Werner Siemens Imaging Center, Department of Preclinical Imaging and Radiopharmacy, Eberhard Karls University Tuebingen, Germany.
Department of Medical Oncology and Pneumology, Internal Medicine VIII, Eberhard Karls University Tuebingen, Germany.
Theranostics. 2021 Jun 16;11(16):7700-7714. doi: 10.7150/thno.61459. eCollection 2021.
CD4 T helper cells are capable of mediating long-term antitumoral immune responses. We developed a combined immunotherapy (COMBO) using tumor antigen-specific T helper 1 cells (Tag-Th1), dual PD-L1/LAG-3 immune checkpoint blockade, and a low-dose total body irradiation (TBI) of 2 Gy, that was highly efficient in controlling the tumor burden of non-immunogenic RIP1-Tag2 mice with late-stage endogenous pancreatic islet carcinomas. In this study, we aimed to explore the impact of 2 Gy TBI on the treatment efficacy and the underlying mechanisms to boost CD4 T cell-based immunotherapies. Heavily progressed RIP1-Tag2 mice underwent COMBO treatment and their survival was compared to a cohort without 2 Gy TBI. Positron emission tomography/computed tomography (PET/CT) with radiolabeled anti-CD3 monoclonal antibodies and flow cytometry were applied to investigate 2 Gy TBI-induced alterations in the biodistribution of endogenous T cells of healthy C3H mice. Migration and homing properties of Cy5-labeled adoptive Tag-Th1 cells were monitored by optical imaging and flow cytometric analyses in C3H and tumor-bearing RIP1-Tag2 mice. Splenectomy or sham-surgery of late-stage RIP1-Tag2 mice was performed before onset of COMBO treatment to elucidate the impact of the spleen on the therapy response. First, we determined a significant longer survival of RIP1-Tag2 mice and an increased CD4 T cell tumor infiltrate when 2 Gy TBI was applied in addition to Tag-Th1 cell PD-L1/LAG-3 treatment. In non-tumor-bearing C3H mice, TBI induced a moderate host lymphodepletion and a tumor antigen-independent accumulation of Tag-Th1 cells in lymphoid and non-lymphoid organs. In RIP1-Tag2, we found increased numbers of effector memory-like Tag-Th1 and endogenous CD4 T cells in the pancreatic tumor tissue after TBI, accompanied by a tumor-specific Th1-driven immune response. Furthermore, the spleen negatively regulated T cell effector function by upregulation PD-1/LAG-3/TIM-3 immune checkpoints, providing a further rationale for this combined treatment approach. Low-dose TBI represents a powerful tool to foster CD4 T cell-based cancer immunotherapies by favoring Th1-driven antitumoral immunity. As TBI is a clinically approved and well-established technique it might be an ideal addition for adoptive cell therapy with CD4 T cells in the clinical setting.
CD4 T 辅助细胞能够介导长期抗肿瘤免疫反应。我们开发了一种联合免疫疗法(COMBO),使用肿瘤抗原特异性 T 辅助 1 细胞(Tag-Th1)、双重 PD-L1/LAG-3 免疫检查点阻断和 2 Gy 的低剂量全身照射(TBI),该疗法在控制晚期内源性胰岛癌的非免疫原性 RIP1-Tag2 小鼠的肿瘤负担方面非常有效。在这项研究中,我们旨在探讨 2 Gy TBI 对治疗效果的影响及其增强基于 CD4 T 细胞的免疫疗法的潜在机制。患有严重进展的 RIP1-Tag2 小鼠接受了 COMBO 治疗,并将其存活情况与未接受 2 Gy TBI 的队列进行了比较。正电子发射断层扫描/计算机断层扫描(PET/CT)结合放射性标记的抗 CD3 单克隆抗体和流式细胞术用于研究健康 C3H 小鼠中内源性 T 细胞的 2 Gy TBI 诱导的生物分布变化。通过光学成像和流式细胞术分析,监测 Cy5 标记的过继性 Tag-Th1 细胞在 C3H 和荷瘤 RIP1-Tag2 小鼠中的迁移和归巢特性。在开始 COMBO 治疗之前,对晚期 RIP1-Tag2 小鼠进行脾切除术或假手术,以阐明脾脏对治疗反应的影响。首先,我们确定了在添加 Tag-Th1 细胞 PD-L1/LAG-3 治疗的基础上应用 2 Gy TBI 时,RIP1-Tag2 小鼠的存活时间显著延长,并且 CD4 T 细胞肿瘤浸润增加。在非肿瘤荷瘤 C3H 小鼠中,TBI 诱导中度宿主淋巴耗竭,并在淋巴和非淋巴器官中肿瘤抗原非依赖性地积累 Tag-Th1 细胞。在 RIP1-Tag2 中,我们发现 TBI 后胰腺肿瘤组织中效应记忆样 Tag-Th1 和内源性 CD4 T 细胞数量增加,伴有肿瘤特异性 Th1 驱动的免疫反应。此外,脾脏通过上调 PD-1/LAG-3/TIM-3 免疫检查点来负调节 T 细胞效应功能,为这种联合治疗方法提供了进一步的依据。低剂量 TBI 通过促进 Th1 驱动的抗肿瘤免疫来代表增强基于 CD4 T 细胞的癌症免疫疗法的有力工具。由于 TBI 是一种临床批准且成熟的技术,因此它可能是在临床环境中使用 CD4 T 细胞进行过继细胞治疗的理想补充。
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