复发急性淋巴细胞白血病患儿的预后及影响因素单中心分析

doi:10.12372/jcp.2025.24e0563

摘要/Abstract

摘要：

目的探讨急性淋巴细胞白血病（ALL）复发患儿的临床特征及分析影响预后的因素。方法选取 2006年2月至2019年12月接受国内儿童急性淋巴细胞白血病协作组方案治疗的458例初诊ALL儿童，回顾性分析76例复发ALL儿童的临床特征及影响预后因素。结果本中心儿童ALL总体复发率为16.6%（76/458）；复发ALL患儿死亡率57.9%（44/76），复发ALL患儿5年总体生存率为（38.6±5.9）%。按复发时间分组，极早期复发26例、早期复发30例、晚期复发20例，三组5年总体总生存率（OS）差异有统计学意义（P<0.001）。按复发部位分组，单纯骨髓复发57例，髓外复发12例及髓内外联合复发7例，三组5年OS率差异有统计学意义（P<0.05）。76例复发儿童11例放弃治疗，65例接受再次治疗，未获得2次完全缓解（CR2）14例，获CR2 51例，两组5年OS率差异有统计学意义（P<0.001）。按照复发后治疗方式分组分为异基因造血干细胞移植组（Allo-HSCT）22例（33.8%），嵌合抗原受体T细胞疗法（CART）治疗组8例（12.3%），CART联合Allo-HSCT组14例（21.5%），单纯化疗和（或）靶向药物组21例（32.2%），组间比较5年OS率差异有统计学意义（P<0.001）。单因素预后分析显示初诊白细胞>100×10⁹/L、初诊危险度、复发时间、复发部位、复发后危险度、复发后治疗方案、是否获得CR2是影响复发ALL儿童预后的独立危险因素（P<0.05）。Cox回归模型进行多因素预后分析，极早期复发和复发后未获得CR2是影响复发ALL患儿预后的独立危险因素（P<0.05），复发后接受CART细胞衔接移植治疗是复发ALL患儿预后保护因素。结论本中心儿童ALL复发时间以早期复发为主，复发部位以骨髓复发为主。多因素预后分析极早期复发和复发后未获得CR2是复发ALL患儿预后的独立危险因素（P<0.05）。CART联合Allo-HSCT可改善复发急淋患儿预后。

关键词: 儿童, 复发急性淋巴细胞白血病, 预后, 嵌合抗原受体T细胞疗法, 异基因造血干细胞移植

Abstract:

Objective To investigate the clinical characteristics and prognostic factors of children with relapsed acute lymphoblastic leukemia (ALL). Methods A total of 458 newly diagnosed ALL children who treated with the Chinese Children's Leukemia Group (CCLG) protocol at hospital between February 2006 and December 2019 were selected. Results The overall relapse rate of childhod ALL in this center was 16.6% (76/458). The mortality rate among relapsed ALL children was 57.9% (44/76), and the 5-year overall survival (OS) rate for relapsed ALL children was 38.6% ± 5.9%. Grouped by time to relapse, the cohort included 26 cases of very early relapse, 30 cases of early relapse, and 20 cases of late relapse. There was a statistically significant difference in the 5-year overall survival rate (OS) among the three groups(P<0.001). When categorized by relapse site, 57 cases involved isolated bone marrow relapse, 12 cases had extramedullary relapse, and 7 cases exhibited combined medullary/extramedullary relapse. There was a statistically significant difference in the 5-year OS rate among the three groups (P<0.05). Among the 76 relapsed children, 11 discontinued treatment, while 65 received retreatment. Among them, 14 failed to achieve a second complete remission (CR2), whereas 51 attained CR2. There was a statistically significant difference in the 5-year OS rate between the two groups (P<0.001). Based on post-relapse treatment modalities,the patients were divided into allogeneic hematopoietic stem cell transplantation (Allo-HSCT) group (22 cases, 33.8%), chimeric antigen receptor T-cell immunotherapy (CART) group (8 cases, 12.3%), CAR-T combined with Allo-HSCT group (14 cases, 21.5%), and chemotherapy and/or targeted therapy group (21 cases, 32.2%). There was a statistically significant difference in the 5-year OS rate among the groups (P<0.001). Univariate prognostic analysis revealed that initial white blood cell count>100×10⁹/L, initial risk stratification, relapse time, relapse site, post-relapse risk stratification, post-relapse treatment modality, and failure to achieve CR2 were independent risk factors affecting the prognosis of relapsed ALL children (P<0.05). Multivariate analysis using the Cox regression model identified very early relapse and failure to attain CR2 after relapse as independent risk factors for poor prognosis in relapsed ALL children (P<0.05), while post-relapse treatment with CAR-T bridging to allogeneic hematopoietic stem cell transplantation (Allo-HSCT) was a protective prognostic factor. Conclusions The predominant relapse pattern in our center was early recurrence, with bone marrow being the main relapse site. Multivariate analysis revealed that very early relapse and failure to achieve CR2 were independent adverse prognostic factors (P<0.05). CART combined with Allo-HSCT significantly improved outcomes in children with relapsed ALL.

