首页> 外文期刊>Molecular cancer research: MCR >DNA damage-inducible gene, Reprimo functions as a tumor suppressor and is suppressed by promoter methylation in gastric cancer
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DNA damage-inducible gene, Reprimo functions as a tumor suppressor and is suppressed by promoter methylation in gastric cancer

机译:DNA损伤诱导基因Reprimo发挥抑癌作用,在胃癌中被启动子甲基化抑制

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In several types of human cancer, the gene expression of Reprimo, a highly glycosylated protein, is frequently silenced via methylation of its promoter. The aim of this study was to characterize the epigenetic inactivation of Reprimo and its biologic function and clinical relevance in gastric cancer. The correlation between Reprimo methylation and clinical relevance was assessed in 83 primary human gastric cancer tissues. The effects of Reprimo expression were also examined using in vitro and in vivo assays. Reprimo methylation was cancer specific and frequently observed. In two gastric cancer cell lines without Reprimo methylation, we observed faint or weak Reprimo expression under normal conditions and high expression under DNA-damaging conditions. In four gastric cancer cell lines with Reprimo methylation, however, Reprimo expression remained faint even under DNA-damaging conditions, with expression being restored in combination with agents that induce demethylation. Enforced Reprimo expression robustly inhibited cell proliferation and anchorage-independent colony formation and enhanced DNA damage-induced apoptosis. Inverse effects were observed via siRNA-mediated knockdown of endogenous Reprimo. Reprimo expression inhibited tumorigenesis in vivo. Reprimo methylation was also associated with a poor response in patients with gastric cancer treated with chemotherapy (P 1/4 0.028), and a poor prognosis in patients with advanced gastric cancer (P1/4 0.03). In conclusion, Reprimo expression is normally induced in response to DNA damage, acting as a novel tumor suppressor in gastric cancer. However, Reprimo methylation abrogates its expression and effects. The clinical assessment of Reprimo promoter methylation may serve not only as a predictive marker for chemotherapy, but also as a marker for tumor aggressiveness.
机译:在几种类型的人类癌症中,高度糖基化的蛋白质Reprimo的基因表达经常通过其启动子的甲基化而沉默。这项研究的目的是表征胃癌中Reprimo的表观遗传失活及其生物学功能和临床意义。在83种原发性人胃癌组织中评估了Reprimo甲基化与临床相关性之间的相关性。还使用体外和体内试验检查了Reprimo表达的影响。 Reprimo甲基化是癌症特有的,经常观察到。在两种没有Reprimo甲基化的胃癌细胞系中,我们观察到正常条件下Reprimo表达微弱或弱,而DNA损伤条件下Reprimo表达高。然而,在四种具有Reprimo甲基化的胃癌细胞系中,即使在DNA破坏的条件下,Reprimo的表达仍保持微弱,与诱导去甲基化的药物结合后,表达恢复。增强的Reprimo表达可强烈抑制细胞增殖和不依赖锚定的菌落形成,并增强DNA损伤诱导的细胞凋亡。通过内源性Reprimo的siRNA介导的敲低观察到了相反的作用。 Reprimo表达抑制体内肿瘤发生。 Reprimo甲基化还与化疗治疗的胃癌患者不良反应有关(P 1/4 0.028),而晚期胃癌患者预后不良(P1 / 4 0.03)。总之,Reprimo表达通常是对DNA损伤的反应而诱导的,可作为胃癌中的新型肿瘤抑制物。但是,Reprimo甲基化消除了它的表达和作用。 Reprimo启动子甲基化的临床评估不仅可以作为化学疗法的预测指标,而且可以作为肿瘤侵袭性的指标。

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