FOXD1 is targeted by miR-30a-5p and miR-200a-5p and suppresses the proliferation of human ovarian carcinoma cells by promoting p21 expression in a p53-independent manner

Wang, Yu; Qiu, Chunping; Lü, Nan; Liu, Zhaojian; Jin, Chengjuan; Sun, Ce; Bu, Hualei; Yu, Hongfeng; Dongol, Samina; Kong, Beihua

doi:10.3892/ijo.2018.4359

Cited by 35 publications

(47 citation statements)

References 55 publications

(71 reference statements)

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“…According to previous reports, miR-30a-5p plays a dual role in different types of cancer as either an oncogene or onco-suppressor [28]. Function of miR-30a-5p as cancer activators has been reported in pharyngeal cancer [29], ovarian cancer [30] and glioma [31]. Their expression profiles also differ between cancer and normal tissue.…”

Section: Plos Onementioning

confidence: 97%

Circulating microRNA/isomiRs as novel biomarkers of esophageal squamous cell carcinoma

et al. 2020

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Background MicroRNA (miR)s are promising diagnostic biomarkers of cancer. Recent next generation sequencer (NGS) studies have found that isoforms of micro RNA (isomiR) circulate in the bloodstream similarly to mature micro RNA (miR). We hypothesized that combination of circulating miR and isomiRs detected by NGS are potentially powerful cancer biomarker. The present study aimed to investigate their application in esophageal cancer.

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Section: Plos Onementioning

confidence: 97%

Circulating microRNA/isomiRs as novel biomarkers of esophageal squamous cell carcinoma

et al. 2020

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“…Oncogenic factors, such as miR‐203, miR‐410, and miR‐34a, have been identified as carcinogenic factors that promote proliferation of PCa cells . Notably, miR‐200a, a member of the miR‐200 family, has been shown to participate in several biological processes that regulate the progression of tumors . However, the role of miR‐200a in prostate cancer development and progression has not been investigated.…”

Section: Introductionmentioning

confidence: 99%

MicroRNA‐200a suppresses prostate cancer progression through BRD4/AR signaling pathway

et al. 2019

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Prostate cancer is still considered a significant health care challenge worldwide due in part to the distinct transformation of androgen‐dependent prostate cancer (ADPC) into treatment‐refractory castration‐resistant prostate cancer (CRPC). Consequently, there is an urgent need to explore novel molecular mechanisms underlying treatment resistance in ADPC. Although numerous studies have alluded to the role of miR‐200a in several cancers, the biological significance of miR‐200a in prostate cancer remains unknown. After performing microarray analysis and reanalysis of the publicly available Memorial Sloan Kettering Cancer Center dataset, miR‐200a expression was found higher in ADPC tissues and its expression was positively associated with survival of CRPC patients. In vitro studies showed that miR‐200a overexpression in CRPC cells markedly suppressed cellular proliferation and facilitated apoptosis. In vivo studies indicated that overexpression of miR‐200a inhibited growth and metastasis of prostate cancer. The luciferase reporter assay demonstrated that BRD4 is a direct target gene of miR‐200a and it could reverse miR‐200a‐mediated biological effects in prostate cancer cells. Most importantly, our findings indicated that miR‐200a suppresses the progression of CRPC by inhibiting the activation of BRD4‐mediated AR signaling. This finding provides the foundation for the development of more personalized therapeutic approaches for CRPC patients.

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“…MYBL2 previously had been reported as miR‐30a target in acute myeloid leukemia 42 and non–small‐cell lung cancer 43 . FOXD1 was also a miR‐30a target in human ovarian carcinoma 44 and osteosarcoma 45 . However, it has not yet been established whether miR‐30a directly targets MYBL2 and FOXD1 to affect AI growth in PCa.…”

Section: Discussionmentioning

confidence: 99%

miR‐30a inhibits androgen‐independent growth of prostate cancer via targeting MYBL2, FOXD1, and SOX4

et al. 2020

The Prostate

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Background: Castrate-resistant prostate cancer (CRPC) is an aggressive and lethal disease. The pathogenesis of CRPC is not fully understood and novel therapeutic targets need to be identified to improve the patients' prognosis. has been demonstrated to be a tumor suppressor in many types of solid malignancies. However, its role in androgen-independent (AI) growth of prostate cancer (PCa) received limited attention as yet. Methods:The clinical association of miR-30a and its potential targets with AI growth was characterized by bioinformatics analyses. Regulation of cell proliferation and colony formation rates by miR-30a were tested using PCa cell models. Xenograft models were used to measure the regulation of prostate tumor growth by miR-30a.The real-time quantitative polymerase chain reaction was used to validate whether miR-30a and its targets regulate cell cycle control genes and androgen receptor (AR)-dependent transcription. Bioinformatics tools, Western blot, and luciferase reporter assays were utilized to identify miR-30a targets. Results: Bioinformatic analysis showed that low expression of miR-30a is associated with castration resistance of PCa patients and poor outcomes. Transfection of miR-30a mimics inhibited the AI growth of PCa cells in vitro and in vivo. Upregulation of miR-30a in 22RV1 cells altered the expression of cell cycle control genes and AR-mediated transcription, while downregulation of miR-30a in LNCaP cells had the opposite effects to AR-mediated transcription. MYBL2, FOXD1, and SOX4 were identified as miR-30a targets. Downregulation of MYBL2, FOXD1, and SOX4 affected the expression of cell cycle control genes and AR-mediated transcription and suppressed the AI growth of 22RV1 cells. Conclusions: Our results suggest that miR-30a inhibits AI growth of PCa by targeting MYBL2, FOXD1, and SOX4. They provide novel insights into developing new treatment strategies for CRPC. K E Y W O R D S castration-resistant prostate cancer, FOXD1, miR-30a, MYBL2, SOX4

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FOXD1 is targeted by miR-30a-5p and miR-200a-5p and suppresses the proliferation of human ovarian carcinoma cells by promoting p21 expression in a p53-independent manner

Cited by 35 publications

References 55 publications

Circulating microRNA/isomiRs as novel biomarkers of esophageal squamous cell carcinoma

Circulating microRNA/isomiRs as novel biomarkers of esophageal squamous cell carcinoma

MicroRNA‐200a suppresses prostate cancer progression through BRD4/AR signaling pathway

miR‐30a inhibits androgen‐independent growth of prostate cancer via targeting MYBL2, FOXD1, and SOX4

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