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Tumor-Infiltrating Lymphocyte Therapy: Addressing Prevailing Questions

机译:肿瘤浸润淋巴细胞疗法:解决普遍存在的问题

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Autologous adoptive T-cell therapies have made tremendous strides over the last few years with excitement currently being generated by technologies that can reprogram T-cell specificities toward any desired antigen including chimeric antigen receptors and recombinant T-cell receptors. Time will tell whether these new genetically engineered T-cell technologies will be effective as advertised, especially in solid tumors, considering the limited availability of specific antigens and the difficulty in managing the unpredictable on-target, off-tissue toxicities. However, a form of T-cell therapy that has been utilized in patients more than any other and has left a lasting mark in the field is tumor-infiltrating lymphocytes (TILs). Tumor-infiltrating lymphocyte therapy has consistently yielded durable clinical responses in selected patients with metastatic melanoma and is now being increasingly applied to treat other solid tumors, including head and neck squamous cell carcinoma, cervical cancer, breast cancer, and lung cancer. Despite its long history in the clinic and key developments over the last few decades that have augmented response rates and have made TIL manufacturing more streamlined, a number of key outstanding conceptual questions remain to be answered in the TIL therapy field. In this review, we address critical questions, including the mechanism of action of TILs and active T-cell subsets, the current need for lymphoablative preconditioning, predictive biomarkers, the role of combination therapy such as checkpoint blockade, new excitement over the recognition of mutated antigens (the mutanome) by TILs, and issues in developing TILs for nonmelanoma indications. In each case, we will critically discuss the main issues and concerns and how they can affect the eventual positioning of TIL therapy in the mainstream of cancer care.
机译:在过去的几年中,自体过继性T细胞疗法取得了长足进步,目前可以通过对包括嵌合抗原受体和重组T细胞受体在内的任何所需抗原重新编程T细胞特异性的技术引起了人们的兴奋。时间将证明这些新的基因工程T细胞技术是否如所宣传的那样有效,特别是在实体瘤中,考虑到特定抗原的有限供应以及难以控制的无法预测的靶标,组织外毒性的问题。但是,已在患者中使用的T细胞疗法的形式比其他任何一种都多,并且在该领域留下了长久的印记,它是肿瘤浸润淋巴细胞(TIL)。肿瘤浸润淋巴细胞疗法一直在选定的转移性黑色素瘤患者中产生持久的临床反应,并且现在正越来越多地用于治疗其他实体瘤,包括头颈部鳞状细胞癌,宫颈癌,乳腺癌和肺癌。尽管其在诊所中的悠久历史和过去几十年来的重要发展提高了反应率,并使TIL的生产更加简化,但在TIL治疗领域仍有许多关键的重要概念性问题需要解答。在这篇综述中,我们解决了关键问题,包括TIL和活跃的T细胞亚群的作用机制,目前对淋巴消融预处理的需求,预测性生物标志物,联合治疗的作用(如检查点封锁),对突变识别的新兴趣TILs产生的抗原(诱变),以及针对非黑素瘤适应症的TILs开发中的问题。在每种情况下,我们都将批判性地讨论主要问题和疑虑,以及它们如何影响TIL治疗最终在癌症治疗主流中的定位。

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