Ablation of T cell–associated PD-1H enhances functionality and promotes adoptive immunotherapy
Li Hu, Ling Chen, Zexiu Xiao, Xu Zheng, Yuangui Chen, Na Xian, Christina Cho, Liqun Luo, Gangxiong Huang, Lieping Chen
Li Hu, Ling Chen, Zexiu Xiao, Xu Zheng, Yuangui Chen, Na Xian, Christina Cho, Liqun Luo, Gangxiong Huang, Lieping Chen
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Research Article Immunology Therapeutics

Ablation of T cell–associated PD-1H enhances functionality and promotes adoptive immunotherapy

Abstract

Programmed death-1 homolog (PD-1H) is a coinhibitory molecule that negatively regulates T cell–mediated immune responses. In this study, we determined whether ablation of T cell–associated PD-1H could enhance adoptive T cell therapy in experimental tumor models. The expression of PD-1H is upregulated in activated and tumor-infiltrating CD8+ T cells. Activated CD8+ T cells from PD-1H–deficient (PD-1H–KO) mice exhibited increased cell proliferation, cytokine production, and antitumor activity in vitro. Adoptive transfer of PD-1H–KO CD8+ T cells resulted in the regression of established syngeneic mouse tumors. Similar results were obtained when PD-1H was ablated in T cells by CRISPR/Cas9-mediated gene silencing. Furthermore, ablation of PD-1H in CAR-T cells significantly improved their antitumor activity against human xenografts in vivo. Our results indicate that T cell–associated PD-1H could suppress immunity in the tumor microenvironment and that targeting PD-1H may improve T cell adoptive immunotherapy.

Authors

Li Hu, Ling Chen, Zexiu Xiao, Xu Zheng, Yuangui Chen, Na Xian, Christina Cho, Liqun Luo, Gangxiong Huang, Lieping Chen

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Figure 2

PKO cell treatment suppressed tumor growth in mouse tumor model.

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PKO cell treatment suppressed tumor growth in mouse tumor model. (A) EG7...
(A) EG7 or B16-OVA tumor–bearing mice (n = 5 per group) received an i.v. injection of OT-I cells or PBS on day 6. (B and C) Tumor growth was measured by caliper every 2 days. Data are representative of 3 independent experiments with mean ± SEM. **P < 0.01, ****P < 0.0001 (2-way ANOVA). Tumors were harvested, and CD45+ TILs were analyzed on day 17. (D and E) TILs including CD4+ and CD8+ T cells, and MDSCs (CD11b+CD11cGr-1+) were identified by flow cytometry (EG7 [D] and B16-OVA [E]). (F and G) The expression level of effector molecules (IFN-γ and granzyme B) by TILs was analyzed after 5 hours of stimulation with OVA peptide (EG7 [F] and B16-OVA [G]). Data are representative of 2 independent experiments with mean ± SEM. *P < 0.05, **P < 0.01, ***P < 0.001, and ****P < 0.0001 (1-way ANOVA).