Transcriptomic analysis of human IL‐7 receptor alpha( low) and( high) effector memory CD8(+) T cells reveals an age‐associated signature linked to influenza vaccine response in older adults

Here, we investigated the relationship of the age‐associated expansion of IL‐7 receptor alpha low (IL‐7Rα(low)) effector memory (EM) CD8(+) T cells with the global transcriptomic profile of peripheral blood cells in humans. We found 231 aging signature genes of IL‐7Rα(low) EM CD8(+ )T cells that corresponded to 15% of the age‐associated genes (231/1,497) reported by a meta‐analysis study on human peripheral whole blood from approximately 15,000 individuals, having high correlation with chronological age. These aging signature genes were the target genes of several transcription factors including MYC, SATB1, and BATF, which also belonged to the 231 genes, supporting the upstream regulatory role of these transcription factors in altering the gene expression profile of peripheral blood cells with aging. We validated the differential expression of these transcription factors between IL‐7Rα(low) and (high) EM CD8(+) T cells as well as in peripheral blood mononuclear cells (PBMCs) of young and older adults. Finally, we found a significant association with influenza vaccine responses in older adults, suggesting the possible biological significance of the aging signature genes of IL‐7Rα(low) EM CD8(+ )T cells. The results of our study support the relationship of the expansion of IL‐7Rα(low) EM CD8(+) T cells with the age‐associated changes in the gene expression profile of peripheral blood cells and its possible biological implications.