Safety and feasibility of anti-CD19 CAR T cells with fully human binding domains in patients with B-cell lymphoma

CD19 淋巴瘤 嵌合抗原受体 免疫原性 毒性 T细胞 弥漫性大B细胞淋巴瘤 医学 抗原 内科学 免疫学 免疫系统
作者
Jennifer N. Brudno,Norris Lam,Danielle Vanasse,Yueh-wei Shen,Jeremy J. Rose,John M. Rossi,Allen Xue,Adrian Bot,Nathalie Scholler,Lekha Mikkilineni,Mark Roschewski,Robert M. Dean,Raúl E. Cachau,Philippe Youkharibache,Rashmika Patel,Brenna Hansen,David F. Stroncek,Steven A. Rosenberg,Ronald E. Gress,James N. Kochenderfer
出处
期刊:Nature Medicine [Nature Portfolio]
卷期号:26 (2): 270-280 被引量:313
标识
DOI:10.1038/s41591-019-0737-3
摘要

Anti-CD19 chimeric antigen receptor (CAR)-expressing T cells are an effective treatment for B-cell lymphoma, but often cause neurologic toxicity. We treated 20 patients with B-cell lymphoma on a phase I, first-in-human clinical trial of T cells expressing the new anti-CD19 CAR Hu19-CD828Z (NCT02659943). The primary objective was to assess safety and feasibility of Hu19-CD828Z T-cell therapy. Secondary objectives included assessments of blood levels of CAR T cells, anti-lymphoma activity, second infusions and immunogenicity. All objectives were met. Fifty-five percent of patients who received Hu19-CD828Z T cells obtained complete remission. Hu19-CD828Z T cells had clinical anti-lymphoma activity similar to that of T cells expressing FMC63-28Z, an anti-CD19 CAR tested previously by our group, which contains murine binding domains and is used in axicabtagene ciloleucel. However, severe neurologic toxicity occurred in only 5% of patients who received Hu19-CD828Z T cells, whereas 50% of patients who received FMC63-28Z T cells experienced this degree of toxicity (P = 0.0017). T cells expressing Hu19-CD828Z released lower levels of cytokines than T cells expressing FMC63-28Z. Lower levels of cytokines were detected in blood from patients who received Hu19-CD828Z T cells than in blood from those who received FMC63-28Z T cells, which could explain the lower level of neurologic toxicity associated with Hu19-CD828Z. Levels of cytokines released by CAR-expressing T cells particularly depended on the hinge and transmembrane domains included in the CAR design.
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