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Oncogene-dependent function of BRG1 in hepatocarcinogenesis

机译:BRG1在肝癌发生中的癌基因依赖性功能

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Hepatocellular carcinoma (HCC) is the major type of primary liver cancer. Genomic studies have revealed that HCC is a heterogeneous disease with multiple subtypes. BRG1, encoded by the SMARCA4 gene, is a key component of SWI/SNF chromatin-remodeling complexes. Based on TCGA studies, somatic mutations of SMARCA4 occur in ~3% of human HCC samples. Additional studies suggest that BRG1 is overexpressed in human HCC specimens and may promote HCC growth and invasion. However, the precise functional roles of BRG1 in HCC remain poorly delineated. Here, we analyzed BRG1 in human HCC samples as well as in mouse models. We found that BRG1 is overexpressed in most of human HCC samples, especially in those associated with poorer prognosis. BRG1 expression levels positively correlate with cell cycle and negatively with metabolic pathways in the Cancer Genome Atlas (TCGA) human HCC data set. In a murine HCC model induced by c-MYC overexpression, ablation of the Brg1 gene completely repressed HCC formation. In striking contrast, however, we discovered that concomitant deletion of Brg1 and overexpression of c-Met or mutant NRas (NRASV12) triggered HCC formation in mice. Altogether, the present data indicate that BRG1 possesses both oncogenic and tumor-suppressing roles depending on the oncogenic stimuli during hepatocarcinogenesis.
机译:肝细胞癌(HCC)是主要肝癌的主要类型。基因组研究表明,HCC是具有多种亚型的异质疾病。由SMARCA4基因编码的BRG1是SWI / SNF染色质重塑复合物的关键组分。基于TCGA研究,SMARCA4的体细胞突变发生在〜3%的人HCC样品中。额外的研究表明BRG1在人类HCC标本中过表达,并可促进HCC生长和入侵。然而,BRG1在HCC中的精确功能作用仍然缺乏差。在这里,我们分析了人类HCC样本以及小鼠模型中的BRG1。我们发现BRG1在大多数人HCC样品中过表达,特别是在与预后较差的人中。 BRG1表达水平与细胞周期呈正相关,对癌症基因组Atlas(TCGA)人HCC数据集的代谢途径负相关。在由C-MYC过表达诱导的鼠HCC模型中,消融BRG1基因完全被压抑的HCC形成。然而,在引人注目的对比中,我们发现伴随BRG1和突变NRAS(NRASV12)的过表达在小鼠中触发HCC形成。总之,本数据表明BRG1根据肝癌发生期间的致癌刺激具有致癌和肿瘤抑制的作用。

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