Circulating CD22+/CD19−/CD24− progenitors and CD22+/CD19+/CD24− mature B cells: Diagnostic pitfalls for minimal residual disease detection in B-lymphoblastic leukemia

IF 2.3 3区医学 Q3 MEDICAL LABORATORY TECHNOLOGY

Cytometry Part B: Clinical Cytometry Pub Date : 2022-11-26 DOI:10.1002/cyto.b.22104

Ting Zhou, Jeremiah Karrs, Truc Ho, Alyssa Doverte, James N. Kochenderfer, Nirali N. Shah, Constance M. Yuan, Hao-Wei Wang

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引用次数: 2

Abstract

Background

Multiparametric flow cytometry (MFC) has become a powerful tool in minimal residual disease (MRD) detection in B-lymphoblastic leukemia/lymphoma (B-ALL). In the setting of targeted immunotherapy, B-ALL MRD detection often relies on alterative gating strategies, such as the utilization of CD22 and CD24. It is important to depict the full diversity of normal cell populations included in the alternative B-cell gating methods to avoid false-positive results. We describe two CD22-positive non-neoplastic cell populations in the peripheral blood (PB), including one progenitor population of uncertain lineage and one mature B-cell population, which are immunophenotypic mimics of B-ALL.

Methods

Using MFC, we investigated the prevalence and phenotypic profiles of both CD22-positive populations in 278 blood samples from 52 patients with B-ALL; these were obtained pre- and post-treatment with CD19 and/or CD22 CAR-T therapies. We further assessed whether these two populations in the blood were exclusively associated with B-ALL or recent anticancer therapies, by performing the same analysis on patients diagnosed with other hematological malignancies but in long-term MRD remission.

Results

The progenitor population and mature B-cell population were detected at low levels in PB of 61.5% and 44.2% of B-ALL patients, respectively. Both cell types showed distinctive and highly consistent antigen expression patterns that are reliably distinguishable from B-ALL. Furthermore, their presence is not restricted solely to B-ALL or recent therapy.

Conclusions

Our findings aid in building a complete immunophenotypic profile of normal cell populations in PB, thereby preventing misdiagnosis of B-ALL MRD and inappropriate management.

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循环CD22+/CD19−/CD24−祖细胞和CD22+/CD19+/CD24−成熟B细胞:B淋巴母细胞白血病最小残留病检测的诊断缺陷

背景多参数流式细胞术(MFC)已成为b淋巴母细胞白血病/淋巴瘤(B-ALL)微小残留病(MRD)检测的有力工具。在靶向免疫治疗的背景下，B-ALL MRD检测通常依赖于替代的门控策略，如CD22和CD24的利用。重要的是描述包括在备选b细胞门控方法中的正常细胞群的全部多样性，以避免假阳性结果。我们描述了外周血(PB)中两个cd22阳性的非肿瘤细胞群，包括一个谱系不确定的祖细胞群和一个成熟的b细胞群，它们是B-ALL的免疫表型模拟物。方法采用MFC技术，研究了52例B-ALL患者278份血液样本中两种cd22阳性人群的患病率和表型特征;这些是在CD19和/或CD22 CAR-T疗法治疗前后获得的。通过对诊断为其他血液恶性肿瘤但长期MRD缓解的患者进行相同的分析，我们进一步评估了血液中的这两种人群是否仅与B-ALL或最近的抗癌治疗相关。结果61.5%和44.2%的B-ALL患者外周血中存在低水平的祖细胞群和成熟b细胞群。两种细胞类型均表现出独特且高度一致的抗原表达模式，可与B-ALL可靠区分。此外，它们的存在不仅限于B-ALL或最近的治疗。结论我们的研究结果有助于建立PB正常细胞群的完整免疫表型谱，从而防止B-ALL MRD的误诊和不适当的治疗。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Cytometry Part B: Clinical Cytometry 医学-病理学

CiteScore

6.80

自引率

32.40%

发文量

审稿时长

>12 weeks

期刊介绍： Cytometry Part B: Clinical Cytometry features original research reports, in-depth reviews and special issues that directly relate to and palpably impact clinical flow, mass and image-based cytometry. These may include clinical and translational investigations important in the diagnostic, prognostic and therapeutic management of patients. Thus, we welcome research papers from various disciplines related [but not limited to] hematopathologists, hematologists, immunologists and cell biologists with clinically relevant and innovative studies investigating individual-cell analytics and/or separations. In addition to the types of papers indicated above, we also welcome Letters to the Editor, describing case reports or important medical or technical topics relevant to our readership without the length and depth of a full original report.