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MiR-200b/200c/429 subfamily negatively regulates Rho/ROCK signaling pathway to suppress hepatocellular carcinoma metastasis

机译:miR-200b / 200c / 429亚家族负调节Rho / ROCK信号通路抑制肝细胞癌转移

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摘要

MiR-200 family is an important regulator of epithelial-mesenchymal transition and has been implicated in human carcinogenesis. However, their expression and functions in human cancers remain controversial. In the work presented here, we showed that miR-200 family members were frequently down-regulated in hepatocellular carcinoma (HCC). Although all five members of miR-200 family inhibited ZEB1/2 expression in HCC cell lines, we showed that overexpression only of the miR-200b/200c/429 subfamily, but not the miR-200a/141 subfamily, resulted in impeded HCC cell migration. Further investigations led to the identification of RhoA and ROCK2 as specific down-stream targets of the miR-200b/200c/429 subfamily. We demonstrated that the miR-200b/200c/429 subfamily inhibited HCC cell migration through modulating Rho/ROCK mediated cell cytoskeletal reorganization and cell-substratum adhesion. Re-expression of miR-200b significantly suppressed lung metastasis of HCC cells in an orthotopic liver implantation model in vivo. In conclusion, our findings identified the miR-200b/200c/429 subfamily as metastasis suppressor microRNAs in human HCC and highlighted the functional discrepancy among miR-200 family members.
机译:MiR-200家族是上皮-间质转化的重要调节剂,并已参与人类致癌作用。然而,它们在人类癌症中的表达和功能仍存在争议。在本文介绍的工作中,我们表明miR-200家族成员在肝细胞癌(HCC)中经常被下调。尽管miR-200家族的所有五个成员均抑制了HCC细胞系中的ZEB1 / 2表达,但我们显示仅miR-200b / 200c / 429亚家族而不是miR-200a / 141亚家族的过表达导致了HCC细胞受损移民。进一步的研究导致将RhoA和ROCK2鉴定为miR-200b / 200c / 429亚家族的特定下游靶标。我们证明了miR-200b / 200c / 429亚家族可通过调节Rho / ROCK介导的细胞骨架重组和细胞基质粘附来抑制HCC细胞迁移。在体内原位肝移植模型中,miR-200b的重新表达显着抑制了HCC细胞的肺转移。总之,我们的发现将miR-200b / 200c / 429亚家族确定为人类HCC中的转移抑制microRNA,并突显了miR-200家族成员之间的功能差异。

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