Статья

Live attenuated influenza vaccine viral vector induces functional cytotoxic T-cell immune response against foreign CD8+ T-cell epitopes inserted into NA and NS1 genes using the 2A self-cleavage site

T. Kotomina, D. Korenkov, V. Matyushenko, P. Prokopenko, L. Rudenko, I. Isakova-Sivak,
2021

The development of viral vector vaccines against various pathogens for which conventional vaccination approaches are not applicable has been a priority for a number of years. One promising approach is the insertion of immunodominant conservative cytotoxic T-cell (CTL) epitopes into the genome of a viral vector, which then delivers these epitopes to target cells, inducing immunity. Many different viruses have been assessed as viral vectors for CTL-based vaccines, but only a few of them are clinically relevant, mainly because of safety issues and limited knowledge about their performance in humans. In this regard, the use of licensed cold-adapted live attenuated influenza vaccine (LAIV) viruses as a vector delivery system has clear advantages for CTL-based vector vaccines against other respiratory pathogens: LAIV is known to induce all arms of the adaptive immune system and is administered via nasal spray, and its production process is relatively easy and inexpensive. Here we present the first results of the use of an LAIV backbone for designing a CTL epitope-based vaccine against respiratory syncytial virus (RSV). The chimeric LAIV-RSV vaccine candidates were attenuated in mice and induced strong, fully functional CTL immunity in this animal model. © 2018, © 2018 Taylor & Francis Group, LLC.

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  • 1. Version of Record от 2021-04-27

Метаданные

Об авторах
  • T. Kotomina
    Department of Virology, Institute of Experimental Medicine, Saint Petersburg, Russian Federation
  • D. Korenkov
  • V. Matyushenko
  • P. Prokopenko
  • L. Rudenko
  • I. Isakova-Sivak
Название журнала
  • Human Vaccines and Immunotherapeutics
Том
  • 14
Выпуск
  • 12
Страницы
  • 2964-2970
Ключевые слова
  • amino acid; epitope; gamma interferon; hemagglutinin; influenza vaccine; major histocompatibility antigen class 1; major histocompatibility antigen class 2; nonstructural protein 1; nose spray; peptide; recombinant vaccine; respiratory syncytial virus vaccine; sialidase; virus RNA; virus vector; adaptive immunity; amino terminal sequence; animal cell; animal experiment; animal model; Article; carboxy terminal sequence; CD8+ T lymphocyte; cellular immunity; cold acclimatization; cytotoxic T lymphocyte; cytotoxicity assay; female; high performance liquid chromatography; Human respiratory syncytial virus; immune response; infectious dose; Influenza A virus (H7N9); mass immunization; MDCK cell line; mouse; nonhuman; plasmid; respiratory virus; target cell; Teschovirus; virus load; virus particle; virus replication
Издатель
  • Taylor and Francis Inc.
Тип документа
  • journal article
Источник
  • scopus