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

Abstract

Adoptive 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.

Keywords: Adoptive cell therapy; CD8(+) T cells; FOXP3; NFAT.