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肿瘤免疫治疗中的 T 细胞工程。

T-cell engineering for cancer immunotherapy.

机构信息

Molecular Pharmacology and Chemistry Program, Center for Cell Engineering, Memorial Sloan-Kettering Cancer Center, New York, NY 10065, USA.

出版信息

Cancer J. 2009 Nov-Dec;15(6):451-5. doi: 10.1097/PPO.0b013e3181c51f37.

Abstract

The adoptive transfer of tumor-reactive cells is a promising approach for the treatment of melanoma and some other cancers. To remedy the difficulties associated with the isolation and expansion of tumor-reactive T cells in most cancer patients, peripheral blood T cells can be retargeted to any chosen tumor antigen by the genetic transfer of an antigen-specific receptor. The transduced receptors may be human leukocyte antigen-restricted, heterodimeric T-cell antigen receptor (TCRs), or chimeric antigen receptors (CARs), which typically recognize native cell-surface antigens. Considerable progress has been made in recent years to address the challenges posed by the transfer of either receptor type. Vector and protein modifications enable the expression of TCR chains in human T cells at functional levels and with a reduced risk of mis-pairing with endogenous TCR chains. The combinatorial inclusion of activating and costimulatory domains in CARs has dramatically enhanced the signaling properties of the chimeric receptors described over a decade ago. Based on the effective T-cell transduction and expansion procedures now available to support clinical investigation, improved designer TCRs and second generation CARs targeting an array of antigens are being evaluated in a range of hematological malignancies and solid tumors.

摘要

肿瘤反应性细胞的过继转移是治疗黑色素瘤和其他一些癌症的一种很有前途的方法。为了克服大多数癌症患者中肿瘤反应性 T 细胞的分离和扩增所面临的困难,可以通过遗传转移抗原特异性受体使外周血 T 细胞重新靶向任何选定的肿瘤抗原。转导的受体可以是人类白细胞抗原受限的异二聚体 T 细胞抗原受体(TCR)或嵌合抗原受体(CAR),它们通常识别天然的细胞表面抗原。近年来,在解决这两种受体类型转移所带来的挑战方面取得了相当大的进展。载体和蛋白修饰使 TCR 链能够以功能性水平在人 T 细胞中表达,并降低了与内源性 TCR 链错误配对的风险。在 CAR 中组合包含激活和共刺激结构域极大地增强了十多年前描述的嵌合受体的信号转导特性。基于现在可用于支持临床研究的有效的 T 细胞转导和扩增程序,针对一系列抗原的改良设计 TCR 和第二代 CAR 正在一系列血液恶性肿瘤和实体瘤中进行评估。

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