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Molecular basis for the host range function of the poxvirus PKR inhibitor E3.

Sherry L HallerChorong ParkRyan C BruneauDewi MegawatiChi ZhangSameera VipatChen PengTatiana G SenkevichGreg BrennanLoubna TaziStefan Rothenburg
Published in: bioRxiv : the preprint server for biology (2024)
The molecular mechanisms that govern the host range of viruses are incompletely understood. A small number of poxvirus genes have been identified that influence the host range of poxviruses. We show that the host range functions of E3 and K3, two host range factors from vaccinia virus, are a result of species-specific interactions with the antiviral protein kinase R (PKR) and that PKR from closely related species displayed dramatic differences in their sensitivities to these viral inhibitors. While there is a substantial body of work demonstrating host-specific interactions with K3, the current model for E3-mediated PKR inhibition is that E3 non-specifically sequesters dsRNA to prevent PKR activation. This model does not predict species-specific sensitivity to E3; therefore, our data suggest that the current model is incomplete, and that dsRNA sequestration is not the primary mechanism for E3 activity.
Keyphrases
  • gene expression
  • genome wide
  • machine learning
  • drug induced