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Adoptive T-cell therapy: adverse events and safety switches

机译:过继性T细胞疗法:不良事件和安全开关

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摘要

The potential of adoptive T-cell therapy in effecting complete and durable responses has been demonstrated in a number of malignant and infectious diseases. Ongoing progress in T-cell engineering has given cause for optimism in the broader clinical applicability of this approach. However, the development of more potent T cells is checked by safety concerns, highlighted by the occurrence of on-target and off-target toxicities that, although uncommon, have been fatal on occasions. Timely pharmacological intervention is effective in the management of a majority of adverse events but adoptively transferred T cells can persist long term, along with any unwanted effects. A recently validated cellular safety switch, inducible caspase 9 (iCasp9), has the potential to mitigate the risks of T-cell therapy by enabling the elimination of transferred T cells if required. In haematopoietic stem cell transplantation, iCasp9-modified donor T cells can be rapidly eliminated in the event of graft-versus-host disease. This review presents an overview of the risks associated with modern T-cell therapy and the development, clinical results and potential future application of the iCasp9 safety switch.
机译:在许多恶性和传染性疾病中已经证明了过继性T细胞疗法在实现完全和持久应答方面的潜力。 T细胞工程学的不断发展使这种方法在更广泛的临床应用中变得乐观。然而,更安全的T细胞的发展受到安全方面的关注,特别是目标上和目标外的毒性的发生,这虽然不常见,但有时会致命。及时的药理干预可有效控制大多数不良事件,但过继转移的T细胞可长期持续存在,并具有任何不良作用。最近经过验证的细胞安全开关,诱导型半胱天冬酶9(iCasp9),有可能通过消除需要转移的T细胞来减轻T细胞治疗的风险。在造血干细胞移植中,如果发生移植物抗宿主病,则可以快速消除iCasp9修饰的供体T细胞。这篇综述概述了与现代T细胞疗法相关的风险以及iCasp9安全开关的开发,临床结果和潜在的未来应用。

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