[No authors listed]
Generation of protective immunity to infections and vaccinations declines with age. Studies in healthy individuals have implicated reduced miR-181a expression in TÂ cells as contributing to this defect. To understand the impact of miR-181a expression on antiviral responses, we examined LCMV infection in mice with miR-181ab1-deficient TÂ cells. We found that miR-181a deficiency delays viral clearance, thereby biasing the immune response in favor of CD4 over CD8 TÂ cells. Antigen-specific CD4 TÂ cells in mice with miR-181a-deficient TÂ cells expand more and have a broader TCR repertoire with preferential expansion of high-affinity TÂ cells than in wild-type mice. Importantly, generation of antigen-specific miR-181a-deficient CD8 effector TÂ cells is particularly impaired, resulting in lower frequencies of CD8 TÂ cells in the liver even at time points when the infection has been cleared. Consistent with the mouse model, CD4 memory TÂ cells in individuals infected with West Nile virus at older ages tend to be more frequent and of higher affinity.
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