Dysregulation of p53-RBM25-mediated circAMOTL1L biogenesis contributes to prostate cancer progression through the circAMOTL1L-miR-193a-5p-Pcdha pathway

Zhan Yang,Long Ma,Jin-Suo Chen,Wei Li,Yong Zhang,Chang-Bao Qu,Dan-Dan Wang,Xiao-Lu Wang,Kai-Long Liu,Jin-Kun Wen,Bin Zheng,Man-Li Zhang,Xin-Hua Zhang,Wen-Feng Zhang,Chun-Cheng Gao

doi:10.1038/s41388-018-0602-8

Zhan Yang, Long Ma + Show 13 more

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https://doi.org/10.1038/s41388-018-0602-8

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p53, circRNAs and miRNAs are important components of the regulatory network that activates the EMT program in cancer metastasis. In prostate cancer (PCa), however, it has not been investigated whether and how p53 regulates EMT by circRNAs and miRNAs. Here we show that a Amotl1-derived circRNA, termed circAMOTL1L, is downregulated in human PCa, and that decreased circAMOTL1L facilitates PCa cell migration and invasion through downregulating E-cadherin and upregulating vimentin, thus leading to EMT and PCa progression. Mechanistically, we demonstrate that circAMOTL1L serves as a sponge for binding miR-193a-5p in PCa cells, relieving miR-193a-5p repression of Pcdha gene cluster (a subset of the cadherin superfamily members). Accordingly, dysregulation of the circAMOTL1L-miR-193a-5p-Pcdha8 regulatory pathway mediated by circAMOTL1L downregulation contributes to PCa growth in vivo. Further, we show that RBM25 binds directly to circAMOTL1L and induces its biogenesis, whereas p53 regulates EMT via direct activation of RBM25 gene. These findings have linked p53/RBM25-mediated circAMOTL1L-miR-193a-5p-Pcdha regulatory axis to EMT in metastatic progression of PCa. Targeting this newly identified regulatory axis provides a potential therapeutic strategy for aggressive PCa.

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Prostate cancer (PCa) is one of the most common carcinoma among men worldwide
Some research has revealed that clustered Pcdhs are mainly expressed in nervous system and play critical roles in neurodevelopment [8, 9], a member of this superfamily, PCDHGC3, is highly expressed in normal colonic epithelium, while its expression is suppressed in carcinoma cell lines [10], and PCDH10 is downregulated in gastric cancer cell lines [11], suggesting that Pcdhs may act as tumor suppressors through influencing tumor growth and metastasis
Our findings demonstrate that circAMOTL1L contributes to epithelial–mesenchymal transition (EMT) via regulation of E-Cadherin, vimentin and β-catenin in PCa cell lines

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Prostate cancer (PCa) is one of the most common carcinoma among men worldwide. Organ-confined PCa can be effectively treated via radical prostatectomy [1]. For advanced PCa, androgen deprivation therapy (ADT) is. These authors contributed : Zhan Yang, Chang-Bao Qu, Yong Zhang. Clustered protocadherin-α (Pcdha, 14 isoforms) belongs to a subset of the cadherin superfamily, a group of cell adhesion molecules. They share significant sequence homology with classic cadherins in their extracellular domain and mediate both hemophilic and heterophilic cell-cell adhesion [6, 7]. Recent studies have revealed multiple roles for the Pcdhs in the context of tumor biology, we still know relatively little about how the expression of EMT-related proteins, including Pcdha, is regulated in PCa growth and metastasis

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