School of Life Sciences, Beijing University of Chinese Medicine, Beijing, China.
Department of Gene and Cellular Therapy, Shenzhen Research Institute, Beijing University of Chinese Medicine, Shenzhen, China.
Oncoimmunology. 2021 Aug 17;10(1):1959102. doi: 10.1080/2162402X.2021.1959102. eCollection 2021.
BCMA-targeting chimeric antigen receptor (CAR)-T cell therapy has shown remarkable clinical efficacy against multiple myeloma, yet antigen escape and tumor relapse still occur after the use of these therapies. Designing CAR-T therapies that targets multiple antigens simultaneously seems a feasible way to avoid antigen escape, and it has been extensively studied elsewhere. Here, we report novel BCMA-OR-CD38 Tan CAR T cells that can trigger robust cytotoxicity against target cells expressing either BCMA or CD38. We demonstrate that, in studies, these BCMA-OR-CD38 Tan CAR T cells exhibit similar CAR expression, superior cytotoxicity and antigen-stimulated T cell proliferation as compared to single-targeted CAR T cells or CD38-OR-BCMA Tan CAR T cells. Importantly, these BCMA-OR-CD38 Tan CAR-T cells can achieve complete tumor clearance in myeloma-bearing mice with no relapse observed through the course of these experiments. Finally, this BCMA-OR-CD38 Tan CAR was fully compatible with existing clinical grade T cell manufacturing procedures and can be implemented using current clinical protocols. Taken together, our results present an effective solution to the challenge of antigen escape in BCMA CAR T-cell therapies.
BCMA 靶向嵌合抗原受体 (CAR)-T 细胞疗法在多发性骨髓瘤的治疗中表现出显著的临床疗效,但在使用这些疗法后仍会发生抗原逃逸和肿瘤复发。设计同时针对多种抗原的 CAR-T 疗法似乎是避免抗原逃逸的一种可行方法,这在其他地方已得到广泛研究。在这里,我们报告了新型的 BCMA-OR-CD38 Tan CAR T 细胞,其可以对表达 BCMA 或 CD38 的靶细胞触发强大的细胞毒性。我们证明,在研究中,与单靶向 CAR T 细胞或 CD38-OR-BCMA Tan CAR T 细胞相比,这些 BCMA-OR-CD38 Tan CAR T 细胞表现出相似的 CAR 表达、优越的细胞毒性和抗原刺激的 T 细胞增殖。重要的是,这些 BCMA-OR-CD38 Tan CAR-T 细胞可以在骨髓瘤荷瘤小鼠中实现完全清除肿瘤,在实验过程中未观察到复发。最后,这种 BCMA-OR-CD38 Tan CAR 与现有的临床级 T 细胞制造程序完全兼容,并可使用当前的临床方案实施。总之,我们的结果为 BCMA CAR-T 细胞疗法中的抗原逃逸挑战提供了一种有效的解决方案。
