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Let-7c inhibits cholangiocarcinoma growth but promotes tumor cell invasion and growth at extrahepatic sites

机译:Let-7c抑制胆管癌的生长,但促进肿瘤细胞在肝外部位的侵袭和生长

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Cholangiocarcinoma (CCA) is a cancer type with high postoperative relapse rates and poor long-term survival largely due to tumor invasion, distant metastasis, and multidrug resistance. Deregulated microRNAs (miRNAs) are implicated in several cancer types including CCA. The specific roles of the miRNA let-7c in cholangiocarcinoma are not known and need to be further elucidated. In our translational study we show that microRNA let-7c expression was significantly downregulated in human cholangiocarcinoma tissues when compared to adjacent tissues of the same patient. Let-7c inhibited the tumorigenic properties of cholangiocarcinoma cells including their self-renewal capacity and sphere formation in vitro and subcutaneous cancer cell growth in vivo. Ectopic let-7c overexpression suppressed migration and invasion capacities of cholangiocarcinoma cell lines in vitro, however, promoted distant invasiveness in vivo. Furthermore, we found that let-7c regulated the aforementioned malignant biological properties, at least in part, through regulation of EZH2 protein expression and through the DVL3/β-catenin axis. The miRNA let-7c thus plays an important dual role in regulating tumorigenic and metastatic abilities of human cholangiocarcinoma through mechanisms involving EZH2 protein and the DVL3/β-catenin axis.
机译:胆管癌(CCA)是一种术后复发率高且长期生存率较低的癌症,主要归因于肿瘤的浸润,远处转移和多药耐药性。失调的microRNA(miRNA)与包括CCA在内的几种癌症类型有关。 miRNA let-7c在胆管癌中的具体作用尚不清楚,需要进一步阐明。在我们的转化研究中,我们发现与相同患者的相邻组织相比,microRNA let-7c表达在人胆管癌组织中显着下调。 Let-7c抑制胆管癌细胞的致癌特性,包括其自我更新能力和体外球形成以及体内皮下癌细胞的生长。异位let-7c的过表达抑制了胆管癌细胞在体外的迁移和侵袭能力,但是,促进了体内的远处侵袭。此外,我们发现let-7c至少部分通过调节EZH2蛋白表达和通过DVL3 /β-catenin轴调节上述恶性生物学特性。因此,miRNA let-7c通过涉及EZH2蛋白和DVL3 /β-catenin轴的机制在调节人胆管癌的致癌和转移能力中起着重要的双重作用。

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