Influenza A Infection of Primary Human Airway Epithelial
Cells Up-Regulates Proteins Related to Purine Metabolism and Ubiquitin-Related
Signaling
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Abstract
Virus–host interactions are
important determinants of virus
replication and immune responses, but they are not well-defined. In
this study we analyzed quantitative host protein alterations in nuclei-enriched
fractions from multiple primary human bronchial airway epithelial
(HBAE) cells infected by an H1N1 influenza A virus (A/PR/8/34). We
first developed an effective detergent-free nuclear lysis method that
was coupled with in-solution digestion and LC–MS/MS. Using
SILAC, we identified 837 HBAE nuclear proteins in three different
donors and compared their responses to infection at 24 h. Some proteins
were altered in all three donors, of which 94 were up-regulated and
13 were down-regulated by at least 1.5-fold. Many of these up-regulated
proteins clustered into purine biosynthesis, carbohydrate metabolism,
and protein modification. Down-regulated proteins were not associated
with any specific pathways or processes. These findings further our
understanding of cellular processes that are altered in response to
influenza in primary epithelial cells and may be beneficial in the
search for host proteins that may be targeted for antiviral therapy