Shurtleff S A, Buijs A, Behm F G, Rubnitz J E, Raimondi S C, Hancock M L, Chan G C, Pui C H, Grosveld G, Downing J R
Department of Pathology and Laboratory Medicine, St Jude Children's Research Hospital, Memphis, TN, USA.
Leukemia. 1995 Dec;9(12):1985-9.
The t(12;21)(p13;q22) is identified by routine cytogenetics in less than 0.05% of pediatric acute lymphoblastic leukemia (ALL) patients. This translocation encodes a TEL/AML-1 chimeric product comprising the helix-loop-helix domain of TEL, a member of the ETS-like family of transcription factors, fused to AML-1, the DNA-binding subunit of the AML-1/CBF beta transcription factor complex. Both TEL and AML-1 are involved in several myeloid leukemia-associated translocations with AML-1/CBF beta being altered in 20-30% of de novo acute myeloid leukemia (AML) cases. We now demonstrate that a TEL/AML1 chimeric transcript encoded by a cryptic t(12;21) is observed in 22% of pediatric ALL, making it the most common genetic lesion in these patients. Moreover, TEL/AML1 expression defined a distinct subgroup of patients characterized by an age between 1 and 10 years, B lineage immunophenotype, non-hyperdiploid DNA content and an excellent prognosis. These data demonstrate that molecular diagnostic approaches are invaluable in identifying clinically distinct subgroups, and that the AML1/CBF beta transcription complex is the most frequent target of chromosomal rearrangements in human leukemia.
在不到0.05%的小儿急性淋巴细胞白血病(ALL)患者中,通过常规细胞遗传学方法可鉴定出t(12;21)(p13;q22)。这种易位编码一种TEL/AML-1嵌合产物,它由TEL的螺旋-环-螺旋结构域(TEL是ETS样转录因子家族的成员)与AML-1融合而成,AML-1是AML-1/CBFβ转录因子复合物的DNA结合亚基。TEL和AML-1都参与了多种髓系白血病相关的易位,在20%-30%的初发急性髓系白血病(AML)病例中,AML-1/CBFβ会发生改变。我们现在证明,在22%的小儿ALL患者中观察到由隐匿性t(12;21)编码的TEL/AML1嵌合转录本,这使其成为这些患者中最常见的基因病变。此外,TEL/AML1表达定义了一个独特的患者亚组,其特征为年龄在1至10岁之间、B系免疫表型、非超二倍体DNA含量以及预后良好。这些数据表明,分子诊断方法在识别临床上不同的亚组方面具有重要价值,并且AML1/CBFβ转录复合物是人类白血病中染色体重排最常见的靶点。
