Diamant Gil, Simchony Goldman Hadar, Gasri Plotnitsky Lital, Roitman Marina, Shiloach Tamar, Globerson-Levin Anat, Eshhar Zelig, Haim Oz, Pencovich Niv, Grossman Rachel, Ram Zvi, Volovitz Ilan
The Cancer Immunotherapy Laboratory, Neurosurgery Department, Tel-Aviv Medical Center, Sackler Faculty of Medicine, Tel-Aviv University Tel-Aviv, Israel.
Neurosurgery Department, Tel-Aviv Medical Center, Sackler Faculty of Medicine, Tel-Aviv University, Tel-Aviv, Israel; and.
J Immunol. 2021 Jul 15;207(2):709-719. doi: 10.4049/jimmunol.2100100. Epub 2021 Jul 2.
Tumor-treating fields (TTFields) are a localized, antitumoral therapy using alternating electric fields, which impair cell proliferation. Combining TTFields with tumor immunotherapy constitutes a rational approach; however, it is currently unknown whether TTFields' locoregional effects are compatible with T cell functionality. Healthy donor PBMCs and viably dissociated human glioblastoma samples were cultured under either standard or TTFields conditions. Select pivotal T cell functions were measured by multiparametric flow cytometry. Cytotoxicity was evaluated using a chimeric Ag receptor (CAR)-T-based assay. Glioblastoma patient samples were acquired before and after standard chemoradiation or standard chemoradiation + TTFields treatment and examined by immunohistochemistry and by RNA sequencing. TTFields reduced the viability of proliferating T cells, but had little or no effect on the viability of nonproliferating T cells. The functionality of T cells cultured under TTFields was retained: they exhibited similar IFN-γ secretion, cytotoxic degranulation, and PD1 upregulation as controls with similar polyfunctional patterns. Glioblastoma Ag-specific T cells exhibited unaltered viability and functionality under TTFields. CAR-T cells cultured under TTFields exhibited similar cytotoxicity as controls toward their CAR target. Transcriptomic analysis of patients' glioblastoma samples revealed a significant shift in the TTFields-treated versus the standard-treated samples, from a protumoral to an antitumoral immune signature. Immunohistochemistry of samples before and after TTFields treatment showed no reduction in T cell infiltration. T cells were found to retain key antitumoral functions under TTFields settings. Our data provide a mechanistic insight and a rationale for ongoing and future clinical trials that combine TTFields with immunotherapy.
肿瘤治疗电场(TTFields)是一种利用交变电场的局部抗肿瘤疗法,可抑制细胞增殖。将TTFields与肿瘤免疫疗法相结合是一种合理的方法;然而,目前尚不清楚TTFields的局部区域效应是否与T细胞功能兼容。将健康供体的外周血单核细胞(PBMC)和可存活解离的人胶质母细胞瘤样本在标准条件或TTFields条件下培养。通过多参数流式细胞术测量选定的关键T细胞功能。使用基于嵌合抗原受体(CAR)-T的检测方法评估细胞毒性。在标准放化疗或标准放化疗+TTFields治疗前后采集胶质母细胞瘤患者样本,并通过免疫组织化学和RNA测序进行检查。TTFields降低了增殖T细胞的活力,但对非增殖T细胞的活力几乎没有影响或没有影响。在TTFields条件下培养的T细胞功能得以保留:它们表现出与对照组相似的干扰素-γ分泌、细胞毒性脱颗粒和PD1上调,且具有相似的多功能模式。胶质母细胞瘤抗原特异性T细胞在TTFields条件下的活力和功能未改变。在TTFields条件下培养的CAR-T细胞对其CAR靶点表现出与对照组相似的细胞毒性。对患者胶质母细胞瘤样本的转录组分析显示,与标准治疗样本相比,TTFields治疗样本从促肿瘤免疫特征向抗肿瘤免疫特征发生了显著转变。TTFields治疗前后样本的免疫组织化学显示T细胞浸润没有减少。发现T细胞在TTFields环境下保留了关键的抗肿瘤功能。我们的数据为正在进行的和未来将TTFields与免疫疗法相结合的临床试验提供了机制性见解和理论依据。
