Genomic Profiling of MicroRNAs in Bladder Cancer: miR-129 Is Associated with Poor Outcome and Promotes Cell Death <i>In vitro</i>

Dyrskjøt, Lars; Ostenfeld, Marie Stampe; Bramsen, Jesper B.; Silahtaroglu, Asli; Lamy, Philippe; Ramanathan, Ramshanker; Fristrup, Niels; Jensen, Jens Ledet; Andersen, Claus Lindbjerg; Zieger, Karsten; Kauppinen, Sakari; Ulhøi, Benedicte Parm; Kjems, Jørgen; Borre, Michael; Ørntoft, Torben F.

doi:10.1158/0008-5472.can-08-4043

Cited by 339 publications

(301 citation statements)

References 46 publications

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“…This phenomenon has been noticed in several occasions. Although it has been shown that miR-200c is consistently upregulated in prostate cancer (20), the opposite has been reported for bladder cancer (27). We conclude that the role of an individual miRNA in tumor initiation or growth is organ or cell type specific so that differences in its deregulation between different tumor entities are not a contradiction, but rather reflect different roles of its target gene or genes in different tumor types.…”

Section: Discussionmentioning

confidence: 59%

The MicroRNA Profile of Prostate Carcinoma Obtained by Deep Sequencing

Szczyrba

Löprich²,

Wach³

et al. 2010

Molecular Cancer Research

208

207

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Prostate cancer is a leading cause of tumor mortality. To characterize the underlying molecular mechanisms, we have compared the microRNA (miRNA) profile of primary prostate cancers and noncancer prostate tissues using deep sequencing. MiRNAs are small noncoding RNAs of 21 to 25 nucleotides that regulate gene expression through the inhibition of protein synthesis. We find that 33 miRNAs were upregulated or downregulated >1.5-fold. The deregulation of selected miRNAs was confirmed by both Northern blotting and quantitative reverse transcription-PCR in established prostate cancer cell lines and clinical tissue samples. A computational search indicated the 3′-untranslated region (UTR) of the mRNA for myosin VI (MYO6) as a potential target for both miR-143 and miR-145, the expression of which was reduced in the tumor tissues. Upregulation of myosin VI in prostate cancer was previously shown by immunohistochemistry. The level of MYO6 mRNA was significantly induced in all primary tumor tissues compared with the nontumor tissue from the same patient. This finding was matched to the upregulation of myosin VI in established prostate cancer cell lines. In luciferase reporter analysis, we find a significant negative regulatory effect on the MYO6 3′UTR by both miR-143 and miR-145. Mutation of the potential binding sites for miR-143 and miR-145 in the MYO6 3′ UTR resulted in a loss of responsiveness to the corresponding miRNA. Our data indicate that miR-143 and miR-145 are involved in the regulation of MYO6 expression and possibly in the development of prostate cancer. Mol Cancer Res; 8(4); 529-38. ©2010 AACR.

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Section: Discussionmentioning

confidence: 59%

The MicroRNA Profile of Prostate Carcinoma Obtained by Deep Sequencing

Szczyrba

Löprich²,

Wach³

et al. 2010

Molecular Cancer Research

208

207

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“…The downregulation of miR-145 ( Figure 1a) in bladder cancer specimens and urothelial cell lines, as compared with normal biopsies (Figures 1b and c) (Dyrskjot et al, 2009), prompted us to investigate whether the differences in miRNA levels measured may reflect tissue heterogeneity and/or an altered ratio of different cell types to the tumor mass, rather than tumor cell-specific expression changes. We performed ISH analysis to identify which cell type(s) expressed miR-145 (Figure 2).…”

Section: Localization Of Mir-145 In Clinical Samples By Ish Analysismentioning

confidence: 99%

“…In accordance, miRNAs have been shown to influence gene regulatory processes in, for example, development, differentiation, and disease, such as cancer (Calin and Croce, 2006;Esquela-Kerscher and Slack, 2006), in which specific miRNA signatures have been associated with different clinical outcomes (Nakajima et al, 2006;Rajewsky, 2006;Yanaihara et al, 2006;Sempere et al, 2007;Tavazoie et al, 2008;Dyrskjot et al, 2009). Approximately 50% of the known miRNAs are located within regions of genomic instability that are amplified or deleted in cancer (Calin et al, 2004), which may in part explain the aberrant expression observed.…”

Section: Introductionmentioning

confidence: 99%

“…We recently identified miR-145 as the most significantly downregulated miRNA (P ¼ 2.1EÀ08) in an miRNA profiling study on bladder cancer comprising 106 clinical samples of bladder cancer and 11 normal bladder biopsies (Dyrskjot et al, 2009). Bladder cancer is the fourth most common cancer among men and can be pathologically classified into discrete stages; Ta are benign papillary tumors, T1 are lamina propriainvasive tumors, carcinoma in situ (CIS) are small in situ lesions of high-grade atypia, and T2-T4 are muscleinvasive tumors.…”

