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. Author manuscript; available in PMC: 2019 Feb 20.
Published in final edited form as: Immunity. 2018 Feb 20;48(2):214–226. doi: 10.1016/j.immuni.2018.02.010

Fig. 1. Traits that distinguish naïve and major memory T cell populations.

Fig. 1

The bars on the left indicate various characteristics, which can be used to distinguish the T cell subsets listed on the right. The first 4 bars indicate trafficking capabilities and stimulation history of the cells, providing rigid distinctions that can be used to define T cell populations – but note that there is only limited concordance between these traits. The other bars indicate gene expression or phenotypic characteristics, focused on molecules associated with trafficking, tissue retention, and “memory markers” (in mice these would include elevated expression of CD44 and CD11a and reduced expression of CD45RB, while in humans this would include elevated expression of CD45RO and CD11a and reduced expression of CD45RA). Grey shading in these bars indicates where phenotypic/gene expression characteristics fail to clearly correlate with the red and green bars on the left. At the far right are T cell subsets typically associated with these combinations of traits and phenotypic/gene expression characteristics – note that the position of these identifiers is inherently vague, since the typical criteria for defining “subsets” use markers that may not faithfully correlate with the cells’ stimulation history or migration potential. Abbreviations for T cells: Naïve, TN; Central Memory, TCM; Effector Memory, TEM; Tissue-Resident Memory, TRM; Virtual Memory (also encompassing “Innate” memory), TVM; Stem Cell Memory, TSCM; Memory T cells with Naïve Phenotype, TMNP; Peripheral Memory, TPM; Long-Lived Effector Cells, TLLEC; CD45RA+ Effector Memory (defined in humans), TEMRA; Exhausted T cells, TEX; TFH Follicular Helpers). Color coding of the T cell subsets indicates whether they have been primarily described for CD8+ T cells (maroon), CD4+ T cells (gold) or both populations (black).