Persistent Ag induces a dysfunctional CD8 T cell state known as "exhaustion" characterized by PD-1 expression. Nevertheless, exhausted CD8 T cells retain functionality through continued differentiation of progenitor into effector cells. However, it remains ill-defined how CD8 T cell effector responses are sustained in situ. In this study, we show using the mouse chronic lymphocytic choriomeningitis virus infection model that CX3CR1 CD8 T cells contain a T-bet-dependent TIM3PD-1 subpopulation that is distinct from the TIM3CX3CR1PD-1 proliferative effector subset. The TIM3CX3CR1 cells are quiescent and express a low but significant level of the transcription factor TCF-1, demonstrating similarity to TCF-1 progenitor CD8 T cells. Furthermore, following the resolution of lymphocytic choriomeningitis virus viremia, a substantial proportion of TCF-1 memory-like CD8 T cells show evidence of CX3CR1 expression during the chronic phase of the infection. Our results suggest a subset of the CX3CR1 exhausted population demonstrates progenitor-like features that support the generation of the CX3CR1 effector pool from the TCF-1 progenitors and contribute to the memory-like pool following the resolution of viremia.
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| http://dx.doi.org/10.4049/jimmunol.2001348 | DOI Listing |
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