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Genetic mapping of the cold-adapted phenotype of B/Ann Arbor/1/66, the master donor virus for live attenuated influenza vaccines (FluMist). | LitMetric

AI Article Synopsis

  • Cold-adapted B/Ann Arbor/1/66 serves as the master donor virus for the FluMist influenza B vaccine, with key internal genes contributing to its cold-adapted, temperature-sensitive, and attenuated properties.
  • Research identifies five specific amino acid locations in the RNA segments PA, NP, and PB2 that are crucial for the cold-adapted phenotype, demonstrating how changes can reverse or confer these characteristics in viruses.
  • Additionally, the MDV-B M1 gene influences virus replication efficiency at warmer temperatures, highlighting the intricate genetic factors that sustain the stability of the FluMist vaccine.

Article Abstract

Cold adapted (ca) B/Ann Arbor/1/66 is the master donor virus for the influenza B (MDV-B) vaccine component of the live attenuated influenza vaccine (FluMist). The six internal genes contributed by MDV-B confer the characteristic cold-adapted (ca), temperature-sensitive (ts) and attenuated (att) phenotypes to the vaccine strains. Previously, it has been determined that the PA and NP segments of MDV-B control the ts phenotype while the att phenotype requires the M segment in addition to PA and NP. Here, we show that the PA, NP and PB2 segments are responsible for the ca phenotype of MDV-B when examined in chicken cell lines. Five loci in three RNA segments, R630 in PB2, M431 in PA and A114, H410 and T509 in NP, are sufficient to allow efficient virus growth at 25 degrees C. Substitution of these five amino acids with wt (wild type) residues completely reverted the MDV-B ca phenotype. Conversely, introduction of these five ca amino acids into B/Yamanashi/166/98 imparted the ca phenotype to this heterologous wt virus. In addition, we also found that the MDV-B M1 gene affected virus replication in chicken cells at 33 and 37 degrees C. Recombinant viruses containing the two MDV-B M1 residues (Q159, V183) replicated less efficiently than those containing wt M1 residues (H159, M183) at 33 and 37 degrees C, implicating the role of the MDV-B M segment to the att phenotype. The complexity of the multigenic signatures controlling the ca, ts and att phenotypes of MDV-B provides the molecular basis for the observed genetic stability of the FluMist vaccines.

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Source
http://dx.doi.org/10.1016/j.virol.2005.10.005DOI Listing

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