Gene expression characteristics of CD28null memory phenotype CD8+ T cells and its implication in T‐cell aging

Abstract

Summary: Accumulation of CD28^nullCD8⁺ T cells is considered as one of the hallmarks of aging in the human immune system. However, the precise changes of CD28^nullCD8⁺ T cells, compared to those of the precursor CD28⁺CD8⁺ memory T cells, have not been determined. In this study, we present an analysis of the global gene expression profiles of CD28⁺ and CD28^null memory phenotype CD8⁺ T cells. These two CD8⁺ T subsets exhibited an overall similar gene expression profile with only a few dozen genes that were differentially expressed. A wide range of functions, including co-stimulation, effector activity, signaling, and transcription, were possessed by these differentially expressed genes, reflecting significant functional changes of CD28^null memory phenotype CD8⁺ T cells from their CD28⁺ counterparts. In addition, CD28^null memory CD8⁺ T cells expressed several natural killer cell receptors and high levels of granzymes, perforin, and FasL, indicating an increasing capacity for cytotoxicity during memory CD8⁺ T-cell aging. Interestingly, in vitro culture of these two subsets with interleukin-15 showed that similar gene expression changes occurred in both subsets. Our analysis provides the gene expression portraits of CD28^null memory phenotype CD8⁺ T cells and alteration from their CD28⁺ counterparts and suggests potential mechanisms of T-cell aging.