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新型 γ 链细胞因子作为癌症免疫治疗中免疫调节剂的候选物。

Novel gamma-chain cytokines as candidate immune modulators in immune therapies for cancer.

机构信息

Dunn School of Pathology, University of Oxford and The Pediatric Oncology Branch, National Cancer Institute, National Institutes of Health, Bethesda, MD, USA.

出版信息

Cancer J. 2010 Jul-Aug;16(4):392-8. doi: 10.1097/PPO.0b013e3181eacbc4.

Abstract

Cytokines that signal through the common-gamma chain are potent growth factors for T cells and natural killer cells. Interleukin (IL)-2, the gammac prototype, can mediate antitumor effects as a single agent or in the context of multimodality regimens but is limited by side effects and a propensity for expansion of regulatory T cells. IL-7, IL-15, and IL-21 each possess properties that can be exploited in the context of immunotherapy for cancer. Each has been demonstrated to mediate potent vaccine adjuvant effects in tumor models, and each can enhance the effectiveness of adoptive immunotherapies. Although the overlap among the agents is significant, IL-7 is uniquely immunorestorative and preferentially augments reactivity of naive populations, IL-15 potently augments reactivity of CD8 memory cells and natural killer cells, and IL-21 preferentially expands the inflammatory Th17 subset and may limit terminal differentiation of effector CD8 cells. Clinical trials of IL-7 and IL-21 have already been completed and, so far, demonstrate safety and biologic activity of these agents. Clinical trials of IL-15 are expected soon. Ultimately, these agents are expected to be most effective in the context of multimodal immunotherapy regimens, and careful clinical trial design will be needed to efficiently identify the proper doses, regimens, and settings in which to exploit their biologic properties for therapeutic gain.

摘要

通过共同γ链传递信号的细胞因子是 T 细胞和自然杀伤细胞的有效生长因子。白细胞介素(IL)-2,γ链原型,可以作为单一药物或在多模态方案的背景下介导抗肿瘤作用,但受到副作用和调节性 T 细胞扩张倾向的限制。IL-7、IL-15 和 IL-21 各自具有可在癌症免疫治疗背景下利用的特性。在肿瘤模型中,每种都被证明具有有效的疫苗佐剂作用,并且每种都可以增强过继免疫疗法的有效性。尽管这些药物之间存在显著的重叠,但 IL-7 具有独特的免疫恢复作用,优先增强幼稚群体的反应性,IL-15 强烈增强 CD8 记忆细胞和自然杀伤细胞的反应性,而 IL-21 优先扩增炎症性 Th17 亚群,并可能限制效应 CD8 细胞的终末分化。IL-7 和 IL-21 的临床试验已经完成,迄今为止,这些药物显示出安全性和生物学活性。IL-15 的临床试验预计很快进行。最终,这些药物在多模态免疫治疗方案的背景下预计最有效,需要仔细的临床试验设计才能有效地确定适当的剂量、方案和利用其生物学特性获得治疗效果的环境。

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