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After virus exposure, early bystander naïve CD8 T cell activation relies on NAD+ salvage metabolism
oleh: Namit Holay, Barry E. Kennedy, Barry E. Kennedy, J. Patrick Murphy, J. Patrick Murphy, Prathyusha Konda, Prathyusha Konda, Michael Giacomantonio, Tatjana Brauer-Chapin, Tatjana Brauer-Chapin, Joao A. Paulo, Vishnupriyan Kumar, Youra Kim, Mariam Elaghil, Mariam Elaghil, Gary Sisson, Derek Clements, Derek Clements, Christopher Richardson, Christopher Richardson, Christopher Richardson, Steven P. Gygi, Shashi Gujar, Shashi Gujar, Shashi Gujar, Shashi Gujar, Shashi Gujar
Format: | Article |
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Diterbitkan: | Frontiers Media S.A. 2023-02-01 |
Deskripsi
CD8 T cells play a central role in antiviral immunity. Type I interferons are among the earliest responders after virus exposure and can cause extensive reprogramming and antigen-independent bystander activation of CD8 T cells. Although bystander activation of pre-existing memory CD8 T cells is known to play an important role in host defense and immunopathology, its impact on naïve CD8 T cells remains underappreciated. Here we report that exposure to reovirus, both in vitro or in vivo, promotes bystander activation of naïve CD8 T cells within 24 hours and that this distinct subtype of CD8 T cell displays an innate, antiviral, type I interferon sensitized signature. The induction of bystander naïve CD8 T cells is STAT1 dependent and regulated through nicotinamide phosphoribosyl transferase (NAMPT)-mediated enzymatic actions within NAD+ salvage metabolic biosynthesis. These findings identify a novel aspect of CD8 T cell activation following virus infection with implications for human health and physiology.