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白血病相关表型:其在急性白血病中的特征与发生率

Leukemia-associated phenotypes: their characteristics and incidence in acute leukemia.

作者信息

Babusíková O, Glasová M, Koníková E, Kusenda J

机构信息

Cancer Research Institute, Slovak Academy of Sciences, Bratislava, Slovakia.

出版信息

Neoplasma. 1996;43(6):367-72.

PMID:8996560
Abstract

Leukemia-associated phenotypes have been suggested to be a valuable tool for the detection of minimal residual disease in acute leukemia patients, as they allow to distinguish leukemic blasts from normal hematopoietic progenitor cells. The aim of the present study was to analyze the proportion of acute leukemia patients (both with lymphoid and myeloid leukemias) in which the immunological detection of leukemia-associated phenotypes was convenient for the distinction of leukemic and normal cells. For this purpose we have studied the blast cells from 186 acute leukemia patients at diagnosis with a large panel of monoclonal antibodies by flow cytometry using double staining combinations. From aberrant phenotypes on blast cells we followed lineage infidelity (coexpression of myeloid markers in lymphoid leukemia cells and vice versa, as well as the simultaneous expression of both, T and B cell markers in one lymphoid blast cell) and asynchronous marker expression (simultaneous expression of early and late markers in one cell). One hundred and five of the 186 acute leukemia cases analyzed (56%) showed the presence of leukemia-associated phenotypes. In 41 of the 90 ALL cases followed (46%) and in 40 of the 96 AML cases studied (42%) lineage infidelity was observed. Asynchronous antigen expression was detected in 24 followed cases (13%). Evaluation of the cell marker density by means of calibration microbeads demonstrated abnormal mean channel immunofluorescence and molecules of equivalent soluble fluorescein for CD8 in two patients with T cell malignancies at diagnosis. Abnormal CD8 density might thus represent a characteristic feature of malignant CD8-positive T cell clone. Quantitative marker evaluation therefore seems to be another important mean for the detection of aberrant phenotypes on leukemia cells suitable for the detection of minimal residual disease.

摘要

白血病相关表型已被认为是检测急性白血病患者微小残留病的一种有价值的工具,因为它们能够区分白血病原始细胞与正常造血祖细胞。本研究的目的是分析急性白血病患者(包括淋巴细胞白血病和髓细胞白血病患者)中,白血病相关表型的免疫检测有助于区分白血病细胞与正常细胞的比例。为此,我们运用双色染色组合的流式细胞术,使用一大组单克隆抗体研究了186例急性白血病患者诊断时的原始细胞。从原始细胞的异常表型中,我们追踪谱系不忠实情况(淋巴细胞白血病细胞中髓系标志物的共表达,反之亦然,以及一个淋巴细胞原始细胞中T和B细胞标志物的同时表达)和异步标志物表达(一个细胞中早期和晚期标志物的同时表达)。在分析的186例急性白血病病例中,有105例(56%)显示存在白血病相关表型。在随访的90例ALL病例中有41例(46%),在研究的96例AML病例中有40例(42%)观察到谱系不忠实。在24例随访病例中检测到异步抗原表达(13%)。通过校准微珠评估细胞标志物密度,发现在诊断时两名T细胞恶性肿瘤患者中,CD8的平均通道免疫荧光和等效可溶性荧光素分子存在异常。因此,异常的CD8密度可能代表恶性CD8阳性T细胞克隆的一个特征。因此,定量标志物评估似乎是检测白血病细胞异常表型的另一个重要手段,适用于微小残留病的检测。

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