What question did this study set out to answer?

The article aims to review strategies for engaging γδ T cells for cancer treatment and their biological properties.

March 1, 2026

γδ T Cells for Cancer Immunotherapy: Unconventional Players Take the Spotlight

Key Points

The article aims to review strategies for engaging γδ T cells for cancer treatment and their biological properties.
Review of existing literature on γδ T cells
Discussion of endogenous and exogenous engagement methods
Analysis of γδ T cell activation and exhaustion
Exploration of immune checkpoint blockade benefits
Description of Vδ1 and Vδ2 T cell subsets
γδ T cells have strong cytotoxic potential and produce antitumor cytokines.
They function independently of MHC-mediated neoantigen presentation.
Strategies exist to enhance γδ T cell efficacy for immunotherapy.
Genetic engineering can boost their performance as next-generation therapies.

Abstract

The success of cancer immunotherapy depends on the mobilization of leukocytes with the capacity to eliminate tumor cells. γδ T cells represent a lymphocyte lineage with strong cytotoxic potential and abundant production of antitumor cytokines. Importantly, they are not restricted to MHC-mediated presentation of neoantigens and thus are highly suited to tackle major challenges in current immunotherapies. In this article, we review the main approaches to engage and expand γδ T cells endogenously (in patients) or exogenously (for adoptive cell therapy) against cancer. We discuss the dichotomy between activation and exhaustion of γδ T cells and how they may benefit from immune checkpoint blockade. Finally, we describe the biological properties of the two main subsets of human γδ T cells, Vδ1 and Vδ2 T cells, and how they are boosted, through genetic engineering, toward maximization of their performance as next-generation cancer immunotherapies.

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γδ T Cells for Cancer Immunotherapy: Unconventional Players Take the Spotlight

Key Points

Abstract

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