首页> 美国卫生研究院文献>Cells >The Potentiation of Anti-Tumor Immunity by Tumor Abolition with Alpha Particles Protons or Carbon Ion Radiation and Its Enforcement by Combination with Immunoadjuvants or Inhibitors of Immune Suppressor Cells and Checkpoint Molecules

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The Potentiation of Anti-Tumor Immunity by Tumor Abolition with Alpha Particles Protons or Carbon Ion Radiation and Its Enforcement by Combination with Immunoadjuvants or Inhibitors of Immune Suppressor Cells and Checkpoint Molecules

机译：通过与免疫抑制细胞和检查点分子的免疫谐振剂或抑制剂的组合通过α颗粒质子或碳离子辐射的肿瘤抗血管和碳离子辐射的抗肿瘤免疫增强

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The delivery of radiation therapy (RT) for cancer with intent to cure has been optimized and standardized over the last 80 years. Both preclinical and clinical work emphasized the observation that radiation destroys the tumor and exposes its components to the immune response in a mode that facilitates the induction of anti-tumor immunity or reinforces such a response. External beam photon radiation is the most prevalent in situ abolition treatment, and its use exposed the “abscopal effect”. Particle radiotherapy (PRT), which has been in various stages of research and development for 70 years, is today available for the treatment of patients in the form of alpha particles, proton, or carbon ion radiotherapy. Charged particle radiotherapy is based on the acceleration of charged species, such as protons or carbon-12, which deposit their energy in the treated tumor and have a higher relative biological effectiveness compared with photon radiation. In this review, we will bring evidence that alpha particles, proton, or carbon ion radiation can destroy tumors and activate specific anti-tumor immune responses. Radiation may also directly affect the distribution and function of immune cells such as T cells, regulatory T cells, and mononuclear phagocytes. Tumor abolition by radiation can trigger an immune response against the tumor. However, abolition alone rarely induces effective anti-tumor immunity resulting in systemic tumor rejection. Immunotherapy can complement abolition to reinforce the anti-tumor immunity to better eradicate residual local and metastatic tumor cells. Various methods and agents such as immunoadjuvants, suppressor cell inhibitors, or checkpoint inhibitors were used to manipulate the immune response in combination with radiation. This review deals with the manifestations of particle-mediated radiotherapy and its correlation with immunotherapy of cancer.

机译：在过去的80年里，有目的地优化和标准化了治疗的癌症的放射治疗（RT）的递送。临床前和临床工作都强调了观察，即辐射破坏肿瘤并将其组分暴露于促进抗肿瘤免疫或增强这种反应的模式中的免疫应答。外梁光子辐射是最普遍的原位取消处理，其使用暴露了“横断面效应”。颗粒放射疗法（PRT）已在70年代的各种研究和开发阶段，今天可用于以α颗粒，质子或碳离子放射疗法的形式治疗患者。带电粒子放射疗法基于带电物种的加速度，例如质子或碳-12，其在处理过的肿瘤中沉积它们的能量，与光子辐射相比具有更高的相对生物效果。在本综述中，我们将提取α颗粒，质子或碳离子辐射可以破坏肿瘤并激活特异性抗肿瘤免疫应答。辐射还可以直接影响免疫细胞如T细胞，调节性T细胞和单核吞噬细胞的分布和功能。通过辐射滥用肿瘤可以引发对肿瘤的免疫应答。然而，无偿的人很少诱导有效的抗肿瘤免疫导致系统性肿瘤排斥。免疫疗法可以补充减少以增强抗肿瘤免疫，以更好地消除残留的局部和转移性肿瘤细胞。各种方法和药剂如免疫造成，抑制细胞抑制剂或检查点抑制剂用于操纵免疫应答与辐射组合。本综述涉及粒子介导的放射疗法的表现及其与癌症免疫疗法的相关性。

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期刊名称 Cells
作者
Yona Keisari; Itzhak Kelson;
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作者单位

