Natural Selection of H5N1 Avian Influenza A Viruses with Increased PA-X and NS1 Shutoff Activity

Nogales, Aitor; Villamayor, Laura; Utrilla-Trigo, Sergio; Ortego, Javier; Martínez-Sobrido, Luis; DeDiego, Marta L.

doi:10.3390/v13091760

Cited by 12 publications

(13 citation statements)

References 67 publications

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“…In this study, a variant virus harboring I127V in the PA was detected in the mice after the dosing of BXM at 0.5 mg/kg twice daily for 5 days. According to a previous report, V127 in the PA was highly conserved in a recent isolate of H5N1 viruses [67]. In addition, some of the H5 HPAIVs tested in the study harbored V127 in the PA (Table S4), and they were susceptible to BXA such as the A/Hong Kong/483/1997 (H5N1) strain.…”

Section: Discussionmentioning

confidence: 56%

Characterization of the In Vitro and In Vivo Efficacy of Baloxavir Marboxil against H5 Highly Pathogenic Avian Influenza Virus Infection

Taniguchi

Ando

Kobayashi

et al. 2022

Viruses

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Human infections caused by the H5 highly pathogenic avian influenza virus (HPAIV) sporadically threaten public health. The susceptibility of HPAIVs to baloxavir acid (BXA), a new class of inhibitors for the influenza virus cap-dependent endonuclease, has been confirmed in vitro, but it has not yet been fully characterized. Here, the efficacy of BXA against HPAIVs, including recent H5N8 variants, was assessed in vitro. The antiviral efficacy of baloxavir marboxil (BXM) in H5N1 virus-infected mice was also investigated. BXA exhibited similar in vitro activities against H5N1, H5N6, and H5N8 variants tested in comparison with seasonal and other zoonotic strains. Compared with oseltamivir phosphate (OSP), BXM monotherapy in mice infected with the H5N1 HPAIV clinical isolate, the A/Hong Kong/483/1997 strain, also caused a significant reduction in viral titers in the lungs, brains, and kidneys, thereby preventing acute lung inflammation and reducing mortality. Furthermore, compared with BXM or OSP monotherapy, combination treatments with BXM and OSP using a 48-h delayed treatment model showed a more potent effect on viral replication in the organs, accompanied by improved survival. In conclusion, BXM has a potent antiviral efficacy against H5 HPAIV infections.

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Section: Discussionmentioning

confidence: 56%

Characterization of the In Vitro and In Vivo Efficacy of Baloxavir Marboxil against H5 Highly Pathogenic Avian Influenza Virus Infection

Taniguchi

Ando

Kobayashi

et al. 2022

Viruses

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“…While PA-X sequences are fairly conserved across strains because of the constraints on both PA-X and PA coding regions, the PA-X from the pH1N1 strain has an X-ORF of 41 amino acids, compared to 61 amino acids for the PR8 and Perth strains (Shi et al, 2012). Moreover, PA-Xs from different strains have been reported to have differences in host shutoff activity (Feng et al, 2016;Nogales et al, 2021;Oishi et al, 2019;Wang et al, 2020). It would thus be interesting to investigate whether the X-ORF has an effect on the cut site specificity, especially as we only tested our best PA-X targets and the differences in cleavage specificity may be subtle.…”

Section: Discussionmentioning

confidence: 99%

The cut site specificity of the influenza A virus endoribonuclease PA-X allows it to discriminate between host and viral mRNAs

Gaucherand

Iyer

Gilabert

et al. 2022

Preprint

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Widespread shutoff of host gene expression through RNA degradation is an advantageous way for many viruses to block antiviral responses. However, viruses need to maintain expression of their own genes and host genes necessary for replication despite the RNA degradation. The influenza A virus host shutoff endoribonuclease PA-X solves this problem by discriminating between RNAs and sparing viral mRNAs and some host RNAs. To understand how PA-X distinguishes between RNAs, we identified and characterized PA-X cut sites transcriptome-wide. This analysis shows that PA-Xs from multiple influenza strains cleave RNAs at GCUG tetramers in hairpin loop structures. Importantly, GCUG tetramers are enriched in the human but not the influenza transcriptome. This finding suggests that PA-X evolved these cleavage characteristics to target host but not viral mRNAs. Our study reveals a new layer of PA-X specificity, and shows how viral endoribonuclease cleavage specificity plays a functional role to selectively target the host.

