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

Nogales, Aitor; Rodríguez, Laura; DeDiego, Marta L.; Topham, David J.; Martínez-Sobrido, Luis

doi:10.1128/jvi.00720-17

Cited by 49 publications

(116 citation statements)

References 69 publications

(150 reference statements)

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“…It has been shown that multiple mechanisms are related to host shutoff in IAV-infected cells. However, recent studies have focused on the following three main mechanisms of global inhibition of host protein expression by IAV infection: (1) blockade of cellular mRNA processing and nuclear export by NS1 [16][17][18][19]; (2) degradation of host RNA Pol II by the viral RNA-dependent RNA polymerase RdRp complex (RdRP) [20][21][22]; and (3) wide-spread host mRNA degradation by the PA-X protein [11,[23][24][25][26][27][28][29][30][31]. In this review, we focus mainly on the shutoff activity of PA-X protein.…”

Section: Global Host-shutoff Activity By the Pa-x Proteinmentioning

confidence: 99%

“…When considering the role of NS1 and PA-X in viral pathogenicity and host shutoff, it is very interesting to see the combined effects of them in modulating viral virulence. Therefore, recently, Nogales et al investigated the interplay of PA-X and NS1-mediated host shutoff in viral replication and pathogenesis using a temperature-sensitive 2009 pandemic H1N1 virus [31]. These researchers found that viruses that simultaneously encode PA-X and NS1, or are deficient in both proteins, are highly attenuated in vivo, suggesting that there is a strict balance between NS1 and PA-X proteins during host gene expression regulation, viral replication, and pathogenesis.…”

Section: Concerted Effect Of Pa-x and Ns1 In Host Shutoff And Pathogementioning

confidence: 99%

“…Thus, these studies clearly suggest that the effects of PA-X on viral replication and virulence are strain or host specific. Considering the concerted role for PA-X and NS1 in blockading host gene expression [28,31], we envisage that the precise impact of PA-X on viral growth and -, [11] Increase in mice [11] Increase in mice [11] -, [11] Increase in mice [11] H5N1(avian) Increase in various mammalian and avian cells, and in mice, chickens, ducks [24,35,84] Increase in 293T, CEF, DEF cells [24,35,84] Increase in CEF, DEF, MDCK and A549 cells [24,35,84] Increase in chickens, ducks and mice [24,35,84] Increase in MDCK cells [35,84) and A549 cells (35] Increase in mice, chickens, ducks [24,35,84] H1N1(2009 pdm) Increase in A549 cells and mice [35]; decrease in Calu-3 cells and mice [33]; decrease in MDCK, A549 and mice [34] Increase in 293T cells [35]; decrease in 293T cells [34] Increase in A549 cells [33][34][35] Increase in mice [35] Increase in A549 cells [35] Increase in mice [33,35]; decrease in mice [34] H9N2 (avian) Have no effect in MDCK and A549 cells, decrease in mice [36] -, [36] Decrease in A549 cells…”

Section: Effects Of Loss Of Pa-x Expression On Virulence In Influenzamentioning

confidence: 99%

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PA-X: a key regulator of influenza A virus pathogenicity and host immune responses

Liu

2018

Med Microbiol Immunol

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PA-X, a fusion protein belonging to influenza A viruses (IAVs), integrating the N-terminal 191 amino acids of PA gene and the ribosomal frame-shifting product that lengthens out to 41 or 61 amino acids. Since its discovery in 2012, multiple functions have been attributed to this small protein, including a process, where wide-spread protein synthesis in infected host cells is shut down (called host shutoff), and viral replication, polymerase activity, viral-induced cell apoptosis, PA nuclear localization, and virulence are modulated. However, many of its proposed functions may be specific to strain, subtype, host, or cell line. In this review, we start by describing the well-defined global host-shutoff ability of PA-X and the potential mechanisms underlying it. We move on to the role played by PA-X in modulating innate and acquired immune responses in the host. We then systematically discuss the role played by PA-X in modulating the virulence of influenza viruses of different subtypes and host origins, and finish with a general overview of the research advances made in identifying the host cell partners that interact with PA-X. To uncover possible clues about the differential effects of PA-X in modulating viral virulence, we focus on systemically evaluating polymorphisms in PA-X from various viral subtypes and hosts, including avian and human H5N1, H5N6, H9N2, and H7N9 viruses. Finally, we conclude with a proposition regarding the possible future research directions for this important protein.

