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C-Jun overexpression in CAR T cells induces exhaustion resistance.

ABSTRACT: Chimeric antigen receptor (CAR) T cells mediate anti-tumour effects in a small subset of patients with cancer1-3, but dysfunction due to T cell exhaustion is an important barrier to progress4-6. To investigate the biology of exhaustion in human T cells expressing CAR receptors, we used a model system with a tonically signaling CAR, which induces hallmark features of exhaustion6. Exhaustion was associated with a profound defect in the production of IL-2, along with increased chromatin accessibility of AP-1 transcription factor motifs and overexpression of the bZIP and IRF transcription factors that have been implicated in mediating dysfunction in exhausted T cells7-10. Here we show that CAR T cells engineered to overexpress the canonical AP-1 factor c-Jun have enhanced expansion potential, increased functional capacity, diminished terminal differentiation and improved anti-tumour potency in five different mouse tumour models in vivo. We conclude that a functional deficiency in c-Jun mediates dysfunction in exhausted human T cells, and that engineering CAR T cells to overexpress c-Jun renders them resistant to exhaustion, thereby addressing a major barrier to progress for this emerging class of therapeutic agents.

SUBMITTER: Lynn RC 

PROVIDER: S-EPMC6944329 | biostudies-literature | 2019 Dec

REPOSITORIES: biostudies-literature

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Chimeric antigen receptor (CAR) T cells mediate anti-tumour effects in a small subset of patients with cancer<sup>1-3</sup>, but dysfunction due to T cell exhaustion is an important barrier to progress<sup>4-6</sup>. To investigate the biology of exhaustion in human T cells expressing CAR receptors, we used a model system with a tonically signaling CAR, which induces hallmark features of exhaustion<sup>6</sup>. Exhaustion was associated with a profound defect in the production of IL-2, along wit  ...[more]

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