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“…This advantage has been broadly used to generate LAIV by introducing specific amino acid substitutions, or deletions, in the viral genome (Martinez-Sobrido et al, 2018;Rodriguez et al, 2018b;Blanco-Lobo et al, 2019;Hilimire et al, 2020). For instance, IAV encoding truncated versions of NS1 or where the NS1 sequence was completely removed (DNS1) have been generated and used as potential LAIV candidates in multiple animal species (Quinlivan et al, 2005;Solorzano et al, 2005;Richt et al, 2006;Vincent et al, 2007;Wang et al, 2008;Chambers et al, 2009;Steel et al, 2009;Kappes et al, 2012;Choi et al, 2015;Jang et al, 2016;Na et al, 2016;Chen et al, 2017;Nogales et al, 2017b;Jang et al, 2018;Nicolodi et al, 2019;Lee et al, 2021;Vandoorn et al, 2022a), or to study IAV infections (Nogales et al, 2021a), including the contribution of NS1, and its domains, in viral pathogenesis (Nogales et al, 2017a;Nogales et al, 2017c;Chauche et al, 2018;Nogales et al, 2018a;Nogales et al, 2018b;Nogales et al, 2021b). Because NS1 is the main countermeasure against cellular antiviral responses, the recovery of NS1 truncated or deficient viruses can be challenging, since these viruses have limited ability to inhibit the cellular innate immune responses induced during viral infection Kochs et al, 2007;Hale et al, 2008;Nogales et al, 2018b;Nogales et al, 2019b).…”

Section: Reverse Genetics Techniques For the Development Of Iav Vacci...mentioning

confidence: 99%

“…The ED is able to interact with multiple host factors, including cellular proteins involved in antiviral responses (Hale et al, 2008;Thulasi Raman and Zhou, 2016;Nogales et al, 2018b). However, many of these interactions can be strain-dependent, and host-adaptation processes could be important for this high variability (Kochs et al, 2007;Steidle et al, 2010;Marc, 2014;Clark et al, 2017;Nogales et al, 2017a;Nogales et al, 2017f;Chauche et al, 2018;Nogales et al, 2018a;Nogales et al, 2021b). The last domain is a C-terminal tail (CTT) of 11-33 amino acids, containing a PDZ-binding motif that is associated with IAV pathogenesis and is not present in all IAV NS1 proteins (Jackson et al, 2008;Hale, 2014).…”

Section: Ns1 Protein Structure and Functionsmentioning

confidence: 99%

Live attenuated influenza A virus vaccines with modified NS1 proteins for veterinary use

Nogales

DeDiego

Martínez-Sobrido

2022

Front. Cell. Infect. Microbiol.

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Influenza A viruses (IAV) spread rapidly and can infect a broad range of avian or mammalian species, having a tremendous impact in human and animal health and the global economy. IAV have evolved to develop efficient mechanisms to counteract innate immune responses, the first host mechanism that restricts IAV infection and replication. One key player in this fight against host-induced innate immune responses is the IAV non-structural 1 (NS1) protein that modulates antiviral responses and virus pathogenicity during infection. In the last decades, the implementation of reverse genetics approaches has allowed to modify the viral genome to design recombinant IAV, providing researchers a powerful platform to develop effective vaccine strategies. Among them, different levels of truncation or deletion of the NS1 protein of multiple IAV strains has resulted in attenuated viruses able to induce robust innate and adaptive immune responses, and high levels of protection against wild-type (WT) forms of IAV in multiple animal species and humans. Moreover, this strategy allows the development of novel assays to distinguish between vaccinated and/or infected animals, also known as Differentiating Infected from Vaccinated Animals (DIVA) strategy. In this review, we briefly discuss the potential of NS1 deficient or truncated IAV as safe, immunogenic and protective live-attenuated influenza vaccines (LAIV) to prevent disease caused by this important animal and human pathogen.

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Natural Selection of H5N1 Avian Influenza A Viruses with Increased PA-X and NS1 Shutoff Activity

Cited by 12 publications

References 67 publications

Characterization of the In Vitro and In Vivo Efficacy of Baloxavir Marboxil against H5 Highly Pathogenic Avian Influenza Virus Infection

Characterization of the In Vitro and In Vivo Efficacy of Baloxavir Marboxil against H5 Highly Pathogenic Avian Influenza Virus Infection

The cut site specificity of the influenza A virus endoribonuclease PA-X allows it to discriminate between host and viral mRNAs

Live attenuated influenza A virus vaccines with modified NS1 proteins for veterinary use

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