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Downregulation of microRNA miR-520h by E1A contributes to anticancer activity.


ABSTRACT: The leading cause of death in cancer patients is cancer metastasis, for which there is no effective treatment. MicroRNAs (miRNA) have been shown to play a significant role in cancer metastasis through regulation of gene expression. The adenovirus type 5 E1A (E1A) is associated with multiple tumor-suppressing activities including the inhibition of metastasis, and E1A gene therapies have been tested in several clinical trials. However, the mechanisms involved in E1A-mediated tumor-suppressing activities are not yet completely defined. Here, we showed that E1A downregulated the expression of the miRNA miR-520h, which was critical for E1A-mediated cancer cell mobility and in vitro invasion activity. In addition, we identified a signal cascade, namely, E1A-->miRNA-520h-->PP2A/C-->IkappaB kinase-->NF-kappaB-->Twist, in which E1A inhibited the expression of Twist through downregulation of miR-520h and the signal cascade. Our results indicated a functional link between miR-520h and tumorigenicity/invasive ability and provided a new insight into the role of E1A-mediated miRNA regulation in tumor suppression. Therefore, the results identified a new cascade of E1A-mediated tumor suppression activity via downregulation of miRNA-520h expression.

SUBMITTER: Su JL 

PROVIDER: S-EPMC2891368 | biostudies-literature | 2010 Jun

REPOSITORIES: biostudies-literature

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Downregulation of microRNA miR-520h by E1A contributes to anticancer activity.

Su Jen-Liang JL   Chen Poshen B PB   Chen Ya-Huey YH   Chen Shang-Chih SC   Chang Yi-Wen YW   Jan Yi-Hua YH   Cheng Xiaoyun X   Hsiao Michael M   Hung Mien-Chie MC  

Cancer research 20100525 12


The leading cause of death in cancer patients is cancer metastasis, for which there is no effective treatment. MicroRNAs (miRNA) have been shown to play a significant role in cancer metastasis through regulation of gene expression. The adenovirus type 5 E1A (E1A) is associated with multiple tumor-suppressing activities including the inhibition of metastasis, and E1A gene therapies have been tested in several clinical trials. However, the mechanisms involved in E1A-mediated tumor-suppressing acti  ...[more]

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