The Journal of Clinical Investigation (Jul 2023)

T-BET and EOMES sustain mature human NK cell identity and antitumor function

  • Pamela Wong,
  • Jennifer A. Foltz,
  • Lily Chang,
  • Carly C. Neal,
  • Tony Yao,
  • Celia C. Cubitt,
  • Jennifer Tran,
  • Samantha Kersting-Schadek,
  • Sathvik Palakurty,
  • Natalia Jaeger,
  • David A. Russler-Germain,
  • Nancy D. Marin,
  • Margery Gang,
  • Julia A. Wagner,
  • Alice Y. Zhou,
  • Miriam T. Jacobs,
  • Mark Foster,
  • Timothy Schappe,
  • Lynne Marsala,
  • Ethan McClain,
  • Patrick Pence,
  • Michelle Becker-Hapak,
  • Bryan Fisk,
  • Allegra A. Petti,
  • Obi L. Griffith,
  • Malachi Griffith,
  • Melissa M. Berrien-Elliott,
  • Todd A. Fehniger

Journal volume & issue
Vol. 133, no. 13

Abstract

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Since the T-box transcription factors (TFs) T-BET and EOMES are necessary for initiation of NK cell development, their ongoing requirement for mature NK cell homeostasis, function, and molecular programming remains unclear. To address this, T-BET and EOMES were deleted in unexpanded primary human NK cells using CRISPR/Cas9. Deleting these TFs compromised in vivo antitumor response of human NK cells. Mechanistically, T-BET and EOMES were required for normal NK cell proliferation and persistence in vivo. NK cells lacking T-BET and EOMES also exhibited defective responses to cytokine stimulation. Single-cell RNA-Seq revealed a specific T-box transcriptional program in human NK cells, which was rapidly lost following T-BET and EOMES deletion. Further, T-BET– and EOMES-deleted CD56bright NK cells acquired an innate lymphoid cell precursor–like (ILCP-like) profile with increased expression of the ILC-3–associated TFs RORC and AHR, revealing a role for T-box TFs in maintaining mature NK cell phenotypes and an unexpected role of suppressing alternative ILC lineages. Our study reveals the critical importance of sustained EOMES and T-BET expression to orchestrate mature NK cell function and identity.

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