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KLRG1+ Memory CD8 T Cells Combine Properties of Short-Lived Effectors and Long-Lived Memory

Kristin R. Renkema, Matthew A. Huggins, Henrique Borges da Silva, Todd P. Knutson, Christine Henzler, Sara E. Hamilton

2020The Journal of Immunology100 citationsDOIOpen Access PDF

Abstract

Abstract CD8 effector T cells with a CD127hi KLRG1− phenotype are considered precursors to the long-lived memory pool, whereas KLRG1+CD127low cells are viewed as short-lived effectors. Nevertheless, we and others have shown that a KLRG1+CD127low population persists into the memory phase and that these T cells (termed long-lived effector cells [LLEC]) display robust protective function during acute rechallenge with bacteria or viruses. Whether these T cells represent a true memory population or are instead a remnant effector cell population that failed to undergo initial contraction has remained unclear. In this study, we show that LLEC from mice express a distinct phenotypic and transcriptional signature that shares characteristics of both early effectors and long-lived memory cells. We also find that in contrast to KLRG1+ effector cells, LLEC undergo homeostatic proliferation and are not critically dependent on IL-15 for their maintenance. Furthermore, we find that LLEC are predominantly derived from KLRG1+ effector cells when isolated at day 12 of the response. Our work challenges the concept that the KLRG1+CD127low population is dominated by short-lived cells and shows that KLRG1 downregulation is not a prerequisite to become a long-lived protective memory T cell.

Topics & Concepts

EffectorPopulationCell biologyPhenotypeMemory T cellCytotoxic T cellBiologyCD8CellImmunologyIn vitroImmune systemMedicineGeneticsGeneEnvironmental healthT-cell and B-cell ImmunologyImmune Cell Function and InteractionImmunotherapy and Immune Responses