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

Yang, Zhan; Qu, Chun-Ying; Zhang, Yong; Zhang, Wenfeng; Wang, Dandan; Gao, Chun-Cheng; Ma, Long; Chen, Jin-Suo; Liu, Kailong; Zheng, Bin; Zhang, Xinhua; Zhang, Manli; Wang, Xiaolu; Wen, Jin‐Kun; Li, Wei

doi:10.1038/s41388-018-0602-8

Cited by 143 publications

(174 citation statements)

References 54 publications

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“…Recent studies have shown that circRNA functions through different actions, including serving as ‘miRNA sponge’, regulation of transcription and splicing, interacting with RNA‐binding protein, and even translating polypeptide . The most extensively studied is circRNA as a competing endogenous RNA (ceRNA) to effectively sponge miRNA, for example, circ‐HIPK3/miR‐7 in colorectal cancer, circ‐EPSTI1/miR‐942 in ovarian cancer, circ‐ANKS1B/miR‐148/152 in breast cancer and circ‐AMOTL1L/miR‐193a‐5p in prostate cancer . It is well recognized that miRNA is a post‐transcriptional regulator by decreasing mRNA stability or inhibiting translation via directly targeting gene 3′‐UTR .…”

Section: Discussionmentioning

confidence: 99%

“…16 The most extensively studied is circRNA as a competing endogenous RNA (ceRNA) to effectively sponge miRNA, for example, circ-HIPK3/miR-7 in colorectal cancer, 17 circ-EPSTI1/miR-942 in ovarian cancer, 18 circ-ANKS1B/ miR-148/152 in breast cancer 19 and circ-AMOTL1L/miR-193a-5p in prostate cancer. 20 It is well recognized that miRNA is a post-transcriptional regulator by decreasing mRNA stability or inhibiting translation via directly targeting gene 3′-UTR. 21 In the current study, we identified that circ-CCND1 could simultaneously sponge three miR-646 to diminish the repression of miR-646 on CCND1 3′-UTR, resulting in enhancing the stability of CCND1 mRNA.…”

Section: Discussionmentioning

confidence: 99%

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circRNA circ‐CCND1 promotes the proliferation of laryngeal squamous cell carcinoma through elevating CCND1 expression via interacting with HuR and miR‐646

Zang

Wan

et al. 2020

J Cellular Molecular Medi

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Cyclin D1 (CCND1) is a well‐known proliferation promoter that accelerates G1/S transition in cancer. However, the underlying mechanism by which CCND1 is regulated is still largely unknown. In this study, we identified a novel circular RNA (circRNA) derived from CCND1 (circ‐CCND1, hsa_circ_0023303) as a key regulator for CCND1. circ‐CCND1 was found to be markedly up‐regulated in laryngeal squamous cell carcinoma (LSCC) and closely associated with aggressive clinical features and adverse prognosis. Depletion of circ‐CCND1 significantly inhibited LSCC cell proliferation in vitro and retarded tumour growth in vivo. Regarding the mechanism, circ‐CCND1 physically bound to human antigen R (HuR) protein to enhance CCND1 mRNA stability; on the other hand, circ‐CCND1 could act as an effective sponge for miR‐646 to alleviate the repression of miR‐646 on CCND1 mRNA. As a result, circ‐CCND1 post‐transcriptionally elevated CCND1 expression via coordinated avoidance of CCND1 mRNA decay, thereby promoting LSCC tumorigenesis. Taken together, our findings uncover the essential proliferation‐promoting role of circ‐CCND1 through regulation of the stability of CCND1 mRNA in LSCC. Targeting circ‐CCND1 may be a promising treatment for LSCC patients.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

circRNA circ‐CCND1 promotes the proliferation of laryngeal squamous cell carcinoma through elevating CCND1 expression via interacting with HuR and miR‐646

Zang

Wan

et al. 2020

J Cellular Molecular Medi

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“…There have been other similar reports in the study of PCa. Yang et al (2019) demonstrated that circAMOTL1L was a sponge that bound miR‐193a‐5p in PCa cells, alleviating the inhibition of miR‐193a‐5p on the Pcdha gene cluster and thus reducing PCa cell invasion and migration by upregulating vimentin and downregulating E‐cadherin. Chen et al (2019) indicated that circAGO2 plays an oncogenic role and promotes tumour progression by enhancing the inhibitory effect of human antigen R (HuR) on AGO2‐miRNA complexes.…”

