The associated mechanisms remain nevertheless elusive. Although progress has been made in identifying determinants of influenza virus transmissibility, α2,6 receptor binding affinity and infection of the upper regions of the respiratory
tract, resulting in excretion of high viral titers, appear not sufficient to allow airborne transmission of avian influenza viruses in mammals. LPAIV H9N2 with α2,6 receptor binding affinity were transmitted via contact Small Molecule Compound Library but not aerosols in ferrets [156]. Likewise, most HPAIV H5N1 engineered to preferentially attach to sialic acids with α2,6 linkage to galactose replicate in the upper regions of the respiratory tract still do not efficiently transmit in animal models, at best only by contact [155]. A handful substitutions in the HA protein of HPAIV H5N1, of which only some were necessary http://www.selleckchem.com/products/epacadostat-incb024360.html to confer α2,6 receptor binding affinity, were necessary to allow airborne transmission of the virus in ferrets [161]. It has been suggested that besides α2,6 receptor binding affinity
and replication to high viral titers in the upper regions of the respiratory tract, more subtle differences in receptor preference and the formation and release of single influenza virus particles, mediated by balanced activity of the HA and NA proteins, represent additional requirements for efficient airborne transmission [155]. Pre-existing immunity in the human population is known to have a marked effect on the epidemic dynamics of influenza virus. In particular, the antigenic shift following the introduction of transmissible zoonotic influenza viruses largely contributes to the development of influenza pandemics, whereby viral spread in the population is unhampered by pre-existing Parvulin immunity. The antigenic shift allows pandemic viruses to invade greater portions of the human
population as well as greater portions of the respiratory tract within individual hosts, typically resulting in more extensive epidemic waves and more severe disease [162] and [163]. The pandemic of 1918 was triggered by influenza virus H1N1 and resulted in 30–50 million deaths [164]. The animal origin of this virus is unclear. Phylogenetic analyses of the eight gene segments of a reconstructed 1918 H1N1 virus [165] placed all gene sequences in the mammalian clade, which contains human and swine strains. However, they were found more closely related to avian isolates than to any other mammalian isolates of influenza virus [166], [167], [168], [169], [170] and [171]. Further analyses suggested that the pandemic virus likely resulted from reassortment events between mammalian and avian viruses [172]. In particular, the PB1 and PA genes appeared to be of recent avian origin.
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