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αPD-1相对于局部肿瘤照射的顺序决定了远隔效应抗肿瘤免疫反应的诱导。

Sequence of αPD-1 relative to local tumor irradiation determines the induction of abscopal antitumor immune responses.

作者信息

Wei Joyce, Montalvo-Ortiz Welby, Yu Lola, Krasco Amanda, Ebstein Sarah, Cortez Czrina, Lowy Israel, Murphy Andrew J, Sleeman Matthew A, Skokos Dimitris

机构信息

Regeneron Pharmaceuticals, 777 Old Saw Mill River Road, Tarrytown, NY 10591, USA.

出版信息

Sci Immunol. 2021 Apr 9;6(58). doi: 10.1126/sciimmunol.abg0117.

Abstract

Although radiotherapy has been used for over a century to locally control tumor growth, alone it rarely induces an abscopal response or systemic antitumor immunity capable of inhibiting distal tumors outside of the irradiation field. Results from recent studies suggest that combining immune checkpoint blockades to radiotherapy may enhance abscopal activity. However, the treatment conditions and underlying immune mechanisms that consistently drive an abscopal response during radiation therapy combinations remain unknown. Here, we analyzed the antitumor responses at primary and distal tumor sites, demonstrating that the timing of αPD-1 antibody administration relative to radiotherapy determined the potency of the induced abscopal response. Blockade of the PD-1 pathway after local tumor irradiation resulted in the expansion of polyfunctional intratumoral CD8 T cells, a decrease in intratumoral dysfunctional CD8 T cells, expansion of reprogrammable CD8 T cells, and induction of potent abscopal responses. However, administration of αPD-1 before irradiation almost completely abrogated systemic immunity, which associated with increased radiosensitivity and death of CD8 T cells. The subsequent reduction of polyfunctional effector CD8 T cells at the irradiated tumor site generated a suboptimal systemic antitumor response and the loss of abscopal responses. Therefore, this report maximizes the potential synergy between radiotherapy and αPD-1 immunotherapy, information that will benefit clinical combinations of radiotherapy and immune checkpoint blockade.

摘要

尽管放射疗法已被用于局部控制肿瘤生长超过一个世纪,但单独使用时,它很少能引发远隔效应或产生能够抑制照射野之外远处肿瘤的全身抗肿瘤免疫。近期研究结果表明,将免疫检查点阻断疗法与放射疗法相结合可能会增强远隔效应。然而,在放射治疗联合过程中持续驱动远隔效应的治疗条件和潜在免疫机制仍然未知。在此,我们分析了原发肿瘤部位和远处肿瘤部位的抗肿瘤反应,证明相对于放射疗法,αPD-1抗体给药的时间决定了诱导远隔效应的效力。局部肿瘤照射后阻断PD-1通路导致多功能肿瘤内CD8 T细胞扩增、肿瘤内功能失调的CD8 T细胞减少、可重编程CD8 T细胞扩增,并诱导出有效的远隔效应。然而,照射前给予αPD-1几乎完全消除了全身免疫,这与CD8 T细胞的放射敏感性增加和死亡有关。随后,照射肿瘤部位多功能效应CD8 T细胞减少,产生了次优的全身抗肿瘤反应并丧失了远隔效应。因此,本报告最大化了放射疗法和αPD-1免疫疗法之间的潜在协同作用,这些信息将有益于放射疗法和免疫检查点阻断的临床联合应用。

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