表观遗传重编程调节人类肝癌的恶性特性。
Epigenetic reprogramming modulates malignant properties of human liver cancer.
作者信息
Raggi Chiara, Factor Valentina M, Seo Daekwan, Holczbauer Agnes, Gillen Matthew C, Marquardt Jens U, Andersen Jesper B, Durkin Marian, Thorgeirsson Snorri S
机构信息
Laboratory of Experimental Carcinogenesis, Center for Cancer Research, National Cancer Institute, NIH, Bethesda, MD.
出版信息
Hepatology. 2014 Jun;59(6):2251-62. doi: 10.1002/hep.27026. Epub 2014 May 1.
UNLABELLED
Reversal of DNA hypermethylation and associated gene silencing is an emerging cancer therapy approach. Here we addressed the impact of epigenetic alterations and cellular context on functional and transcriptional reprogramming of hepatocellular carcinoma (HCC) cells. Our strategy employed a 3-day treatment of established and primary human HCC-derived cell lines grown as a monolayer at various cell densities with the DNMT1 inhibitor zebularine (ZEB) followed by a 3D culture to identify cells endowed with self-renewal potential. Differences in self-renewal, gene expression, tumorigenicity, and metastatic potential of spheres at generations G1-G5 were examined. Transient ZEB exposure produced differential cell density-dependent responses. In cells grown at low density, ZEB caused a remarkable increase in self-renewal and tumorigenicity associated with long-lasting gene expression changes characterized by a stable overexpression of cancer stem cell-related and key epithelial-mesenchymal transition genes. These effects persisted after restoration of DNMT1 expression. In contrast, at high cell density, ZEB caused a gradual decrease in self-renewal and tumorigenicty, and up-regulation of apoptosis- and differentiation-related genes. A permanent reduction of DNMT1 protein using short hairpin RNA (shRNA)-mediated DNMT1 silencing rendered HCC cells insensitive both to cell density and ZEB effects. Similarly, WRL68 and HepG2 hepatoblastoma cells expressing low DNMT1 basal levels also possessed a high self-renewal, irrespective of cell density or ZEB exposure. Spheres formed by low-density cells treated with ZEB or shDNMT1 displayed a high molecular similarity which was sustained through consecutive generations, confirming the essential role of DNMT1 depletion in the enhancement of cancer stem cell properties.
CONCLUSION
These results identify DNA methylation as a key epigenetic regulatory mechanism determining the pool of cancer stem cells in liver cancer and possibly other solid tumors.
未标记
DNA 高甲基化的逆转及相关基因沉默是一种新兴的癌症治疗方法。在此,我们探讨了表观遗传改变和细胞环境对肝细胞癌(HCC)细胞功能和转录重编程的影响。我们的策略是用 DNA 甲基转移酶 1(DNMT1)抑制剂泽布勒林(ZEB)对以单层形式在不同细胞密度下培养的已建立的和原发性人 HCC 衍生细胞系进行为期 3 天的处理,随后进行三维培养,以鉴定具有自我更新潜力的细胞。检测了第 G1 - G5 代球体在自我更新、基因表达、致瘤性和转移潜力方面的差异。短暂暴露于 ZEB 产生了不同的细胞密度依赖性反应。在低密度培养的细胞中,ZEB 导致自我更新和致瘤性显著增加,伴有持久的基因表达变化,其特征为癌症干细胞相关和关键上皮 - 间质转化基因的稳定过表达。这些效应在 DNMT1 表达恢复后仍然持续。相比之下,在高细胞密度下,ZEB 导致自我更新和致瘤性逐渐降低,以及凋亡和分化相关基因的上调。使用短发夹 RNA(shRNA)介导的 DNMT1 沉默使 DNMT1 蛋白永久性减少,使 HCC 细胞对细胞密度和 ZEB 效应均不敏感。同样,基础 DNMT1 水平低的 WRL68 和 HepG2 肝母细胞瘤细胞也具有高自我更新能力,无论细胞密度或 ZEB 暴露情况如何。用 ZEB 或 shDNMT1 处理的低密度细胞形成的球体显示出高度的分子相似性,并在连续几代中持续存在,证实了 DNMT1 缺失在增强癌症干细胞特性中的关键作用。
结论
这些结果表明 DNA 甲基化是决定肝癌及可能其他实体瘤中癌症干细胞库的关键表观遗传调控机制。
Zotero 插件