Section: Introductionmentioning

confidence: 99%

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miR-145 induces caspase-dependent and -independent cell death in urothelial cancer cell lines with targeting of an expression signature present in Ta bladder tumors

et al. 2009

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Downregulation of miR-145 in a variety of cancers suggests a possible tumor suppressor function for this microRNA. Here, we show that miR-145 expression is reduced in bladder cancer and urothelial carcinoma in situ, compared with normal urothelium, using transcription profiling and in situ hybridization. Ectopic expression of miR-145 induced extensive apoptosis in urothelial carcinoma cell lines (T24 and SW780) as characterized by caspase activation, nuclear condensation and fragmentation, cellular shrinkage, and detachment. However, cell death also proceeded upon caspase inhibition by the pharmacological inhibitor zVAD-fmk and ectopic expression of anti-apoptotic Bcl-2, indicating the activation of an alternative caspase-independent death pathway. Microarray analysis of transcript levels in T24 cells, before the onset of cell death, showed destabilization of mRNAs enriched for miR-145 7mer target sites. Among these, direct targeting of CBFB, PPP3CA, and CLINT1 was confirmed by a luciferase reporter assay. Notably, a 22-gene signature targeted on enforced miR-145 expression in T24 cells was significantly (Po0.00003) upregulated in 55 Ta bladder tumors with concomitant reduction of miR-145. Our data indicate that reduction in miR-145 expression may provide bladder cancer cells with a selective advantage by inhibition of cell death otherwise triggered in malignant cells.

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“…MiR-129-5p, one of the mature forms of miR-129-1 and miR-129-2, has been reported to be involved in various neoplastic processes, including GC [7][8][9]. It has been demonstrated that miR-129-5p serves as an important tumor suppressor, and overexpression of miR-129-5p could significantly decrease the cell proliferation activity of multiple tumor cell lines, such as endometrial tumor cells, lung adenocarcinoma cell lines, bladder cancer cells, and GC cells [7,[10][11][12]. Another mature form of miR-129-1 and miR-129-2, miR-129-3p, has been suggested as a diagnostic and prognostic biomarker for renal cell carcinoma (RCC), and could regulate cell migration and invasion by downregulating multiple metastasis-related genes [13].…”

mentioning

confidence: 99%

MiR-129-5p is down-regulated and involved in migration and invasion of gastric cancer cells by targeting interleukin-8

Jiang¹,

Wang²,

Li³

et al. 2016

neo

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Expression of microRNA-129-5p (miR-129-5p) has been reported to decrease in gastric cancer (GC). However, little information is available about how miR-129-5p affects cell migration and invasion of GC. Cancer samples and matched non-tumor adjacent tissues were obtained from patients with GC. Besides, peripheral blood samples were collected from both the patients and healthy volunteers. Expression of miR-129-5p was analyzed by real-time PCR (RT-PCR). After transfection with miR-129-5p mimics, miR-129-5p inhibitor, or negative controls in human GC cell line SGC-7901, cell viability, colony-formation ability, migration, and invasion assay were evaluated. Luciferase reporter assay, RT-PCR, and enzyme-linked immunosorbent assay (ELISA) were performed to explore whether interleukin-8 was a target of miR-129-5p. Further, small interfering RNA (siRNA) against IL-8 was transfected into cells, and then the effects of miR-129-5p inhibitor on migration and invasion were assessed. MiR-129-5p was down-regulated in both GC samples and blood samples compared to their matched non-tumor adjacent tissues and healthy volunteers (both P < 0.05). Compared to the control group, transfection with miR-129-5p inhibitor markedly increased the cell viability, colony-forming ability, and numbers of migrated and invaded cells. Luciferase reporter assay confirmed that IL-8 was a direct target of miR-129-5p, and IL-8 was negatively regulated by miR-129-5p. Cotransfection of miR-129-5p inhibitor with si-IL-8 reversed the effect of miR-129-5p inhibitor on the migration and invasion of the cells. MiR-129-5p and regulates migration and invasion of GC cells by targeting IL-8.

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Genomic Profiling of MicroRNAs in Bladder Cancer: miR-129 Is Associated with Poor Outcome and Promotes Cell Death In vitro

Cited by 339 publications

References 46 publications

The MicroRNA Profile of Prostate Carcinoma Obtained by Deep Sequencing

The MicroRNA Profile of Prostate Carcinoma Obtained by Deep Sequencing

miR-145 induces caspase-dependent and -independent cell death in urothelial cancer cell lines with targeting of an expression signature present in Ta bladder tumors

MiR-129-5p is down-regulated and involved in migration and invasion of gastric cancer cells by targeting interleukin-8

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