Fest Thierry, Mougey Virginie, Dalstein Véronique, Hagerty Marlon, Milette Danielle, Silva Santiago, Mai Sabine
Hematology Department, University Hospital Jean Minjoz, 20539 Besançon Cedex, France.
Oncogene. 2002 May 2;21(19):2981-90. doi: 10.1038/sj.onc.1205274.
Overexpression of c-Myc in tumors is usually associated with cell proliferation and increased susceptibility to apoptosis. Concomitantly, c-Myc contributes to tumorigenesis by its ability to destabilize the cellular genome. Here, we examined whether c-Myc induces genomic instability and apoptosis in c-Myc-activated cells. Wild-type Myc (wt-Myc) and two mutated Myc myc box II proteins (mt-Myc) were overexpressed in IL3-dependent murine Ba/F3 cells. As expected, wt-Myc triggered apoptosis in absence of IL3. Standard karyotyping, spectral karyotyping, and fluorescent in situ hybridization (FISH) were performed before and after c-Myc activation. Structural and numerical genomic instability was detected 48 h after wt-Myc activation and included gene amplification, the formation of extrachromosomal elements (EEs), chromosome breakage, deletions, increased aneuploidy, and polyploidization. Interestingly, some cells simultaneously displayed genomic instability and apoptosis. Both wt- and mt-Myc proteins were equally potent promoters of genomic instability. However, only wt-Myc simultaneously induced genomic instability and apoptosis. Mt-Myc proteins failed to induce apoptosis, thereby generating a strong imbalance towards the survival of genomically unstable cells.
肿瘤中c-Myc的过表达通常与细胞增殖以及对凋亡的易感性增加相关。同时,c-Myc通过其破坏细胞基因组稳定性的能力促进肿瘤发生。在此,我们研究了c-Myc是否在c-Myc激活的细胞中诱导基因组不稳定和凋亡。野生型Myc(wt-Myc)和两种突变的Myc myc盒II蛋白(mt-Myc)在依赖IL3的小鼠Ba/F3细胞中过表达。如预期的那样,wt-Myc在无IL3的情况下触发凋亡。在c-Myc激活前后进行了标准核型分析、光谱核型分析和荧光原位杂交(FISH)。在wt-Myc激活48小时后检测到结构和数量基因组不稳定,包括基因扩增、染色体外元件(EEs)的形成、染色体断裂、缺失、非整倍性增加和多倍体化。有趣的是,一些细胞同时表现出基因组不稳定和凋亡。wt-Myc和mt-Myc蛋白都是基因组不稳定的同等强效促进剂。然而,只有wt-Myc同时诱导基因组不稳定和凋亡。Mt-Myc蛋白未能诱导凋亡,从而导致基因组不稳定细胞的存活出现强烈失衡。