Abstract
Control of chronic viral infections by CD8 T cells is critically dependent on CD4 help. In particular, helper-derived IL-21 plays a key role in sustaining the CD8 T cell response; however, the molecular pathways by which IL-21 sustains CD8 T cell immunity remain unclear. We demonstrate that IL-21 causes a phenotypic switch of transcription factor expression in CD8 T cells during chronic viral infection characterized by sustained BATF expression. Importantly, BATF expression during chronic infection is both required for optimal CD8 T cell persistence and anti-viral effector function and sufficient to rescue "unhelped" CD8 T cells. Mechanistically, BATF sustains the response by cooperating with IRF4, an antigen-induced transcription factor that is also critically required for CD8 T cell maintenance, to preserve Blimp-1 expression and thereby sustain CD8 T cell effector function. Collectively, these data suggest that CD4 T cells "help" the CD8 response during chronic infection via IL-21-induced BATF expression. Xin et al. identify a pathway that connects CD4-derived IL-21 to a BATF-mediated transcriptional program in CD8 T cells, which plays a key role in the sustained effector function of CD8 T cells during chronic viral infection.
Original language | English |
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Pages (from-to) | 1118-1124 |
Number of pages | 7 |
Journal | Cell Reports |
Volume | 13 |
Issue number | 6 |
DOIs | |
Publication status | Published - 10 Nov 2015 |