采珠时外周血白血病负荷对CART19治疗难治性或复发性B-ALL的临床疗效有负面影响。

Molecular Therapy. Methods & Clinical Development Pub Date : 2021-10-27 eCollection Date: 2021-12-10 DOI:10.1016/j.omtm.2021.10.006
Biping Deng, Jing Pan, Zhaoli Liu, Shuangyou Liu, Yunlong Chen, Xiaomin Qu, Yu'e Zhang, Yuehui Lin, Yanlei Zhang, Xinjian Yu, Zhongxin Zhang, Xuansha Niu, Rong Luan, Ming Ma, Xiaomei Li, Tingting Liu, Xi'ai Wu, Huan Niu, Alex H Chang, Chunrong Tong
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引用次数: 4

摘要

我们之前的临床研究表明,靶向CD19 (CART19)的嵌合抗原受体T细胞治疗难治性/复发性B细胞急性淋巴细胞白血病(r/r B- all)后,完全缓解(CR)率>90%;然而,白血病负荷对外周血(PB)母细胞的影响尚不清楚。在这里,我们回顾性分析了143例接受CART19治疗的患者(包括36例PB原细胞患者),以评估采血时外周白血病负荷的影响。117例高疾病负担患者达到了91.5%的CR或不完全计数恢复CR和86.3%的最小残留疾病阴性CR, 26例低疾病负担患者达到96.2%的MRD- CR。总的来说,36例PB母细胞患者中有9例(25%)和107例无PB母细胞患者中有2例(1.87%)对CART19治疗没有反应。白血病在PB中的负担对体外细胞特性(包括CD3+ T细胞的转导效率及其倍数扩增)和体内细胞动力学(包括峰值CART19比例和绝对计数、倍数扩增和持续时间)产生负面影响。进一步的研究表明,这些患者在CART19产物中具有较高的程序性死亡-1表达。我们的数据表明,PB母细胞对r/r B-ALL患者的CART19产生和CART19治疗的临床疗效产生负面影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Peripheral leukemia burden at time of apheresis negatively affects the clinical efficacy of CART19 in refractory or relapsed B-ALL.

Peripheral leukemia burden at time of apheresis negatively affects the clinical efficacy of CART19 in refractory or relapsed B-ALL.

Peripheral leukemia burden at time of apheresis negatively affects the clinical efficacy of CART19 in refractory or relapsed B-ALL.

Peripheral leukemia burden at time of apheresis negatively affects the clinical efficacy of CART19 in refractory or relapsed B-ALL.

Our previous clinical study achieved complete remission (CR) rates of >90% following chimeric antigen receptor T cells targeting CD19 (CART19) treatment of refractory/relapsed B cell acute lymphoblastic leukemia (r/r B-ALL); however, the influence of the leukemia burden in peripheral blood (PB) blasts remains unclear. Here, we retrospectively analyzed 143 patients treated with CART19 (including 36 patients with PB blasts) to evaluate the effect of peripheral leukemia burden at the time of apheresis. One hundred seventeen patients with high disease burdens achieved 91.5% CR or incomplete count recovery CR and 86.3% minimal residual disease-negative CR, and 26 patients with low disease burdens obtained 96.2% MRD- CR. Collectively, 9 of 36 (25%) patients with PB blasts and 2 of 107 (1.87%) patients without PB blasts did not respond to CART19 therapy. The leukemia burden in PB negatively influenced ex vivo cell characteristics, including the transduction efficiency of CD3+ T cells and their fold expansion, and in vivo cell dynamics, including peak CART19 proportion and absolute count, fold expansion, and persistence duration. Further studies showed that these patients had higher programmed death-1 expression in CART19 products. Our data imply that PB blasts negatively affected CART19 production and the clinical efficacy of CART19 therapy in patients with r/r B-ALL.

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