Key words: child, relapsed acute lymphoblastic leukemia, prognosis, CART, allo-HSCT

王真, 朱嘉莳, 付盼, 王丹, 张娜, 邵静波, 李红. 复发急性淋巴细胞白血病患儿的预后及影响因素单中心分析[J]. 临床儿科杂志, 2025, 43(4): 271-277.

WANG Zhen, ZHU Jiashi, FU Pan, WANG Dan, ZHANG Na, SHAO Jingbo, LI Hong. Single center analysis of prognosis and influencing factors in relapsed pediatric acute lymphoblastic leukemia[J]. Journal of Clinical Pediatrics, 2025, 43(4): 271-277.

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分期	B-ALL			T-ALL
分期	单纯髓外复发	髓内外联合复发	单纯骨髓复发	单纯髓外复发	髓内外联合复发	单纯骨髓复发
非常早期	高危	高危	高危	高危	高危	高危
早期	中危	中危	高危	中危	高危	高危
晚期	标危	中危	中危	标危	高危	高危

因素	5年OS ($\bar{x}±s$)/%	例数	χ²值	P
年龄/岁			2.11	0.147
<10	41.2±6.6	64
≥10	25.0±12.5	12
初发治疗方案			3.68	0.055
SCMC-ALL-2005	31.5±6.6	50
CCCG-ALL-2015	55.5±10.9	26
性别			0.00	0.992
男	38.9±7.9	44
女	38.2±9.0	32
初诊WBC/×10⁹·L^-1			9.80	0.002
<100	41.1±6.3	69
≥100	14.3±13.2	7
免疫分型			1.29	0.256
B-ALL	39.7±6.1	72
T-ALL	0	4
危险度			9.73	0.008
LR	67.8±11.2	22
IR	30.8±8.6	32
HR	22.7±8.9	22
细胞遗传学异常		16	2.16	0.706
TEL/AML	60.0±21.9	5
E2A-PBX1	0	1
MLL	37.5±17.1	8
BCR/ABL	0	2
染色体			2.57	0.464
亚二倍体	0	3
超高二倍体	66.7±15.7	9
其他	37.9±6.9	51
无分裂相	29.9±16.5	13
复发部位			7.36	0.025
骨髓复发	30.3±6.4	57
单纯髓外复发	61.9±15.2	12
髓内外联合复发	68.6±18.6	7
复发时间			28.49	<0.001
极早期复发	11.5±6.3	26
早期复发	44.2±9.4	30
晚期复发	68.3±12.2	20
复发后危险分组			16.34	<0.001
LR	100%	4
IR	58.2±10.4	27
HR	22.7±6.4	45
初诊D19MRD		56	2.98	0.395
<0.01	55.6±14.9	12
0.01~0.09	50.9±16.3	11
0.1~0.99	61.1±12.6	17
≥1.0	29.2±11.8	16
初诊D46MRD		56	0.93	0.336
<0.01	54.0±8.4	40
≥0.01	40.0±17.4	16
是否获得CR2		65	9.45	0.002
是	59.9±7.5	51
否	0	14
复发后治疗方式		65	19.61	<0.001
化疗和/或靶向药物	14.3±7.6	21
CART	42.9±22.4	8
Allo-HSCT	48.2±11.0	22
CART联合 Allo-HSCT	91.7±8.0	14

因素	β	SE	Wald χ²	HR	95%CI	P
复发时间
极早期复发				1
早期复发	1.52	0.42	13.14	0.43	0.20~0.93	0.032
晚期复发	2.67	0.66	22.74	0.21	0.07~0.63	0.005
是否CR2
否				1
是	0.89	0.58	1.01	0.38	0.14~0.99	0.004
复发后治疗
CART联合Allo-HSCT				1
CART	1.87	0.65	9.72	6.19	0.58~66.00	0.131
化疗（或）靶向药物	2.66	0.53	0.17	12.54	1.52~103.63	0.019
Allo-HSCT	2.17	0.96	1.31	10.65	1.37~82.96	0.024