Section: Discussionmentioning

confidence: 99%

Extracellular vesicle‐derived circ_SLC19A1 promotes prostate cancer cell growth and invasion through the miR‐497/septin 2 pathway

Zheng

Chen

et al. 2020

Cell Biology International

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The occurrence and development of prostate cancer (PCa) is complex, and the related mechanism is not fully understood. Current studies have found that extracellular vesicles (EVs) and circular RNAs (circRNAs) have important functions in various tumours and other diseases. In this study, the detection of circRNAs in PCa showed that circ_SLC19A1 was increased in PCa cells and their secreted EVs. EVs with high expression of circ_SLC19A1 could be taken up by PCa cells, which promoted cell proliferation and invasion. The sequence of circ_SLC19A1 contained multiple binding sites for miR‐497, and circ_SLC19A1 could bind directly to miR‐497 in cells. The expression of miR‐497 was downregulated in PCa cells, while the expression of its target gene septin 2 (SEPT2) was upregulated significantly. Transfection of circ_SLC19A1 small interfering RNA (siRNA) or miR‐497 mimics could significantly inhibit the expression of SEPT2 and the phosphorylation of extracellular signal‐regulated kinase 1 and 2 (ERK1/2). After co‐transfection of circ_SLC19A1 siRNA and miR‐497 inhibitors or SEPT2 overexpression vector, the expression of SEPT2 and ERK1/2 phosphorylation levels showed no significant changes. Similar results were obtained with co‐transfection of miR‐497 mimics and the SEPT2 overexpression vector. Therefore, cancer cells can regulate the expression of SEPT2 through miR‐497 by secreting EVs with high expression of circ_SLC19A1, thus affecting the activation of the downstream ERK1/2 pathway and ultimately regulating PCa cell growth and invasion. Therefore, EV‐derived circ_SLC19A1 plays an important regulatory role in PCa and may be an important target for PCa prevention and treatment.

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“…While, as described above, linear ANRIL affects p53 stability via ARF [141], circANRIL expression impairs rRNA processing and maturation, ultimately leading to nucleolar stress and p53 activation [170]. The activation of p53 is also affected by other circRNAs, including: i) circ_0000263, which sponges miR-150-5p, in turn causing the up-regulation of the p53 inhibitor MDM4 [171]; ii) circ_0055538, whose loss in oral squamous cell carcinoma attenuates p53's pro-apoptotic response [172]; and iii) circAMOTL1L, whose downregulation promotes prostate cancer progression by impairing the p53dependent regulation of EMT [173]. Despite the numerous reports demonstrating the functional interactions between circRNAs and the p53 pathway (Table 3), further efforts are still needed to show whether circRNAs can also affect the stability or the activity of the remaining members of the p53 family and what consequences this interplay may have in human cancers and other biological processes.…”

Section: Circular Rnas and Their Effects On The P53 Pathwaymentioning

confidence: 99%

“…[171] circ_0055538 tumour suppressor required for p53-dependent apoptosis [172] circAMOTL1L tumour suppressor mediating p53 suppression of EMT [173] circANRIL causes p53 activation via nucleolar stress [170] PINT p53 target encoding a small tumour suppressive peptide [169]…”

Section: Marco Napolimentioning

confidence: 99%

The p53 family reaches the final frontier: the variegated regulation of the dark matter of the genome by the p53 family in cancer

Napoli

Flores

2020

RNA Biology

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The tumour suppressor p53 and its paralogues, p63 and p73, are essential to maintain cellular homoeostasis and the integrity of the cell's genetic material, thus meriting the title of 'guardians of the genome'. The p53 family members are transcription factors and fulfill their activities by controlling the expression of protein-coding and non-coding genes. Here, we review how the latter group transcended from the 'dark matter' of the transcriptome, providing unexpected and intriguing anti-cancer therapeutic strategies. ARTICLE HISTORY

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

Cited by 143 publications

References 54 publications

circRNA circ‐CCND1 promotes the proliferation of laryngeal squamous cell carcinoma through elevating CCND1 expression via interacting with HuR and miR‐646

circRNA circ‐CCND1 promotes the proliferation of laryngeal squamous cell carcinoma through elevating CCND1 expression via interacting with HuR and miR‐646

Extracellular vesicle‐derived circ_SLC19A1 promotes prostate cancer cell growth and invasion through the miR‐497/septin 2 pathway

The p53 family reaches the final frontier: the variegated regulation of the dark matter of the genome by the p53 family in cancer

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