首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Low-Intensity Focused Ultrasound Induces Reversal of Tumor-Induced T Cell Tolerance and Prevents Immune Escape
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Low-Intensity Focused Ultrasound Induces Reversal of Tumor-Induced T Cell Tolerance and Prevents Immune Escape

机译:低强度聚焦超声诱导肿瘤诱导的T细胞耐受性逆转,防止免疫逸出

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摘要

Immune responses against cancer cells are often hindered by immunosuppressive mechanisms that are developed in the tumor microenvironment. Induction of a hyporesponsive state in tumor Ag-specific T cells is one of the major events responsible for the inability of the adaptive immune system to mount an efficient antitumor response and frequently contributes to lessen the efficacy of immunotherapeutic approaches. Treatment of localized tumors by focused ultrasound (FUS) is a minimally invasive therapy that uses a range of input energy for in situ tumor ablation through the generation of thermal and cavitation effect. Using a murine B16 melanoma tumor model, we show that a variant of FUS that delivers a reduced level of energy at the focal point and generates mild mechanical and thermal stress in target cells has the ability to increase immunogenic presentation of tumor Ags, which results in reversal of tumor-induced T cell tolerance. Furthermore, we show that the combination of nonablative low-energy FUS with an ablative hypofractionated radiation therapy results in synergistic control of primary tumors and leads to a dramatic reduction in spontaneous pulmonary metastases while prolonging recurrence-free survival only in immunocompetent mice.
机译:对癌细胞的免疫反应通常通过肿瘤微环境中显影的免疫抑制机制阻碍。诱导肿瘤专用T细胞中的低响应状态是负责用于安装有效抗肿瘤反应的适应性免疫系统的主要事件之一,并且经常有助于减少免疫治疗方法的疗效。通过聚焦超声(FU)处理局部肿瘤是一种微创侵袭治疗,其通过产生热和空化效果来使用一系列输入能量的输入能量。使用鼠B16黑色素瘤肿瘤模型,我们表明,在焦点处提供减少的能量水平并在靶细胞中产生温和机械和热应力的变体具有增加肿瘤AGS的免疫原性呈递,这导致肿瘤诱导的T细胞耐受性的逆转。此外,我们表明,具有烧蚀的低能量的放射疗法的非布解低能量FU的组合导致原发性肿瘤的协同控制,并导致自发性肺转移的显着降低,同时仅在免疫活性小鼠中延长无复发存活。

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