Local γδ T cells: translating promise to practice in cancer immunotherapy
- PMID: 37311978
- PMCID: PMC10403623
- DOI: 10.1038/s41416-023-02303-0
Local γδ T cells: translating promise to practice in cancer immunotherapy
Abstract
Rapid bench-to-bedside translation of basic immunology to cancer immunotherapy has revolutionised the clinical practice of oncology over the last decade. Immune checkpoint inhibitors targeting αβ T cells now offer durable remissions and even cures for some patients with hitherto treatment-refractory metastatic cancers. Unfortunately, these treatments only benefit a minority of patients and efforts to improve efficacy through combination therapies utilising αβ T cells have seen diminishing returns. Alongside αβ T cells and B cells, γδ T cells are a third lineage of adaptive lymphocytes. Less is known about these cells, and they remain relatively untested in cancer immunotherapy. Whilst preclinical evidence supports their utility, the few early-phase trials involving γδ T cells have failed to demonstrate convincing efficacy in solid cancers. Here we review recent progress in our understanding of how these cells are regulated, especially locally within tissues, and the potential for translation. In particular, we focus on the latest advances in the field of butyrophilin (BTN) and BTN-like (BTNL) regulation of γδ T cells and speculate on how these advances may address the limitations of historical approaches in utilising these cells, as well as how they may inform novel approaches in deploying these cells for cancer immunotherapy.
© 2023. The Author(s).
Conflict of interest statement
IZ is employed on a sponsored research agreement with Takeda Pharmaceutical Company. IZ has provisional patent applications on targeting the BTNL3/8 axis in the human gut. YW consults for PersonGen Biotherapeutics. The authors declare no other competing interests.
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