Based on the expression of CD45RA and CCR7, human peripheral blood CD8+ T cell is sub-divided into naïve, central memory (TCM), effector memory (TEM) and terminally differentiated effector cells (TEMRA). The expression of IL-7 receptor and cognate downstream signaling molecules in CD8 effector cells was found to be correlated with the prognosis of autoimmune disease. Previously, we found that the frequency of IFN- γ+ granzyme B+ CD8+ T cell in peripheral blood from either oral cancer or oral lichen planus (OLP) patients was significantly higher, while the expression of IL-7 receptor α chain, CD127, in CD8+ T cells was lower than in healthy control. The specific aim of this study is to identify the CD127 expression on distinct CD8+ T cell subsets and characterize their differences in cytokine production and survival after stimulation. The distribution of peripheralCD8+ TEM or TEMRA subsets is significantly increased in cancer and autoimmune patients. Moreover, these CD8+ T cell subpopulations are also found infiltrating into OLP lesion or tumor site. RT-PCR analysis of sorted CD8+T cells from oral cancer or OLP patients indicated that TEM or TEMRA express significantly higher level of mRNAs encoding IFN-γ, granzyme B and perforin than the naïve or central memory counterparts. Interestingly, CD127+ TEM or TEMRA subsets express and produce higher level of IFN-γ and IL-2 than CD127- subsets and exhibits higher proliferating ability and resistance to apoptosis following stimulation. Together, these results suggested that TEM and TEMRA may be the predominant effector cell subsets to cause OLP lesion or anti-tumor immunity.