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儿童急性淋巴细胞白血病中的免疫球蛋白/T细胞受体基因同时重排与多克隆性

Simultaneous immunoglobulin/T-cell receptor gene rearrangements and multiclonality in childhood acute lymphoblastic leukemia.

作者信息

Forestier E, Nordenson I, Lindström A, Roos G, Lindh J

机构信息

Department of Pediatrics, University of Umeå, Sweden.

出版信息

Acta Paediatr. 1994 Mar;83(3):319-26. doi: 10.1111/j.1651-2227.1994.tb18104.x.

DOI:10.1111/j.1651-2227.1994.tb18104.x
PMID:8038538
Abstract

Twenty-five children less than 16 years of age with acute lymphoblastic leukemia (ALL) were investigated with immunologic, cytogenetic and molecular genetic techniques at diagnosis. All pre-B-cell ALL showed clonal rearrangements in the immunoglobulin heavy chain gene (JH and/or C mu). A very high proportion of the pre-B-cell leukemias (17 of 23 cases) also showed clonal rearrangements in T-cell receptor genes (T gamma and/or T beta). The two T-cell leukemias exhibited clonal T-cell receptor gene rearrangements and in one JH and kappa light chain rearrangements also. The T-cell receptor gene rearrangements found in pre-B-cell leukemias appeared to occur randomly with respect to the T beta and T gamma genes. A significant proportion of the leukemias (at least 24%) seemed to harbor more than one malignant (sub)clone at diagnosis. Cytogenetic studies revealed a clonal abnormality in 10 cases. Only 2 showed hyperdiploidy (> 50 chromosomes). The only correlation between cytogenetic findings and rearrangement patterns was extra bands corresponding to a possible trisomy of chromosome 14. Our data indicate, in line with previous studies, that childhood ALL has complex rearrangement patterns not useful for lineage sub-classification. For this purpose immunophenotyping appears to be superior. However, molecular analysis can reveal the presence of more than one clone not detected by immunophenotyping or karyotyping, and distribution of clones in different compartments. In this study no correlation with clinical outcome was observed.

摘要

对25名16岁以下的急性淋巴细胞白血病(ALL)患儿在诊断时采用免疫、细胞遗传学和分子遗传学技术进行了研究。所有前B细胞ALL在免疫球蛋白重链基因(JH和/或Cμ)中均显示克隆性重排。很高比例的前B细胞白血病(23例中的17例)在T细胞受体基因(Tγ和/或Tβ)中也显示克隆性重排。两例T细胞白血病表现出克隆性T细胞受体基因重排,其中一例还出现JH和κ轻链重排。在前B细胞白血病中发现的T细胞受体基因重排似乎在Tβ和Tγ基因方面随机发生。很大比例的白血病(至少24%)在诊断时似乎含有不止一个恶性(亚)克隆。细胞遗传学研究在10例中发现了克隆异常。只有2例显示超二倍体(>50条染色体)。细胞遗传学结果与重排模式之间唯一的关联是对应于可能的14号染色体三体的额外条带。我们的数据与先前的研究一致,表明儿童ALL具有复杂的重排模式,对谱系亚分类无用。为此,免疫表型分析似乎更具优势。然而,分子分析可以揭示免疫表型分析或核型分析未检测到的不止一个克隆的存在,以及克隆在不同区室中的分布。在本研究中未观察到与临床结果的相关性。

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