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细胞因子作为癌症疫苗和细胞疗法的佐剂

Cytokines as Adjuvants for Vaccine and Cellular Therapies for Cancer.

作者信息

Capitini Christian M, Fry Terry J, Mackall Crystal L

机构信息

Immunology Section, Pediatric Oncology Branch, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892.

出版信息

Am J Immunol. 2009 Jan 1;5(3):65-83. doi: 10.3844/ajisp.2009.65.83.

Abstract

PROBLEM STATEMENT

The development of a potent vaccine that can help treat tumors resistant to conventional cytotoxic therapies remains elusive. While part of the problem may be that trials have focused on patients with bulky residual disease, the desire to maximize responses to the vaccine remains. APPROACH: The gamma(c) family of cytokines offer a unique opportunity to support the expansion and effector potential of vaccine-responding T-cells, as well as stimulate other effectors, such as natural killer (NK) cells, to become activated. RESULTS: Combining vaccines with cytokines seems logical but can bring unwanted toxicity, as has been observed with interleukin (IL)-2. In addition, the nonspecific activation or expansion of unwanted cell subsets, such as regulatory T-cells, can contribute to global immunosuppression and limit vaccine responses. The development of IL-7 and IL-21 for the clinic offers the promise of enhancing anti-tumor responses but with far less systemic toxicity and no expansion of regulatory T cells. Preclinical studies demonstrate that IL-15 could also improve T-cell, and especially NK-cell, responses as well. CONCLUSIONS/RECOMMENDATIONS: Future work should expand the use of vaccines with IL-7, IL-21 and hopefully IL-15 in high-risk patients, and consider treatment while in a state of minimal residual disease to maximize benefit. Identifying tumors that can signal through gamma(c) cytokines will also be essential so that induction of relapse will be avoided.

摘要

问题陈述

开发一种有效的疫苗来帮助治疗对传统细胞毒性疗法耐药的肿瘤仍然难以实现。虽然部分问题可能在于试验主要集中在有大量残留病灶的患者身上,但人们仍希望最大限度地提高对疫苗的反应。方法:γ(c)细胞因子家族提供了一个独特的机会,可支持对疫苗有反应的T细胞的扩增和效应潜力,并刺激其他效应细胞,如自然杀伤(NK)细胞被激活。结果:将疫苗与细胞因子联合使用似乎合乎逻辑,但可能会带来不必要的毒性,如白细胞介素(IL)-2所观察到的那样。此外,不需要的细胞亚群(如调节性T细胞)的非特异性激活或扩增会导致全身免疫抑制并限制疫苗反应。用于临床的IL-7和IL-21的开发有望增强抗肿瘤反应,但全身毒性要小得多,且不会使调节性T细胞扩增。临床前研究表明,IL-15也能改善T细胞,尤其是NK细胞的反应。结论/建议:未来的工作应扩大在高危患者中使用含有IL-7、IL-21以及有望使用IL-15的疫苗,并考虑在残留病灶最少的状态下进行治疗以最大化获益。识别能够通过γ(c)细胞因子发出信号的肿瘤也至关重要,这样可以避免复发的诱导。

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