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年(卷),期 2021(10),2
年度 2021
页码 228
总页数 13
原文格式 PDF
正文语种
中图分类细胞生物学;
关键词
alpha radiation; proton radiation; carbon ion; immunotherapy; immunoadjuvants; checkpoint inhibitors; immune suppressor cells; toll-like receptors; tumor abolition; anti-tumor immunity;

机译：alpha辐射;质子辐射;碳离子;免疫疗法;免疫侵害;检查点抑制剂;免疫抑制剂;免疫抑制细胞;造成的受体;肿瘤废除;抗肿瘤免疫;

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1. Small molecule AZD4635 inhibitor of A2AR signaling rescues immune cell function including CD103 dendritic cells enhancing anti-tumor immunity [J] . Alexandra Borodovsky, Christine M Barbon, Yanjun Wang, Journal for ImmunoTherapy of Cancer . 2020,第2期

机译：A2AR信号传导的小分子AZD4635抑制剂免疫细胞功能，包括CD103树突细胞增强抗肿瘤免疫力
2. Activation of the cytosolic RNA receptor RIG-I in tumor and immune cells triggers efficient anti-tumor immunity and synergizes with checkpoint blockade [J] . Heidegger S., Alexander W., Kreppel D., European journal of cancer: official journal for European Organization for Research and Treatment of Cancer (EORTC) [and] European Association for Cancer Research (EACR) . 2016,第Suppla1期

机译：在肿瘤和免疫细胞中激活细胞溶质RNA受体钻井液I触发有效的抗肿瘤免疫力，并通过检查点封闭来协同增长
3. Systemically Administered Sindbis Virus in Combination with Immune Checkpoint Blockade Induces Curative Anti-tumor Immunity [J] . Iris Scherwitzl, Alicia Hurtado, Carolyn M. Pierce, Molecular Therapy - Oncolytics . 2018,第1期

机译：系统管理的Sindbis病毒与免疫检查站封锁相结合可诱导治疗性抗肿瘤免疫
4. Combination of PDT and a DNA demethylating agent produces anti-tumor immune response in a mouse tumor model [C] . Pawel Mroz, Michael R Hamblin World congress of the International Photodynamic Association . 2009

机译：PDT和DNA去甲基化剂的组合在小鼠肿瘤模型中产生抗肿瘤免疫应答
5. Understanding How Adrenergic Stress Signaling Impacts the Anti-Tumor Immune Response and the Efficacy of Checkpoint Inhibitors in Murine Tumor Models [D] . Bucsek, Mark Joseph. 2019

机译：了解肾上腺素能应激信号如何影响抗肿瘤免疫应答以及检查点抑制剂在鼠肿瘤模型中的疗效
6. Targeting the TGFβ pathway with galunisertib a TGFβRI small molecule inhibitor promotes anti-tumor immunity leading to durable complete responses as monotherapy and in combination with checkpoint blockade [O] . Rikke B. Holmgaard, David A. Schaer, Yanxia Li, 2018

机译：与TGFβRI小分子抑制剂galunisertib一起靶向TGFβ途径可增强抗肿瘤免疫力从而产生持久完全的反应可作为单一疗法并与检查点阻断结合使用
7. The Potentiation of Anti-Tumor Immunity by Tumor Abolition with Alpha Particles, Protons, or Carbon Ion Radiation and Its Enforcement by Combination with Immunoadjuvants or Inhibitors of Immune Suppressor Cells and Checkpoint Molecules [O] . Yona Keisari, Itzhak Kelson 2021

机译：通过与免疫抑制细胞和检查点分子的免疫谐振剂或抑制剂的组合，通过α颗粒，质子或碳离子辐射的肿瘤抗血管和碳离子辐射的抗肿瘤免疫增强

The Potentiation of Anti-Tumor Immunity by Tumor Abolition with Alpha Particles Protons or Carbon Ion Radiation and Its Enforcement by Combination with Immunoadjuvants or Inhibitors of Immune Suppressor Cells and Checkpoint Molecules

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