Suto Y, Sato Y, Smith S D, Rowley J D, Bohlander S K
Department of Medicine, The University of Chicago, Illinois, USA.
Genes Chromosomes Cancer. 1997 Apr;18(4):254-68. doi: 10.1002/(sici)1098-2264(199704)18:4<254::aid-gcc3>3.0.co;2-#.
ETV6 (TEL) is rearranged in various types of hematologic malignancies. The B-cell precursor acute lymphoblastic leukemia (ALL) cell line SUP-B2 has a t(6;12)(q23;p13) involving ETV6 at 12p13 and a submicroscopic deletion of the other ETV6 allele. The reciprocal translocation results in the fusion of ETV6 to a previously unknown gene at 6q23, which we named STL (six-twelve leukemia gene). Both reciprocal fusion transcripts can be detected: On the der(6) chromosome, the ETV6/STL mRNA shows an apparently out of frame fusion of ETV6 at nucleotide 187 to STL, which would result in the addition of 14 amino acids to the first 54 amino acids of ETV6. On the der(12) chromosome three different variants of the STL/ETV6 fusion mRNA could be detected; variable size segments were inserted at the breakpoint between STL and ETV6 exon 3. One of these variants could give rise to a protein in which the first 54 amino acids of ETV6 are replaced by 12 amino acids from one of the STL short open reading frames. Sequence analysis of a 1.4 kb STL cDNA clone from a skeletal muscle library revealed no long open reading frames. This cell line will be very useful in studying the different mechanisms by which alterations of ETV6 contribute to leukemogenesis and in testing the hypothesis that ETV6 might act as a tumor suppressor gene.
ETV6(TEL)在多种血液系统恶性肿瘤中发生重排。B细胞前体急性淋巴细胞白血病(ALL)细胞系SUP - B2存在t(6;12)(q23;p13),涉及12p13处的ETV6以及另一个ETV6等位基因的亚显微缺失。相互易位导致ETV6与6q23处一个先前未知的基因融合,我们将其命名为STL(6;12白血病基因)。两种相互融合转录本均可检测到:在der(6)染色体上,ETV6/STL mRNA显示ETV6在核苷酸187处与STL明显的移码融合,这将导致在ETV6的前54个氨基酸上添加14个氨基酸。在der(12)染色体上可检测到STL/ETV6融合mRNA的三种不同变体;可变大小的片段插入在STL与ETV6外显子3之间的断点处。这些变体之一可产生一种蛋白质,其中ETV6的前54个氨基酸被来自STL短开放阅读框之一的12个氨基酸所取代。对来自骨骼肌文库的1.4 kb STL cDNA克隆进行序列分析未发现长开放阅读框。该细胞系对于研究ETV6改变促进白血病发生的不同机制以及检验ETV6可能作为肿瘤抑制基因的假说将非常有用。
