eLife (Mar 2020)

SLAMF6​ deficiency augments tumor killing and skews toward an effector phenotype revealing it as a novel T cell checkpoint

  • Emma Hajaj,
  • Galit Eisenberg,
  • Shiri Klein,
  • Shoshana Frankenburg,
  • Sharon Merims,
  • Inna Ben David,
  • Thomas Eisenhaure,
  • Sarah E Henrickson,
  • Alexandra Chloé Villani,
  • Nir Hacohen,
  • Nathalie Abudi,
  • Rinat Abramovich,
  • Jonathan E Cohen,
  • Tamar Peretz,
  • Andre Veillette,
  • Michal Lotem

DOI
https://doi.org/10.7554/eLife.52539
Journal volume & issue
Vol. 9

Abstract

Read online

SLAMF6 is a homotypic receptor of the Ig-superfamily whose exact role in immune modulation has remained elusive. Its constitutive expression on resting and activated T cells precludes it from being a bona fide exhaustion marker. By breeding Pmel-1 mice with SLAMF6 -/- mice, we generated donors for T cells lacking SLAMF6 and expressing a transgenic TCR for gp100-melanoma antigen. Activated Pmel-1xSLAMF6 -/- CD8+ T cells displayed improved polyfunctionality and strong tumor cytolysis. T-bet was the dominant transcription factor in Pmel-1 x SLAMF6 -/- cells, and upon activation, they acquired an effector-memory phenotype. Adoptive transfer of Pmel-1 x SLAMF6 -/- T cells to melanoma-bearing mice resulted in lasting tumor regression in contrast to temporary responses achieved with Pmel-1 T cells. LAG-3 expression was elevated in the SLAMF6 -/- cells, and the addition of the LAG-3-blocking antibody to the adoptive transfer protocol improved the SLAMF6 -/- T cells and expedited the antitumor response even further. The results from this study support the notion that SLAMF6 is an inhibitory immune receptor whose absence enables powerful CD8+ T cells to eradicate tumors.

Keywords