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TIL 2.0: More effective and predictive T-cell products by enrichment for defined antigen specificities

机译:直到2.0:更有效的和预测t细胞产品定义抗原的浓缩特异性

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摘要

Adoptive transfer of in vitro-expanded T cells derived from tumor-infiltrating lymphocytes (TILs) in melanoma patients started the era of tumor immunotherapy three decades ago. The approach has demonstrated remarkable clinical responses in several studies since. Reinfusion of TIL-derived T cells represents a highly personalized form of immunotherapy, taking into account the enormous interindividual tumor heterogeneity. However, despite its successes, TIL therapy does not lead to objective clinical responses in all cases. It is thus crucial to find out which tumor antigens are particularly valuable targets and to develop strategies to enhance the reactivity of T-cell products toward them. In this issue of the European Journal of Immunology, Kelderman et al. [Eur. J. Immunol. 2016. 46: 1351-1360] present a platform for the generation of antigen-specific TIL therapy. Combining recently developed technologies for clinical identification and enrichment of antigen-specific CD8(+) T cells, such as MHC Streptamers and UV-mediated peptide exchange, the authors could enrich T-cell populations with defined antigen specificities from melanoma-derived TILs. This T-cell product showed higher reactivity against autologous tumor cell lines than bulk TIL-derived T cells. The novel platform might enable the generation of more effective and predictable TIL-derived T-cell products for future clinical applications.
机译:在vitro-expanded T细胞过继转移来自肿瘤浸润淋巴细胞(尖)黑色素瘤患者开始的时代肿瘤免疫治疗30年前。展示了非凡的临床方法在几项研究的反应。TIL-derived T细胞代表一个高度个性化的免疫治疗,账户的巨大个人间肿瘤非均质性。直到治疗不会导致客观临床在所有情况下的反应。发现特别的肿瘤抗原有价值的目标和发展战略对提高t细胞的反应性产品他们。免疫学、Kelderman et al .(欧元。2016. 代的抗原直到疗法。结合最近开发的技术临床识别和浓缩抗原CD8 (+) T细胞,如MHCStreptamers UV-mediated肽交流,作者可以丰富t细胞的数量定义的抗原特异性的melanoma-derived尖。更高的反应性对自体肿瘤细胞行比散装TIL-derived T细胞。平台可能使一代的更多有效的和可预测的TIL-derived t细胞产品未来的临床应用。

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