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髓系表面抗原阳性急性淋巴细胞白血病(My+ ALL):免疫表型、超微结构、细胞遗传学及分子特征

Myeloid surface antigen-positive acute lymphoblastic leukemia (My+ ALL): immunophenotypic, ultrastructural, cytogenetic, and molecular characteristics.

作者信息

Childs C C, Hirsch-Ginsberg C, Walters R S, Andersson B S, Reuben J, Trujillo J M, Cork A, Stass S A, Freireich E J, Zipf T F

机构信息

Division of Laboratory Medicine, University of Texas M. D. Anderson Cancer Center, Houston 77030.

出版信息

Leukemia. 1989 Nov;3(11):777-83.

PMID:2811478
Abstract

Leukemic blasts from 40 consecutively admitted adults with untreated acute lymphoblastic leukemia (ALL) were examined for myeloid surface antigen expression. Of these, 14 (35%) were reactive with one or more myeloid monoclonal antibodies. Each example of myeloid surface antigen-positive (My+ ALL) met the standard morphologic and cytochemical criteria for ALL. In addition, none of the 13 samples studied for ultrastructural evidence of myeloperoxidase met the criteria for acute myelocytic leukemia (AML). All patient samples reacted with lymphoid monoclonal antibodies: CD10+ (8 patients), CD19+ CD10- (2 patients), T cell+ (2 patients), and T cell+ CD10+ (2 patients). Coexpression of myeloid and lymphoid determinants was established by two-color immunofluorescence studies using flow cytometry in five of five samples analyzed. Cytogenetic abnormalities that have been associated with myeloid and mixed leukemias were common, including t(9;22), 7q-, abnormalities of 11q with or without a translocation, 20q-, and -5. Blasts from seven patients were studied at the molecular level. Immunoglobulin heavy chain gene rearrangements were detected in five of five samples with B cell+ T cell- phenotypes. One sample that was T cell+ CD10+ was germline for the immunoglobulin heavy chain and the T cell receptor gamma- and beta-chain genes. The other patient with T cell+ CD10+ blasts relapsed with AML following allogeneic bone marrow transplantation. The leukemia cells at the time of diagnosis and the cells at relapse demonstrated similar cytogenetics and the same immunoglobulin gene rearrangement, suggesting a clonal relationship. As a group, the My+ ALL patients had a significantly decreased complete remission rate when compared to My- ALL patients. Further studies at the molecular level will be required to determine the significance of karyotype abnormalities in My+ ALL.

摘要

对40例连续收治的未经治疗的成人急性淋巴细胞白血病(ALL)患者的白血病原始细胞进行了髓系表面抗原表达检测。其中,14例(35%)与一种或多种髓系单克隆抗体发生反应。每个髓系表面抗原阳性(My+ ALL)病例均符合ALL的标准形态学和细胞化学标准。此外,对13个样本进行髓过氧化物酶超微结构证据研究,无一符合急性髓细胞白血病(AML)标准。所有患者样本均与淋巴系单克隆抗体发生反应:CD10+(8例)、CD19+ CD10-(2例)、T细胞+(2例)和T细胞+ CD10+(2例)。通过流式细胞术进行双色免疫荧光研究,在分析的5个样本中的5个样本中确定了髓系和淋巴系决定簇的共表达。与髓系和混合性白血病相关的细胞遗传学异常很常见,包括t(9;22)、7q-、11q异常(有或无易位)、20q-和-5。对7例患者的原始细胞进行了分子水平研究。在5个具有B细胞+ T细胞-表型的样本中,5个样本检测到免疫球蛋白重链基因重排。1个T细胞+ CD10+样本的免疫球蛋白重链以及T细胞受体γ链和β链基因均为种系。另1例T细胞+ CD10+原始细胞患者在异基因骨髓移植后复发为AML。诊断时的白血病细胞和复发时的细胞显示出相似的细胞遗传学和相同的免疫球蛋白基因重排,提示存在克隆关系。总体而言,与My- ALL患者相比,My+ ALL患者的完全缓解率显著降低。需要在分子水平进行进一步研究,以确定My+ ALL中核型异常的意义。

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