Author: Amici, Carla; La Frazia, Simone; Brunelli, Claudia; Balsamo, Mirna; Angelini, Mara; Santoro, M. Gabriella
Title: Inhibition of viral protein translation by indomethacin in vesicular stomatitis virus infection: role of eIF2α kinase PKR Cord-id: slj53no5 Document date: 2015_5_13
ID: slj53no5
Snippet: Indomethacin, a cyclooxygenaseâ€1 and â€2 inhibitor widely used in the clinic for its potent antiâ€inflammatory/analgesic properties, possesses antiviral activity against several viral pathogens; however, the mechanism of antiviral action remains elusive. We have recently shown that indomethacin activates the doubleâ€stranded RNA (dsRNA)â€dependent protein kinase R (PKR) in human colon cancer cells. Because of the important role of PKR in the cellular defence response against viral infectio
Document: Indomethacin, a cyclooxygenaseâ€1 and â€2 inhibitor widely used in the clinic for its potent antiâ€inflammatory/analgesic properties, possesses antiviral activity against several viral pathogens; however, the mechanism of antiviral action remains elusive. We have recently shown that indomethacin activates the doubleâ€stranded RNA (dsRNA)â€dependent protein kinase R (PKR) in human colon cancer cells. Because of the important role of PKR in the cellular defence response against viral infection, herein we investigated the effect of indomethacin on PKR activity during infection with the prototype rhabdovirus vesicular stomatitis virus. Indomethacin was found to activate PKR in an interferon†and dsRNAâ€independent manner, causing rapid (< 5 min) phosphorylation of eukaryotic initiation factorâ€2 αâ€subunit (eIF2α). These events resulted in shutting off viral protein translation and blocking viral replication (IC (50) = 2 μM) while protecting host cells from virusâ€induced damage. Indomethacin did not affect eIF2α kinases PKRâ€like endoplasmic reticulumâ€resident protein kinase (PERK) and general control nonâ€derepressibleâ€2 (GCN2) kinase, and was unable to trigger eIF2α phosphorylation in the presence of PKR inhibitor 2â€aminopurine. In addition, smallâ€interfering RNAâ€mediated PKR gene silencing dampened the antiviral effect in indomethacinâ€treated cells. The results identify PKR as a critical target for the antiviral activity of indomethacin and indicate that eIF2α phosphorylation could be a key element in the broad spectrum antiviral activity of the drug.
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