多色流式细胞术在未选择的急性髓系白血病患者队列中评估可测量残余疾病的技术和临床有效性。

Archives of pathology & laboratory medicine Pub Date : 2025-06-16 DOI:10.5858/arpa.2025-0053-OA

Sa A Wang, Shaoying Li, Wei Wang, Jie Xu, Beenu Thakral, Shimin Hu, Chi Young Ok, Fuli Jia, Jeffrey L Jorgensen, L Jeffrey Medeiros, Farhad Ravandi, Nicholas J Short, Sanam Loghavi

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引用次数: 0

摘要

上下文。在验证了多色流式细胞术（MFC）检测急性髓性白血病（AML）可测量残留病（MRD）的方法后，本研究探讨了其临床适用性。-：评估基于mfc的MRD检测在aml设计中的实用性和性能。-：通过随访研究、分子遗传学和生存数据，前瞻性评估未选择的AML MRD MFC患者实现形态学缓解。-：在该队列的379例患者骨髓样本中，359例（95%）获得了可解释的结果。359例中57例（16%）MRD阳性，最常见的免疫表型为CD34+CD117+髓系(n = 46；81%)，其次是CD34-/CD117+髓细胞(n = 8；14%)和单核细胞(n = 3；5%)。在57例MRD+病例中，6例（11%）没有可用的白血病相关免疫表型，51例（31%）白血病相关免疫表型的患者中有16例（31%）表现出明显的免疫表型漂移/切换，突出了“偏离正常”方法的重要性。其余302例MRD阴性；其中，21例（6%）患者在18例（86%）患者中表现出与持续克隆造血相关的白血病前期免疫表型。MFC阳性结果与后续随访MRD阳性（45例中有41例[91%]对240例中有14例[6%]，P < 0.01）、形态复发（55例中有42例[76%]对301例中有48例[16%]，P < 0.01）、较差的总生存期（12.5个月对未达到，P < 0.01）和无白血病生存期（6.5个月对未达到，P < 0.01）密切相关。在mrd阴性患者中，白血病前期表型与较短的总生存期相关（P = 0.03），但与无白血病生存期无关（P = 0.16）。我们的研究为考虑MFC AML MRD实施的实验室提供了数据驱动的技术见解，并提供了强有力的证据，支持MFC在不同阶段治疗和监测的AML患者中MRD评估的效用。

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Technical and Clinical Validity of Assessing Measurable Residual Disease by Multicolor Flow Cytometry in an Unselected Acute Myeloid Leukemia Patient Cohort.

Context.—: Following the validation of a multicolor flow cytometry (MFC) assay for measurable residual disease (MRD) in acute myeloid leukemia (AML), this study examines its clinical applicability.

Objective.—: To evaluate the practicality and performance of MFC-based MRD detection in AML.

Design.—: Prospectively assessed AML MRD MFC in unselected AML patients achieving morphologic remission with follow-up studies, molecular genetics, and survival data.

Results.—: Among 379 patient bone marrow samples in this cohort, an interpretable result was obtained in 359 (95%). A total of 57 of the 359 cases (16%) were positive for MRD, and the most frequently observed immunophenotype was CD34+CD117+ myeloid (n = 46; 81%), followed by CD34-/CD117+ myeloid (n = 8; 14%) and monocytic (n = 3; 5%). Of 57 MRD+ cases, 6 (11%) had no leukemia-associated immunophenotypes available, and 16 of 51 (31%) with leukemia-associated immunophenotype for comparison exhibited significant immunophenotypic drift/switch, highlighting the importance of the "deviation from normal" approach. The remaining 302 cases were MRD negative; among these, 21 (6%) displayed a preleukemic immunophenotype that was associated with persistent clonal hematopoiesis in 18 patients (86%). A positive MFC result was strongly associated with subsequent follow-up positive MRD (41 of 45 [91%] versus 14 of 240 [6%], P < .01), morphologic relapse (42 of 55 [76%] versus 48 of 301 [16%], P < .01), an inferior overall survival (12.5 months versus not reached, P < .01), and leukemia-free survival (6.5 months versus not reached, P < .01). Among MRD-negative patients, a preleukemic phenotype was associated with a shorter overall survival (P = .03), but not leukemia-free survival (P = .16).

Conclusions.—: Our study provides data-driven technical insights for laboratories considering MFC AML MRD implementation and offers strong evidence supporting the utility of MRD assessment by MFC in patients with AML undergoing various stages of treatment and surveillance.

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Archives of pathology & laboratory medicine

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