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利用针对人前B细胞受体的新型单克隆抗体通过流式细胞术诊断急性淋巴细胞白血病的细胞谱系和发育阶段。

Flow cytometric diagnosis of the cell lineage and developmental stage of acute lymphoblastic leukemia by novel monoclonal antibodies specific to human pre-B-cell receptor.

作者信息

Tsuganezawa K, Kiyokawa N, Matsuo Y, Kitamura F, Toyama-Sorimachi N, Kuida K, Fujimoto J, Karasuyama H

机构信息

Department of Immunology, The Tokyo Metropolitan Institute of Medical Science, Tokyo, Japan.

出版信息

Blood. 1998 Dec 1;92(11):4317-24.

PMID:9834238
Abstract

Three novel monoclonal antibodies (MoAbs) have been established that recognize distinct epitopes of a human pre-B-cell receptor (pre-BCR) composed of a mu heavy (muH) chain and a lambda5/VpreB surrogate light (SL) chain. HSL11 reacts with lambda5 whereas HSL96 reacts with VpreB. Intriguingly, HSL2 does not bind to each component of the pre-BCR but does bind to the completely assembled pre-BCR complex. Flow cytometric analyses with cytoplasmic staining of a panel of human cell lines showed that HSL11 and HSL96 specifically stained cell lines derived from the pro-B and pre-B-cell stages of B-cell development. In contrast, HSL2 stained exclusively cell lines derived from the pre-B-cell stage. These results prompted us to explore the possibility of clinical application of these MoAbs for the determination of the cell lineage and developmental stage of acute lymphoblastic leukemia (ALL). Whereas none of mature B-lineage ALLs (B-ALLs), T-lineage ALLs (T-ALLs), and acute myeloid leukemias analyzed were stained in the cytoplasm with these three MoAbs, the vast majority of non-B- and non-T-ALLs (53 out of 56 cases) were found positive for either lambda5, Vpre-B, or both in their cytoplasm. Among these 53 cytoplasmic SL chain-positive ALLs, 19 cases were also positive for cytoplasmic muH chain, indicative of pre-B-cell origin. Interestingly, 6 out of these 19 pre-B-ALL cases were found negative for cytoplasmic staining with HSL2. From these results, we propose a novel classification of B-ALL in which five subtypes are defined on the basis of the differential expression of SL chain, muH chain, pre-BCR, and light chain along the B-cell development.

摘要

已制备出三种新型单克隆抗体(MoAb),它们可识别由μ重链(μH)和λ5/VpreB替代轻链(SL)组成的人类前B细胞受体(pre-BCR)的不同表位。HSL11与λ5反应,而HSL96与VpreB反应。有趣的是,HSL2不与pre-BCR的每个组分结合,但确实与完全组装好的pre-BCR复合物结合。对一组人类细胞系进行细胞质染色的流式细胞术分析表明,HSL11和HSL96特异性地染色源自B细胞发育的前B和前B细胞阶段的细胞系。相比之下,HSL2仅对源自前B细胞阶段的细胞系染色。这些结果促使我们探索这些MoAb在临床应用中用于确定急性淋巴细胞白血病(ALL)细胞谱系和发育阶段的可能性。在分析的成熟B系ALL(B-ALL)、T系ALL(T-ALL)和急性髓系白血病中,没有一种在细胞质中被这三种MoAb染色,但绝大多数非B和非T-ALL(56例中的53例)在其细胞质中被发现λ5、Vpre-B或两者呈阳性。在这53例细胞质SL链阳性的ALL中,19例细胞质μH链也呈阳性,表明起源于前B细胞。有趣的是,在这19例前B-ALL病例中,有6例在细胞质染色中被发现HSL2呈阴性。根据这些结果,我们提出了一种新的B-ALL分类,其中根据SL链、μH链、pre-BCR和轻链在B细胞发育过程中的差异表达定义了五个亚型。

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