首页|TCR-induced FOXP3 expression by CD8+ T cells impairs their anti-tumor activity

TCR-induced FOXP3 expression by CD8+ T cells impairs their anti-tumor activity

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? 2021Adoptive cell transfer therapy using CD8+ T lymphocytes showed promising results eradicating metastatic malignancies. However, several regulatory mechanisms limit its efficacy. We studied the role of the expression of the transcription factor FOXP3 on CD8+ T cell function and anti-tumor immunity. Here we show that suboptimal T cell receptor stimulation of CD8+ T cells upregulates FOXP3 in vitro. Similarly, CD8 T cells transferred into tumor-bearing mice upregulate FOXP3 in vivo. Cell-intrinsic loss of FOXP3 by CD8+ T cells resulted in improved functionality after TCR stimulation and better antitumor responses in vivo. Inhibition of the FOXP3/NFAT interaction likewise improved CD8+ T cell functionality. Transcriptomic analysis of cells after TCR stimulation revealed an enrichment of genes implicated in the response to IFN-γ, IFN-α, inflammatory response, IL-6/JAK/STAT, G2M checkpoint and IL-2/STAT signaling in FOXP3-deficient CD8+ T cells with respect to FOXP3-wt CD8+ T cells. Our results suggest that transient expression of FOXP3 by CD8+ T cells in the tumor microenvironment restrains their anti-tumor activity, with clear implications for improving T cell responses during immunotherapy.

Adoptive cell therapyCD8+ T cellsFOXP3NFAT

Lozano T.、Conde E.、Martin-Otal C.、Navarro F.、Lasarte-Cia A.、Nasrallah R.、Alignani D.、Gorraiz M.、Sarobe P.、Romero J.P.、Vilas A.、Roychoudhuri R.、Hervas-Stubbs S.、Casares N.、Lasarte J.J.

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Immunology and Immunotherapy Center for Applied Medical Research (CIMA) University of Navarra

Laboratory of Lymphocyte Signalling and Development Babraham Institute

Flow Cytometry Core Center for Applied Medical Research (CIMA) University of Navarra

Oncohematology Programs Center for Applied Medical Research (CIMA) University of Navarra

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2022

Cancer letters

Cancer letters

SCI
ISSN:0304-3835
年,卷(期):2022.528
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