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具有T淋巴细胞特征的急性髓系白血病:一种独特的生物学和临床实体。

Acute myeloid leukemia with T-lymphoid features: a distinct biologic and clinical entity.

作者信息

Cross A H, Goorha R M, Nuss R, Behm F G, Murphy S B, Kalwinsky D K, Raimondi S, Kitchingman G R, Mirro J

机构信息

Department of Virology and Molecular Biology, St Jude Children's Research Hospital, Memphis, TN 38101.

出版信息

Blood. 1988 Aug;72(2):579-87.

PMID:3261183
Abstract

We studied the clinical and biologic features of 10 cases of acute leukemia that met standard French-American-British (FAB) criteria for acute myeloid leukemia (AML) but in which the blast cells also expressed the T-cell-associated CD2 surface antigen. All cases had greater than 3% myeloperoxidase and Sudan black B-positive leukemic blasts, and blasts from seven cases contained Auer rods. Reactivity of the cells with a panel of monoclonal antibodies (MAbs) indicated that leukemic cells in all cases expressed myeloid-associated (CD11b, CD13) surface antigens, further supporting the diagnosis of AML. However, blasts from every patient coexpressed the T-cell-associated surface CD2 and CD7 as well as cytoplasmic CD3 antigens. Blasts from five patients expressed surface CD25, whereas blasts from only one expressed surface CD3. Five patients had rearranged T-cell receptor beta-chain genes, whereas only three had rearranged T-cell receptor gamma-chain genes. This pattern of lineage-related gene expression appears to define a distinct subtype of AML with T-lymphoid features (CD2+ AML) and could reflect either aberrant gene expression in leukemic blasts or transformation of a pluripotent stem cell having a flexible pattern of gene expression. Clinically, these 10 patients presented at an older age with a higher leukocyte count and a higher frequency of lymphadenopathy than did children whose blast cells were characteristic of myeloid leukemia. Patients with CD2+ AML also had poorer responses to remission induction therapy (50% v 80% entered complete remission, P = .05). However, each of the five children who failed induction chemotherapy on AML protocols had a striking response to drug combinations usually reserved for lymphoid leukemia. We conclude that this leukemia with mixed lymphoid and myeloid characteristics is a distinct biologic and clinical entity.

摘要

我们研究了10例急性白血病的临床和生物学特征,这些病例符合法国 - 美国 - 英国(FAB)急性髓系白血病(AML)的标准,但原始细胞也表达T细胞相关的CD2表面抗原。所有病例的髓过氧化物酶和苏丹黑B阳性白血病原始细胞均超过3%,7例病例的原始细胞含有Auer小体。一组单克隆抗体(MAb)与细胞的反应表明,所有病例中的白血病细胞均表达髓系相关(CD11b、CD13)表面抗原,进一步支持AML的诊断。然而,每位患者的原始细胞均共表达T细胞相关表面CD2和CD7以及细胞质CD3抗原。5例患者的原始细胞表达表面CD25,而只有1例患者的原始细胞表达表面CD3。5例患者的T细胞受体β链基因发生重排,而只有3例患者的T细胞受体γ链基因发生重排。这种谱系相关基因表达模式似乎定义了一种具有T淋巴细胞特征的AML独特亚型(CD2 + AML),可能反映白血病原始细胞中的异常基因表达或具有灵活基因表达模式的多能干细胞的转化。临床上,与原始细胞具有髓系白血病特征的儿童相比,这10例患者就诊时年龄较大,白细胞计数较高,淋巴结病发生率较高。CD2 + AML患者对缓解诱导治疗的反应也较差(50%对80%进入完全缓解,P = 0.05)。然而,在AML方案诱导化疗失败的5名儿童中,每一名对通常用于淋巴白血病的联合药物都有显著反应。我们得出结论,这种具有混合淋巴和髓系特征的白血病是一种独特的生物学和临床实体。

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