MiR-204 down-regulation elicited perturbation of a gene target signature common to human cholangiocarcinoma and gastric cancer

MiR-204 下调引起人类胆管癌和胃癌共有的基因靶标特征的扰动

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作者：Valeria Canu, Andrea Sacconi, Laura Lorenzon, Francesca Biagioni, Federica Lo Sardo, Maria Grazia Diodoro, Paola Muti, Alfredo Garofalo, Sabrina Strano, Antonietta D'Errico, Gian Luca Grazi, Mario Cioce, Giovanni Blandino

期刊：

Oncotarget

影响因子：

时间：

2017

起止号：

2017 May 2;8(18):29540-29557.

doi：

10.18632/oncotarget.15290

研究方向：

肿瘤

疾病类型：

胃癌、胆管癌

Aims

There is high need of novel diagnostic and prognostic tools for tumors of the digestive system, such as gastric cancer and cholangiocarcinoma. We recently found that miR-204 was deeply downregulated in gastric cancer tissues. Here we investigated whether this was common to other tumors of the digestive system and whether this elicited a miR-204-dependent gene target signature, diagnostically and therapeutically relevant. Finally, we assessed the contribution of the identified target genes to the cell cycle progression and clonogenicity of gastric cancer and cholangiocarcinoma cell lines.

Background & aims

Conclusions

We suggest that restoring the physiological levels of miR-204 in some gastrointestinal cancers might be exploited therapeutically.

Methods

We employed quantitative PCR and Affymetrix profiling for gene expression studies. In silico analysis aided us to identifying a miR-204 target signature in publicly available databases (TGCA). We employed transient transfection experiments, clonogenic assays and cell cycle profiling to evaluate the biological consequences of miR-204 perturbation.

Results

We identified a novel miR-204 gene target signature perturbed in gastric cancer and in cholangiocarcinoma specimens. We validated its prognostic relevance and mechanistically addressed its biological relevance in GC and CC cell lines. Conclusions: We suggest that restoring the physiological levels of miR-204 in some gastrointestinal cancers might be exploited therapeutically.