Effective MRD clearance and long-term survival with CD19 CAR-T in pediatric B-ALL patients with MRD positivity or chemotherapy intolerance.

IF 5.9 2区医学 Q1 IMMUNOLOGY

Frontiers in Immunology Pub Date : 2025-10-06 eCollection Date: 2025-01-01 DOI:10.3389/fimmu.2025.1672509

Yu Wang, Yue-Ping Jia, Ai-Dong Lu, Le-Ping Zhang, Yu-Juan Xue, Hui-Min Zeng

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Abstract

Background: While CD19-directed chimeric antigen receptor T-cell (CAR-T) therapy demonstrates remarkable efficacy in relapsed/refractory (R/R) ALL, its application in earlier treatment lines requires further investigation. This study aimed to evaluate the efficacy, safety, and cellular kinetics of CD19 CAR-T therapy in pediatric B-cell ALL (B-ALL) patients with minimal residual disease (MRD) positivity or chemotherapy intolerance.

Methods: Between 2017 and 2021, 50 eligible pediatric B-ALL patients (with positive MRD or chemotherapy intolerance) received CD19 CAR-T therapy. Efficacy endpoints included complete remission (CR), MRD-negative CR (MRD-CR), overall survival (OS), and leukemia-free survival (LFS). CAR-T cellular kinetics parameters (C_max, AUC_0-28d, persistence) were quantified via qPCR and correlated with clinical outcomes. Safety assessment covered cytokine release syndrome (CRS), immune effector cell-associated neurotoxicity syndrome (ICANS), and infections.

Results: At day 28 post-infusion, the CR and MRD-CR rates were 98% and 96%, respectively. With a median follow-up of 68.7 months, the 5-year OS and LFS rates were 74.9% and 67.8%. Multivariate analysis identified prolonged B-cell aplasia (BCA) duration (HR = 0.969, p = 0.021) and female sex (HR = 0.235, p = 0.032) as independent protective factors for LFS. Cellular kinetics analysis showed effective in vivo expansion in 98% of patients, with a median C_max of 30,860 copies/μg DNA and a median time-to-peak of 10.5 days. The MRD-CR group at day 28 exhibited significantly higher C_max and AUC_0-28d (p = 0.017; p = 0.029) and superior CAR-T persistence (p = 0.030) compared to the non-MRD-CR group. Pre-infusion tumor burden levels did not significantly impact CAR-T expansion or duration. BCA duration positively correlated with CAR-T persistence (r=0.570, p < 0.001), but CAR-T expansion parameters (Cmax and AUC0-28d) did not significantly influence BCA. Regarding safety, grade ≥3 CRS occurred in 16% of patients, and ICANS in 10%. Pre-infusion MRD ≥ 10^-3 was an independent predictor of severe CRS.

Conclusion: CD19 CAR-T therapy demonstrates highly effective MRD clearance and provides long-term survival benefits with a manageable safety profile in pediatric B-ALL patients with MRD positivity or chemotherapy intolerance. Effective CAR-T expansion occurs even at low tumor burdens. These findings support the potential for advancing CAR-T therapy into earlier treatment lines, although its value requires further validation in prospective studies.

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MRD阳性或化疗不耐受的儿童B-ALL患者的有效MRD清除和CD19 CAR-T的长期生存

背景：虽然cd19靶向嵌合抗原受体t细胞（CAR-T）治疗在复发/难治性ALL （R/R）中表现出显著的疗效，但其在早期治疗中的应用还有待进一步研究。本研究旨在评估CD19 CAR-T疗法在患有微小残留病（MRD）阳性或化疗不耐受的儿童b细胞ALL （B-ALL）患者中的疗效、安全性和细胞动力学。方法：在2017年至2021年期间，50名符合条件的儿童B-ALL患者（MRD阳性或化疗不耐受）接受了CD19 CAR-T治疗。疗效终点包括完全缓解（CR）、mrd阴性CR （MRD-CR）、总生存期（OS）和无白血病生存期（LFS）。CAR-T细胞动力学参数（Cmax, AUC0-28d，持续时间）通过qPCR量化，并与临床结果相关。安全性评估包括细胞因子释放综合征（CRS）、免疫效应细胞相关神经毒性综合征（ICANS）和感染。结果：注射后第28天，CR和MRD-CR率分别为98%和96%。中位随访68.7个月，5年OS和LFS分别为74.9%和67.8%。多因素分析发现b细胞发育不全（BCA）持续时间延长（HR = 0.969, p = 0.021）和女性性别（HR = 0.235, p = 0.032）是LFS的独立保护因素。细胞动力学分析表明，98%的患者体内扩增有效，中位Cmax为30,860拷贝/μg DNA，中位峰时间为10.5天。与非MRD-CR组相比，MRD-CR组在第28天表现出更高的Cmax和AUC0-28d （p = 0.017; p = 0.029）和更好的CAR-T持久性（p = 0.030）。输注前肿瘤负荷水平对CAR-T扩增或持续时间没有显著影响。BCA持续时间与CAR-T持续时间呈正相关（r=0.570, p < 0.001），但CAR-T扩展参数（Cmax和AUC0-28d）对BCA无显著影响。在安全性方面，16%的患者发生≥3级CRS， 10%的患者发生ICANS。输注前MRD≥10-3是严重CRS的独立预测因子。结论：CD19 CAR-T疗法在MRD阳性或化疗不耐受的儿童B-ALL患者中显示出高效的MRD清除，提供长期生存益处和可管理的安全性。有效的CAR-T扩增即使在低肿瘤负荷时也能发生。这些发现支持将CAR-T疗法推进到早期治疗线的潜力，尽管其价值需要在前瞻性研究中进一步验证。

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来源期刊

Frontiers in Immunology IMMUNOLOGY-

CiteScore

9.80

自引率

11.00%

发文量

7153

审稿时长

14 weeks

期刊介绍： Frontiers in Immunology is a leading journal in its field, publishing rigorously peer-reviewed research across basic, translational and clinical immunology. This multidisciplinary open-access journal is at the forefront of disseminating and communicating scientific knowledge and impactful discoveries to researchers, academics, clinicians and the public worldwide. Frontiers in Immunology is the official Journal of the International Union of Immunological Societies (IUIS). Encompassing the entire field of Immunology, this journal welcomes papers that investigate basic mechanisms of immune system development and function, with a particular emphasis given to the description of the clinical and immunological phenotype of human immune disorders, and on the definition of their molecular basis.