iScience (Apr 2024)

Exogenous IL-2 delays memory precursors generation and is essential for enhancing memory cells effector functions

  • Shaoying Wang,
  • Margaux Prieux,
  • Simon de Bernard,
  • Maxence Dubois,
  • Daphne Laubreton,
  • Sophia Djebali,
  • Manon Zala,
  • Christophe Arpin,
  • Laurent Genestier,
  • Yann Leverrier,
  • Olivier Gandrillon,
  • Fabien Crauste,
  • Wenzheng Jiang,
  • Jacqueline Marvel

Journal volume & issue
Vol. 27, no. 4
p. 109411

Abstract

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Summary: To investigate the impact of paracrine IL-2 signals on memory precursor (MP) cell differentiation, we activated CD8 T cell in vitro in the presence or absence of exogenous IL-2 (ex-IL-2). We assessed memory differentiation by transferring these cells into virus-infected mice. Both conditions generated CD8 T cells that participate in the ongoing response and gave rise to similar memory cells. Nevertheless, when transferred into a naive host, T cells activated with ex-IL-2 generated a higher frequency of memory cells displaying increased functional memory traits. Single-cell RNA-seq analysis indicated that without ex-IL-2, cells rapidly acquire an MP signature, while in its presence they adopted an effector signature. This was confirmed at the protein level and in a functional assay. Overall, ex-IL-2 delays the transition into MP cells, allowing the acquisition of effector functions that become imprinted in their progeny. These findings may help to optimize the generation of therapeutic T cells.

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