Papas T S, Watson D K, Sacchi N, Fujiwara S, Seth A K, Fisher R J, Bhat N K, Mavrothalassitis G, Koizumi S, Jorcyk C L
Laboratory of Molecular Oncology, National Cancer Institute, Frederick, Maryland 21701-1013.
Am J Med Genet Suppl. 1990;7:251-61. doi: 10.1002/ajmg.1320370751.
The human ETS2 and ERG genes are members of the ETS gene family, with sequence homology to the viral ets gene of the avian erythroblastosis retrovirus, E26. These genes are located on chromosome 21 and molecular genetic analysis of Down syndrome (DS) patients with partial trisomy 21 suggested that ETS2 may be a gene within the minimal DS genetic region. We have, in fact, been able to confirm the presence of the ETS2 gene dosage in triplicate occurring in occult human 21 chromosome abnormalities. It is known that ERG and ETS2 gene translocations occur in certain specific leukemias associated with defined chromosome rearrangements [e.g., t(8;21)]. Moreover, it is known that DS individuals are at greater risk for leukemic disease than their normal familial cohorts, implying that trisomy of that region of human chromosome 21 may play a role in the development of this type of neoplasia. The human ETS genes, first identified in our laboratory, are highly conserved, being found from lower organisms, like Drosophila and sea urchin, to humans. In mammals, the ETS genes are structurally distinct, located on separate chromosomes; they are transcriptionally active and differentially regulated. The ETS2 protein is phosphorylated and turns over with a half-life of approximately 20 min. After activation with the tumor promoter, TPA, the level of ETS2 elevates 5- to 20-fold. The properties of the ETS2 protein, such as nuclear localization, phosphorylation, rapid turnover, and response to protein kinase C, indicate that this protein belongs to a group of oncogene proteins thought to have regulatory functions in the nucleus. In the mouse thymus ets-1 and ets-2 are 8-10-fold higher, respectively, in the CD4+ subset than in other subsets examined, suggesting a role in T-cell development for these genes. Cells transfected with the cellular ets-2 gene, expressing higher levels of ets-2 products, showed a stimulated proliferation response, abolished their serum requirement and formed colonies in soft agar that could induce tumors in nude mice. Collectively, these data suggest that this family of genes might play a role in controlling specific steps of the signaling transduction pathway. Thus, the ETS genes, as other genes with homology to viral oncogenes, might be instrumental in regulating cellular growth and differentiation, as well as organismal development.
人类ETS2和ERG基因是ETS基因家族的成员,与禽成红细胞增多症逆转录病毒E26的病毒ets基因具有序列同源性。这些基因位于21号染色体上,对部分21三体唐氏综合征(DS)患者的分子遗传学分析表明,ETS2可能是最小DS遗传区域内的一个基因。事实上,我们已经能够证实在隐匿性人类21号染色体异常中存在三倍体的ETS2基因剂量。已知ERG和ETS2基因易位发生在某些与特定染色体重排相关的特定白血病中[例如,t(8;21)]。此外,已知DS个体患白血病的风险高于其正常家族人群,这意味着人类21号染色体该区域的三体性可能在这种肿瘤的发生发展中起作用。人类ETS基因最初是在我们实验室中鉴定出来的,具有高度保守性,从果蝇和海胆等低等生物到人类均有发现。在哺乳动物中,ETS基因在结构上是不同的,位于不同的染色体上;它们具有转录活性且受到差异调节。ETS2蛋白被磷酸化,其半衰期约为20分钟。在用肿瘤启动子佛波酯(TPA)激活后,ETS2的水平升高5至20倍。ETS2蛋白的特性,如核定位、磷酸化、快速周转以及对蛋白激酶C的反应,表明该蛋白属于一类被认为在细胞核中具有调节功能的癌基因蛋白。在小鼠胸腺中,ets-1和ets-2在CD4+亚群中的表达分别比其他检测亚群高8至10倍,表明这些基因在T细胞发育中起作用。用细胞ets-2基因转染的细胞,表达更高水平的ets-2产物,表现出增殖反应受到刺激,不再需要血清,并在软琼脂中形成集落,这些集落在裸鼠中可诱导肿瘤形成。总体而言,这些数据表明该基因家族可能在控制信号转导途径的特定步骤中起作用。因此,ETS基因与其他与病毒癌基因具有同源性的基因一样,可能在调节细胞生长和分化以及生物体发育中发挥作用。
