Litcius/Paper detail

Regulatory T cells suppress the formation of potent KLRK1 and IL-7R expressing effector CD8 T cells by limiting IL-2

Oksana Tsyklauri, Tereza Chadimová, Veronika Niederlová, Jiřina Kovářová, Juraj Michálik, Iva Malatova, Sarka Janusova, Olha Ivashchenko, Hélène Rossez, Ales Drobek, Hana Vecerova, Virginie Galati, Marek Kovář, Ondřej Štěpánek

2023eLife35 citationsDOIOpen Access PDF

Abstract

Regulatory T cells (Tregs) are indispensable for maintaining self-tolerance by suppressing conventional T cells. On the other hand, Tregs promote tumor growth by inhibiting anti-cancer immunity. In this study, we identified that Tregs increase the quorum of self-reactive CD8 + T cells required for the induction of experimental autoimmune diabetes in mice. Their major suppression mechanism is limiting available IL-2, an essential T-cell cytokine. Specifically, Tregs inhibit the formation of a previously uncharacterized subset of antigen-stimulated KLRK1 + IL7R + (KILR) CD8 + effector T cells, which are distinct from conventional effector CD8 + T cells. KILR CD8 + T cells show a superior cell killing abilities in vivo. The administration of agonistic IL-2 immunocomplexes phenocopies the absence of Tregs, i.e., it induces KILR CD8 + T cells, promotes autoimmunity, and enhances anti-tumor responses in mice. Counterparts of KILR CD8 + T cells were found in the human blood, revealing them as a potential target for immunotherapy.

Topics & Concepts

Cytotoxic T cellBiologyCD8Cell biologyEffectorImmunologyFOXP3Interleukin-7 receptorInterleukin 21T cellIL-2 receptorAntigen-presenting cellImmune systemIn vitroBiochemistryImmune Cell Function and InteractionT-cell and B-cell ImmunologyCAR-T cell therapy research