PD-1-cis IL-2R agonism yields better effectors from stem-like CD8+ T cells

白细胞介素2受体 细胞毒性T细胞 效应器 CD8型 细胞生物学 生物 免疫学 细胞因子 癌症研究 人口 干细胞 T细胞 抗原 免疫系统 医学 遗传学 体外 环境卫生
作者
Laura Codarri Deak,Valeria Nicolini,Masao Hashimoto,Maria Karagianni,Petra Schwalie,Laura Lauener,Eleni Maria Varypataki,Marine Richard,Esther Bommer,Johannes Sam,Stefanie Joller,Mario Perro,Floriana Cremasco,Leo Kunz,Emilio Yángüez,Tamara Hüsser,Ramona Schlenker,Marisa Mariani,Vinko Toševski,Sylvia Herter
出处
期刊:Nature [Nature Portfolio]
卷期号:610 (7930): 161-172 被引量:252
标识
DOI:10.1038/s41586-022-05192-0
摘要

Expansion and differentiation of antigen-experienced PD-1+TCF-1+ stem-like CD8+ T cells into effector cells is critical for the success of immunotherapies based on PD-1 blockade1-4. Hashimoto et al. have shown that, in chronic infections, administration of the cytokine interleukin (IL)-2 triggers an alternative differentiation path of stem-like T cells towards a distinct population of 'better effector' CD8+ T cells similar to those generated in an acute infection5. IL-2 binding to the IL-2 receptor α-chain (CD25) was essential in triggering this alternative differentiation path and expanding better effectors with distinct transcriptional and epigenetic profiles. However, constitutive expression of CD25 on regulatory T cells and some endothelial cells also contributes to unwanted systemic effects from IL-2 therapy. Therefore, engineered IL-2 receptor β- and γ-chain (IL-2Rβγ)-biased agonists are currently being developed6-10. Here we show that IL-2Rβγ-biased agonists are unable to preferentially expand better effector T cells in cancer models and describe PD1-IL2v, a new immunocytokine that overcomes the need for CD25 binding by docking in cis to PD-1. Cis binding of PD1-IL2v to PD-1 and IL-2Rβγ on the same cell recovers the ability to differentiate stem-like CD8+ T cells into better effectors in the absence of CD25 binding in both chronic infection and cancer models and provides superior efficacy. By contrast, PD-1- or PD-L1-blocking antibodies alone, or their combination with clinically relevant doses of non-PD-1-targeted IL2v, cannot expand this unique subset of better effector T cells and instead lead to the accumulation of terminally differentiated, exhausted T cells. These findings provide the basis for the development of a new generation of PD-1 cis-targeted IL-2R agonists with enhanced therapeutic potential for the treatment of cancer and chronic infections.
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