Abstract
Earlier we reported that NF-κB is activated by protein kinase R (PKR) in herpes simplex virus 1-infected cells. Here we report that in PKR -/- cells the yields of wild-type virus are 10-fold higher than in PKR+/+ cells. In cells lacking NF-κB p50 (nfkb1), p65 (relA), or both p50 and p65, the yields of virus were reduced 10-fold. Neither wild-type nor mutant cells undergo apoptosis following infection with wild-type virus. Whereas PKR+/+ and NF-κB+/+ control cell lines undergo apoptosis induced by the d120 (Δα4) mutant of HSV-1, the mutant PKR-/- and HF=κB-/- cell lines were resistant. The evidence suggests that the stress-induced apoptosis resulting from d120 infection requires activation of NF-κB and that this proapoptotic pathway is blocked in cells in which NF-κB is not activated or absent. Activation of NF-κB in the course of viral infection may have dual roles of attempting to curtain viral replication by rendering the cell susceptible to apoptosis induced by the virus and by inducing the synthesis of proteins that enhance viral replication.
Original language | English |
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Pages (from-to) | 11615-11621 |
Number of pages | 7 |
Journal | Journal of Virology |
Volume | 78 |
Issue number | 21 |
DOIs | |
State | Published - Nov 2004 |