Deciphering stage 0 hematogones by flow cytometry in follow-up bone marrow samples of pediatric B—Acute lymphoblastic leukemia cases: A potential mimicker of residual disease after anti CD19 therapy

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS
Thulasi Raman Ramalingam, Lakshman Vaidhyanathan, Anurekha Muthu, Venkateswaran Vellaichamy Swaminathan, Ramya Uppuluri, Revathi Raj
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Abstract

CD19 is frequently targeted for immunotherapy in B cell malignancies, which may result in loss of CD19 expression in leukemic cells as an escape mechanism. Stage 0 hematogones (Hgs) are normal CD19-negative very early B cell precursors that can be potentially mistaken for CD19 negative residual leukemic cells by flow cytometry (FCM) in B cell acute lymphoblastic leukemia (BCP-ALL) cases treated with anti CD19 therapy. Our main objective was to characterize and study the incidence of stage 0 hematogones in follow-up bone marrow samples of pediatric BCP-ALL cases. We analyzed the flow cytometry standard files of 61 pediatric BCP-ALL cases treated with conventional chemotherapy and targeted anti-CD19 therapy, for identifying the residual disease and normal B cell precursors including stage 0 Hgs. A non-CD19 alternate gating strategy was used to isolate the B cells for detecting the residual disease and stage 0 Hgs. The stage 0 Hgs were seen in 95% of marrow samples containing CD19+ Hgs. When compared with controls and posttransplant marrow samples, the fraction of stage 0 Hgs was higher in patients receiving anti CD19 therapy (p = 0.0048), but it was not significant when compared with patients receiving chemotherapy (p = 0.1788). Isolated stage 0 Hgs are found in samples treated with anti-CD19 therapy simulating CD19 negative residual illness. Our findings aid in understanding the stage 0 Hgs and its association with CD19+ Hgs in anti CD19 therapy and conventional chemotherapy. This is crucial as it can be potentially mistaken for residual disease in patients treated with anti CD19 therapy.

通过流式细胞术破译小儿 B 型急性淋巴细胞白血病随访骨髓样本中的 0 期血细胞:抗 CD19 治疗后残留疾病的潜在模拟者。
在 B 细胞恶性肿瘤中,CD19 经常是免疫疗法的靶点,这可能会导致白血病细胞中 CD19 表达的缺失,成为一种逃逸机制。在接受抗 CD19 治疗的 B 细胞急性淋巴细胞白血病(BCP-ALL)病例中,0 期血原(Hgs)是正常的 CD19 阴性极早期 B 细胞前体,通过流式细胞术(FCM)可能会被误认为是 CD19 阴性的残留白血病细胞。我们的主要目的是描述和研究小儿 BCP-ALL 病例随访骨髓样本中 0 期血原的发生率。我们分析了61例接受常规化疗和抗CD19靶向治疗的小儿BCP-ALL病例的流式细胞术标准文件,以确定残留的疾病和正常B细胞前体,包括0期Hgs。采用非 CD19 交替选通策略来分离 B 细胞,以检测残留疾病和 0 期 Hgs。在 95% 含有 CD19+ Hgs 的骨髓样本中都能看到 0 期 Hgs。与对照组和移植后骨髓样本相比,接受抗 CD19 治疗的患者中 0 期 Hgs 的比例更高(p = 0.0048),但与接受化疗的患者相比,0 期 Hgs 的比例并不显著(p = 0.1788)。在模拟 CD19 阴性残留病的抗 CD19 治疗样本中发现了孤立的 0 期 Hgs。我们的研究结果有助于了解抗 CD19 疗法和传统化疗中的 0 期 Hgs 及其与 CD19+ Hgs 的关联。这一点至关重要,因为它有可能被误认为是抗 CD19 治疗患者的残留疾病。
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
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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