2011
DOI: 10.1128/jvi.05582-11
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Increased Pathogenicity of a Reassortant 2009 Pandemic H1N1 Influenza Virus Containing an H5N1 Hemagglutinin

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Cited by 45 publications
(52 citation statements)
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“…The primer sequences are presented in Table 2. sortant CA/09 viruses expressing individual HK/483 viral genes were generated (30). The reassortant viruses all replicated to similar levels in MDCK cells (30).…”
Section: Resultsmentioning
confidence: 99%
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“…The primer sequences are presented in Table 2. sortant CA/09 viruses expressing individual HK/483 viral genes were generated (30). The reassortant viruses all replicated to similar levels in MDCK cells (30).…”
Section: Resultsmentioning
confidence: 99%
“…Unbound virus was removed, and the cells were washed in PBS and maintained in RPMI 1640 medium containing 0.075% bovine serum albumin (BSA) in the presence (non-H5 viruses and low-pathogenicity H5 viruses) or absence (HPAI H5 viruses) of 1 g of TPCK (tolylsulfonyl phenylalanyl chloromethyl ketone)-treated trypsin (Pierce, Rockford, IL)/ml. Cell culture medium was removed at the indicated times and stored at Ϫ80°C for the determination of virus titers by TCID 50 analysis on MDCK cells as described previously (30). All TCID 50 titers are normalized to background levels of residual virus remaining in the culture wells after the inoculum was washed off.…”
Section: Ethicsmentioning
confidence: 99%
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“…When the replicative capacity of a panel of eight H5N1 viruses was tested in RAW264.7 cells, only those associated with high virulence in mammals were capable of productive replication, demonstrating a correlation between replication in macrophages and disease severity [39]. Further, a reassortant CA/09 virus expressing the HA protein from a HPAI H5 virus was capable of productive replication in macrophages and was associated with higher morbidity and mortality in mice relative to the WT CA/09 virus, which does not replicate in macrophages [51]. The increased disease severity was not linked directly to the ability of the virus to replicate in macrophages in this study, but it is intriguing to speculate that productive replication of H5N1 viruses in macrophages may alter antiviral macrophage functions in ways that lead to enhanced disease severity.…”
Section: Impact Of Productive Replication In Macrophages On Iav Pathomentioning
confidence: 99%
“…Reverse genetics-derived reassortant viruses (RGd-RV) that possess the H5N1 (H5) HA in an otherwise H3N2 genetic background show high replicative capacities in MDCK cells (10). Similarly, RGd-RV with the HA gene from H5N1 virus in the H1N1pdm2009 genetic background replicated efficiently in primary human respiratory epithelial cells and caused 100% mortality in mice (19). However, phylogenetic analyses of natural or experimental reassortant viruses have shown that the HA segment from avian, swine, or equine viruses was never incorporated alone in the genetic background of a human virus (13,14,20): The HA segment is packaged with additional groups of gene segments depending on the viral subtypes involved in the coinfection process (13,14).The inability to obtain a virus containing a nonhuman HA gene in an otherwise human genetic background, in contrast with the ability to produce "7+1" RGd-RV with a high yield of replication, suggests that the reassortment process might be restricted by suboptimal compatibility between the vRNA-packaging signals (10).…”
mentioning
confidence: 99%