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重新改造 T 细胞用于癌症治疗:从小鼠模型到临床试验。

Re-adapting T cells for cancer therapy: from mouse models to clinical trials.

机构信息

Clinical Research Division, Program in Immunology, Fred Hutchinson Cancer Research Center, Seattle, WA, USA; Department of Immunology, University of Washington, Seattle, WA, USA.

出版信息

Immunol Rev. 2014 Jan;257(1):145-64. doi: 10.1111/imr.12141.

Abstract

Adoptive T-cell therapy involves the isolation, expansion, and reinfusion of T lymphocytes with a defined specificity and function as a means to eradicate cancer. Our research has focused on specifying the requirements for tumor eradication with antigen-specific T cells and T cells transduced to express a defined T-cell receptor (TCR) in mouse models and then translating these strategies to clinical trials. Our design of T-cell-based therapy for cancer has reflected efforts to identify the obstacles that limit sustained effector T-cell activity in mice and humans, design approaches to enhance T-cell persistence, develop methods to increase TCR affinity/T-cell functional avidity, and pursue strategies to overcome tolerance and immunosuppression. With the advent of genetic engineering, a highly functional population of T cells can now be rapidly generated and tailored for the targeted malignancy. Preclinical studies in faithful and informative mouse models, in concert with knowledge gained from analyses of successes and limitations in clinical trials, are shaping how we continue to develop, refine, and broaden the applicability of this approach for cancer therapy.

摘要

过继性 T 细胞疗法涉及分离、扩增和再输注具有特定特异性和功能的 T 淋巴细胞,作为消除癌症的一种手段。我们的研究集中于确定用抗原特异性 T 细胞和转导表达特定 T 细胞受体 (TCR) 的 T 细胞消除肿瘤的要求,然后将这些策略转化为临床试验。我们设计的基于 T 细胞的癌症治疗方法反映了努力识别限制小鼠和人类中持续效应 T 细胞活性的障碍,设计增强 T 细胞持久性的方法,开发提高 TCR 亲和力/T 细胞功能亲和力的方法,并寻求克服耐受和免疫抑制的策略。随着基因工程的出现,现在可以快速产生并针对靶向恶性肿瘤进行定制的高功能 T 细胞群体。在忠实且信息丰富的小鼠模型中的临床前研究,与从临床试验的成功和局限性分析中获得的知识相结合,正在塑造我们如何继续开发、改进和扩大这种方法在癌症治疗中的应用。

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