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Section: Global Host-shutoff Activity By the Pa-x Proteinmentioning

confidence: 99%

Section: Concerted Effect Of Pa-x and Ns1 In Host Shutoff And Pathogementioning

confidence: 99%

Section: Effects Of Loss Of Pa-x Expression On Virulence In Influenzamentioning

confidence: 99%

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PA-X: a key regulator of influenza A virus pathogenicity and host immune responses

Liu

2018

Med Microbiol Immunol

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“…NS1 is a multifunctional protein and a key viral factor that counteracts the host antiviral responses. NS1 has been shown to inhibit the production of interferon (IFN), the activity and expression of multiple interferon-induced genes (ISG) and the processing and nuclear transport of host mRNAs causing cellular shut-off [25,26]. Segment 3 of IAV also encodes two proteins, the polymerase component PA and PA-X.…”

mentioning

confidence: 99%

“…Synergistically with NS1, PA-X is also able to block the cellular antiviral responses by inhibiting host protein expression. Moreover, the PA-X protein has been shown to modulate host inflammation, immune responses, apoptosis, and virus pathogenesis [25][26][27][28][29][30].…”

mentioning

confidence: 99%

Host Single Nucleotide Polymorphisms Modulating Influenza A Virus Disease in Humans

Nogales¹,

DeDiego

2019

Pathogens

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A large number of human genes associated with viral infections contain single nucleotide polymorphisms (SNPs), which represent a genetic variation caused by the change of a single nucleotide in the DNA sequence. SNPs are located in coding or non-coding genomic regions and can affect gene expression or protein function by different mechanisms. Furthermore, they have been linked to multiple human diseases, highlighting their medical relevance. Therefore, the identification and analysis of this kind of polymorphisms in the human genome has gained high importance in the research community, and an increasing number of studies have been published during the last years. As a consequence of this exhaustive exploration, an association between the presence of some specific SNPs and the susceptibility or severity of many infectious diseases in some risk population groups has been found. In this review, we discuss the relevance of SNPs that are important to understand the pathology derived from influenza A virus (IAV) infections in humans and the susceptibility of some individuals to suffer more severe symptoms. We also discuss the importance of SNPs for IAV vaccine effectiveness. multiple mechanisms, although there are some differences between strains. For that genome plasticity, IAV take advantage of multiple strategies, such as alternative splicing, frameshift mechanisms, and overlapping open reading frames (ORFs) [7][8][9]. In addition, the coding capability of the viral genome is extended by encoding multifunctional proteins that act at different steps during virus infection. of synthetized vRNP, ensuring that the vRNPs are available for packaging [24]. Moreover, NEP has also other functions during IAV infection, contributing to viral budding and to regulate viral RNA synthesis. NS1 is a multifunctional protein and a key viral factor that counteracts the host antiviral responses. NS1 has been shown to inhibit the production of interferon (IFN), the activity and expression of multiple interferon-induced genes (ISG) and the processing and nuclear transport of host mRNAs causing cellular shut-off [25,26]. Segment 3 of IAV also encodes two proteins, the polymerase component PA and PA-X. PA is translated directly from the PA mRNA, whereas PA-X is translated using a +1 frameshift mechanism from the same open reading frame (ORF) [9]. Synergistically with NS1, PA-X is also able to block the cellular antiviral responses by inhibiting host protein expression. Moreover, the PA-X protein has been shown to modulate host inflammation, immune responses, apoptosis, and virus pathogenesis [25][26][27][28][29][30].

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Nucleoprotein phosphorylation site (Y385) mutation confers temperature sensitivity to influenza A virus due to impaired nucleoprotein oligomerization at a lower temperature

Zheng

Cui

et al. 2020

Sci. China Life Sci.

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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

Cited by 49 publications

References 69 publications

PA-X: a key regulator of influenza A virus pathogenicity and host immune responses

PA-X: a key regulator of influenza A virus pathogenicity and host immune responses

Host Single Nucleotide Polymorphisms Modulating Influenza A Virus Disease in Humans

Nucleoprotein phosphorylation site (Y385) mutation confers temperature sensitivity to influenza A virus due to impaired nucleoprotein oligomerization at a lower temperature

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