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Off-target effects of an insect cell-expressed influenza HA-pseudotyped Gag-VLP preparation in limiting postinfluenza Staphylococcus aureus infections. | LitMetric

AI Article Synopsis

  • Influenza viruses can interact with Staphylococcus aureus, increasing the risk of severe bacterial pneumonia, a leading cause of death during influenza outbreaks, especially since there is no vaccine for S. aureus and antibiotic resistance is growing.
  • The study tested a vaccine using virus-like particles (VLP) that expressed an influenza protein in mice, finding that a single low dose could help prevent severe bacterial infections after influenza.
  • However, while the vaccine generated a strong immune response against the influenza virus, it wasn't enough to stop the replication of different strains of the virus or protect against subsequent bacterial infections, indicating that more comprehensive strategies may be needed.

Article Abstract

Clinical and historical data underscore the ability of influenza viruses to ally with Staphylococcus aureus and predispose the host for secondary bacterial pneumonia, which is a leading cause of influenza-associated mortality. This is fundamental because no vaccine for S. aureus is available and the number of antibiotic-resistant strains is alarmingly rising. Hence, this leaves influenza vaccination the only strategy to prevent postinfluenza staphylococcal infections. In the present work, we assessed the off-target effects of a Tnms42 insect cell-expressed BEI-treated Gag-VLP preparation expressing the HA of A/Puerto Rico/8/1934 (H1N1) in preventing S. aureus superinfection in mice pre-infected with a homologous or heterologous H1N1 viral challenge strain. Our results demonstrate that matched anti-hemagglutinin immunity elicited by a VLP preparation may suffice to prevent morbidity and mortality caused by lethal secondary bacterial infection. This effect was observed even when employing a single low antigen dose of 50 ng HA per animal. However, induction of anti-hemagglutinin immunity alone was not helpful in inhibiting heterologous viral replication and subsequent bacterial infection. Our results indicate the potential of the VLP vaccine approach in terms of immunogenicity but suggest that anti-HA immunity should not be considered as the sole preventive method for combatting influenza and postinfluenza bacterial infections.

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Source
http://dx.doi.org/10.1016/j.vaccine.2019.10.083DOI Listing

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