IL-12/18/21 pre-activation enhances the anti-tumor efficacy of expanded γδT cells and overcomes resistance to anti-PD-L1 treatment

Author:

Teo Huey Yee,Song YuanORCID,Yong Kylie Su Mei,Liu Yonghao,Mei Yu,Hanafi Zuhairah Binte,Zhu Ying,Gascoigne Nicholas R. J.,Chen Qingfeng,Liu Haiyan

Abstract

AbstractγδT cells are promising candidates for cellular immunotherapy due to their immune regulation through cytokine production and MHC-independent direct cytotoxicity against a broad spectrum of tumors. However, current γδT cell-based cancer immunotherapy has limited efficacies and novel strategies are needed to improve its clinical outcomes. Here, we report that cytokine pre-treatment with IL-12/18, IL-12/15/18, IL-12/18/21 and IL-12/15/18/21 could effectively enhance the activation and cytotoxicity ofin vitroexpanded murine and human γδT cells. However, only adoptive transfer of IL-12/18/21 pre-activated γδT cells significantly inhibited tumor growth in a murine melanoma model and a hepatocellular carcinoma model. Both IL-12/18/21 pre-activated antibody-expanded and zoledronate-expanded human γδT cells effectively controlled tumor growth in a humanized mouse model. IL-12/18/21 pre-activation promoted γδT cell proliferation and cytokine productionin vivoand enhanced IFN-γ and TNF-α production, as well as granzyme B expression by endogenous CD8+T cells in a cell-cell contact dependent manner. Furthermore, the adoptive transfer of IL-12/18/21 pre-activated γδT cells could overcome the resistance to anti-PD-L1 therapy, and the combination therapy had a synergistic effect on the therapeutic outcomes. Moreover, the enhanced anti-tumor function of adoptively transferred IL-12/18/21 pre-activated γδT cells was largely diminished in the absent of endogenous CD8+T cells when administered alone or in combination with anti-PD-L1, suggesting a CD8+T cell-dependent mechanism. Taken together, IL-12/18/21 pre-activation could promote γδT cell anti-tumor function and overcome the resistance to checkpoint blockade therapy, indicating an effective combinational cancer immunotherapeutic strategy.SynopsisIL-12/18/21 pre-activation enhances the anti-tumor efficacy of adoptively transferred γδT cells by promoting its proliferation, activation, and cytotoxicity, as well as activating endogenous CD8+T cells.Adoptive transfer of IL-12/18/21 pre-activated γδT cells could overcome the resistance to anti-PD-L1 therapy, indicating an effective combinational cancer immunotherapeutic strategy.

Publisher

Cold Spring Harbor Laboratory

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