Longitudinal studies of chronically infected mice indeed reveal t

Longitudinal studies of chronically infected mice indeed reveal that the development of the exhausted phenotype of antigen-specific CD8 T cells occurs during a gradual progression of changes to the gene expression programme.[52, 58] Specifically, the reduction in check details cytokine production and killing potential is coupled to persistence of high viral load and is exacerbated in the absence of CD4 T-cell help.[59-61] What is not definitively demonstrated by these longitudinal studies is whether development of an exhaustion transcriptional programme is solely accomplished through survival of a subset of cells that were prone

to exhaustion or if the resulting phenotype is an acquired property obtained through progressive modification of transcriptional programmes in antigen-specific cells. To address Selleck Ulixertinib the issue of selection versus progression, the Walker laboratory recently investigated clonal selection of HIV-specific CD8 T cells from HIV controllers versus progressors. Their data indicate that the different functions

of HIV-specific CD8 T cells from HIV progressors versus HIV controllers is a result of the different chronic environments (high versus low viral load) promoting survival of distinct antigen-specific CD8 T-cell clones.[62] Further analysis is needed to completely resolve the contribution of clonal selection of virus-specific cells as the majority of the functional data came from cells following ex vivo expansion. It is important to note that these data do not rule out the progression of transcriptional regulation. The apparent gross difference in gene expression profiles between functional memory and exhausted antigen-specific

almost T cells as well as the recent report by the Walker laboratory on distinct clonal selection during differing severities of HIV infection raise the question as to whether the state of exhaustion is obtained through progressive changes in gene regulation. An initial examination of this complex issue has been performed using mouse model systems. West et al.[63] controlled for clonal selection by adoptively transferring clonal naive and functional memory CD8 T cells (generated from P14 TCR transgenic mice) into naive recipient mice, which were then challenged with the chronic strain of lymphocytic choriomeningitis virus. Surprisingly, naive cells were better suited than functional memory cells for generating cells that persisted during chronic infection. These data demonstrate that naive cells contain a cell intrinsic mechanism that allows them to adapt to the chronic antigen whereas this mechanism is absent in memory CD8 T cells. In a different set of experiments, Shin et al.[64] showed that exhausted CD8 T cells that were adoptively transferred into naive mice or epitope variant chronic infection-matched mice decline over the course of several weeks in the absence of TCR ligation.

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