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共表达淋巴细胞标志物的急性髓系白血病(AML)的特征:T细胞抗原阳性和B细胞抗原阳性AML之间不同的生物学特征

Characterization of acute myeloid leukemia (AML) coexpressing lymphoid markers: different biologic features between T-cell antigen positive and B-cell antigen positive AML.

作者信息

Tien H F, Wang C H, Chen Y C, Shen M C, Lin D T, Lin K H

机构信息

Department of Internal Medicine, National Taiwan University Hospital, Taipei, Republic of China.

出版信息

Leukemia. 1993 May;7(5):688-95.

PMID:8483320
Abstract

The clinical and biologic characteristics of acute myeloid leukemia (AML) with coexpression of lymphoid-associated antigens (Lym+ AML) were studied from 39 cases who represented 24% of 161 newly diagnosed de novo AML. Twenty-seven cases (16.8%) were positive for the expression of T-cell markers (T+ AML) and 12 (7.5%) for B-cell markers (B+ AML). Chromosomal abnormalities t(9;22)(q34;q11) and t/del(11)(q23), which were considered to be associated with acute leukemia coexpressing markers of more than one cell lineage, were detected in five and in four patients, respectively. There was no prognostic significance of B-cell or T-cell antigen expression in AML. Of 12 T+ AML cases in which cells were available for gene analysis, all showed germline configuration of immunoglobulin heavy chain and T-cell receptor beta chain genes, while seven of nine B+ AML showed rearrangements of either or both of the genes. Double labeling of the cells with myeloperoxidase and lymphoid markers demonstrated that individual blasts in all the five T+ AML tested were simultaneously expressing myeloperoxidase activity and CD7; however, most blasts in the three B+ AML studied expressed either myeloperoxidase activity or CD10, but not both. In eight of the nine T+ AML tested, the T-cell antigen-positive leukemic blasts were significantly decreased to less than 10%, after in vitro culture with the differentiation-inducing agent phorbol ester. B-cell markers remained positive (> or = 20%) on the cells in the two B+ AML who had the same study. These findings suggested that T+ AML and B+ AML might have different biologic features. Further studies on more patients are needed to clarify this point.

摘要

对161例新诊断的初发急性髓系白血病(AML)患者中的39例(占24%)进行了研究,这些患者同时表达淋巴系相关抗原(淋巴系抗原阳性AML)。27例(16.8%)表达T细胞标志物(T + AML),12例(7.5%)表达B细胞标志物(B + AML)。分别在5例和4例患者中检测到染色体异常t(9;22)(q34;q11)和t/del(11)(q23),这些异常被认为与共表达多个细胞系标志物的急性白血病相关。AML中B细胞或T细胞抗原表达无预后意义。在12例可进行基因分析的T + AML病例中,所有病例的免疫球蛋白重链和T细胞受体β链基因均呈胚系构型,而9例B + AML中的7例显示其中一个或两个基因发生重排。用髓过氧化物酶和淋巴系标志物对细胞进行双重标记显示,所有检测的5例T + AML中的单个原始细胞同时表达髓过氧化物酶活性和CD7;然而,所研究的3例B + AML中的大多数原始细胞要么表达髓过氧化物酶活性,要么表达CD10,但并非两者同时表达。在检测的9例T + AML中的8例中,用分化诱导剂佛波酯进行体外培养后,T细胞抗原阳性的白血病原始细胞显著减少至低于10%。在进行相同研究的2例B + AML中,细胞上的B细胞标志物仍为阳性(≥20%)。这些发现提示T + AML和B + AML可能具有不同的生物学特征。需要对更多患者进行进一步研究以阐明这一点。

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