstrate that PA-X decreases the level of complement components, ROS, cell death and inflammatory response, which may together contribute to the alleviated lung injury and the attenuation of the virulence of H5N1 virus in mice.

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PA-X is a virulence factor in avian H9N2 influenza virus

Cited by 56 publications

References 22 publications

Interplay of PA-X and NS1 Proteins in Replication and Pathogenesis of a Temperature-Sensitive 2009 Pandemic H1N1 Influenza A Virus

Interplay of PA-X and NS1 Proteins in Replication and Pathogenesis of a Temperature-Sensitive 2009 Pandemic H1N1 Influenza A Virus

Comparing the functions of equine and canine influenza H3N8 virus PA-X proteins: Suppression of reporter gene expression and modulation of global host gene expression

PA-X-associated early alleviation of the acute lung injury contributes to the attenuation of a highly pathogenic H5N1 avian influenza virus in mice

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