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首页> 外文期刊>Biochemical and Biophysical Research Communications >ZFR promotes cell proliferation and tumor development in colorectal and liver cancers
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ZFR promotes cell proliferation and tumor development in colorectal and liver cancers

机译:ZFR在结肠直肠和肝癌中促进细胞增殖和肿瘤发育

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Colorectal cancer (CRC) and liver cancer are the second and fourth leading causes of cancer-related deaths in the whole world, respectively, and each year over 1.6 million people die from these diseases. To identify driver genes in CRC and liver cancer, we have performed Sleeping Beauty transposon mutagenesis screens in mouse models. Zinc finger RNA binding protein, ZFR, was one of the novel candidate cancer genes identified in these forward genetic screens. Consistent with this discovery, a pan-cancer analysis of sequencing results of thousands of human cancer genomes demonstrated that ZFR is a potential potent oncogene. In this study, we aimed to investigate ZFR's roles in both types of cancer and found that overexpression of ZFR in CRC and liver cancer cells led to accelerated tumor development. Consistently, knockdown of ZFR resulted in significantly decelerated tumor development. ZFR over-expression also promoted tumor development of immortalized mouse liver cells. ZFR overexpression and shRNA knockdown led to accelerated and decelerated cell proliferation, respectively, indicating that ZFR promotes tumor development mainly by regulating cell proliferation.
机译:结肠直肠癌(CRC)和肝癌分别是全世界癌症相关死亡的第二和第四个主要原因,每年有超过160万人死于这些疾病。为了鉴定CRC和肝癌中的司机基因,我们在小鼠模型中进行了睡眠美容转座子诱变屏幕。锌指RNA结合蛋白,ZFR是在这些前向遗传筛网中鉴定的新型候选癌症基因之一。与此发现一致,持续数千人癌症基因组的测序结果的泛癌分析证明ZFR是潜在的强化癌基因。在这项研究中,我们旨在调查ZFR在两种癌症中的作用,发现ZFR在CRC和肝癌细胞中过表达导致肿瘤发育加速。始终如一地,ZFR的敲低产生了显着减速的肿瘤发育。 ZFR过表达还促进了永生化小鼠肝细胞的肿瘤发育。 ZFR过表达和ShRNA敲低导致加速和减速的细胞增殖,表明ZFR主要通过调节细胞增殖来促进肿瘤发育。

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