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试验观察:用于抗癌免疫治疗的过继性细胞转移

Trial Watch: Adoptive cell transfer for anticancer immunotherapy.

作者信息

Vacchelli Erika, Eggermont Alexander, Fridman Wolf Hervé, Galon Jérôme, Tartour Eric, Zitvogel Laurence, Kroemer Guido, Galluzzi Lorenzo

机构信息

Institut Gustave Roussy; Villejuif, France ; Université Paris-Sud/Paris XI; Le Kremlin-Bicêtre; Paris France ; INSERM, U848; Villejuif, France.

出版信息

Oncoimmunology. 2013 May 1;2(5):e24238. doi: 10.4161/onci.24238.

Abstract

Adoptive cell transfer (ACT) represents a prominent form of immunotherapy against malignant diseases. ACT is conceptually distinct from dendritic cell-based approaches (which de facto constitute cellular vaccines) and allogeneic transplantation (which can be employed for the therapy of hematopoietic tumors) as it involves the isolation of autologous lymphocytes exhibiting antitumor activity, their expansion/activation ex vivo and their reintroduction into the patient. Re-infusion is most often performed in the context of lymphodepleting regimens (to minimize immunosuppression by host cells) and combined with immunostimulatory interventions, such as the administration of Toll-like receptor agonists. Autologous cells that are suitable for ACT protocols can be isolated from tumor-infiltrating lymphocytes or generated by engineering their circulating counterparts for the expression of transgenic tumor-specific T-cell receptors. Importantly, lymphocytes can be genetically modified prior to re-infusion for increasing their persistence in vivo, boosting antitumor responses and minimizing side effects. Moreover, recent data indicate that exhausted antitumor T lymphocytes may be rejuvenated in vitro by exposing them to specific cytokine cocktails, a strategy that might considerably improve the clinical success of ACT. Following up the Trial Watch that we published on this topic in the third issue of (May 2012), here we summarize the latest developments in ACT-related research, covering both high-impact studies that have been published during the last 13 months and clinical trials that have been initiated in the same period to assess the antineoplastic profile of this form of cellular immunotherapy.

摘要

过继性细胞转移(ACT)是一种针对恶性疾病的重要免疫治疗形式。ACT在概念上不同于基于树突状细胞的方法(实际上构成细胞疫苗)和同种异体移植(可用于治疗造血系统肿瘤),因为它涉及分离具有抗肿瘤活性的自体淋巴细胞,在体外进行扩增/激活,然后重新引入患者体内。重新输注通常在淋巴细胞清除方案的背景下进行(以尽量减少宿主细胞的免疫抑制作用),并与免疫刺激干预措施相结合,如给予Toll样受体激动剂。适用于ACT方案的自体细胞可以从肿瘤浸润淋巴细胞中分离出来,或者通过对其循环对应物进行工程改造以表达转基因肿瘤特异性T细胞受体来产生。重要的是,淋巴细胞在重新输注前可以进行基因改造,以增加其在体内的持久性,增强抗肿瘤反应并最小化副作用。此外,最近的数据表明,通过将耗竭的抗肿瘤T淋巴细胞暴露于特定的细胞因子混合物中,可以在体外使其恢复活力,这一策略可能会大大提高ACT的临床成功率。继我们在2012年5月第三期发表的关于该主题的《试验观察》之后,在此我们总结ACT相关研究的最新进展,涵盖过去13个月内发表的高影响力研究以及同期启动的评估这种细胞免疫治疗抗肿瘤特性的临床试验。

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