Loss of p63 and its microRNA-205 target results in enhanced cell migration and metastasis in prostate cancer

Tucci, Paola; Agostini, Massimiliano; Grespi, Francesca; Markert, Elke; Terrinoni, Alessandro; Vousden, Karen H.; Muller, Patricia A J; Dötsch, Volker; Kehrloesser, Sebastian; Sayan, Berna S.; Giaccone, Giuseppe; Lowe, Scott W.; Takahashi, Nozomi; Vandenabeele, Peter; Knight, Richard; Levine, Arnold J.; Melino, Gerry

doi:10.1073/pnas.1110977109

Cited by 249 publications

(246 citation statements)

References 27 publications

(30 reference statements)

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“…Notably, some of the outcomes observed during ExEn formation in EBs were inconsistent with the reported role of miR-205 in maintaining epithelial fates and E-cadherin expression and in forestalling the epithelial to mesenchymal transition (EMT) during tumor progression (29,33,34). The few reported targets of miR-205 in tumor cells include Although these experiments were not designed to identify genes directly targeted by miR-205, we selected the most probable miR-205 mouse target genes in each of three public databases (miRDB.org, TargetScan.org, and microRNA.org) and chose 26 genes for further analysis that were concordantly ranked in the "top 60."…”

Section: Discussionmentioning

confidence: 55%

“…Down-regulation of miR-205 in tumor cells promotes the EMT and metastasis in several forms of cancer (29,33,34,40,41). A parsimonious hypothesis is that a role for Arf as a tumor suppressor in somatic cells is mediated, at least in part, by its regulation of EMT in response to oncogene activation.…”

Section: Discussionmentioning

confidence: 99%

“…Analysis of EBs in which Arf expression could be conditionally up-or down-regulated provided direct evidence for positively correlated Arf and miR-205 expression. In turn, miR-205 expression is induced by p53, and its promoter is directly regulated by other p53 family members (27)(28)(29).…”

Section: Discussionmentioning

confidence: 99%

“…In unrelated studies, we determined that the levels of a single microRNA, miR-205, were selectively decreased by >15-fold in the Arf-null testes of postnatal day-18 mice, a time when p19 Arf levels in spermatogonia are maximal and are synchronously expressed throughout the developing seminiferous tubules. miR-205 is up-regulated by p53 (27), and its promoter is directly bound and induced by other p53-related family members, p63 and p73 (28,29).…”

Section: Significancementioning

confidence: 99%

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Arf tumor suppressor and miR-205 regulate cell adhesion and formation of extraembryonic endoderm from pluripotent stem cells

Finkelstein

Sherr

2013

Proc. Natl. Acad. Sci. U.S.A.

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Significance The Arf tumor suppressor gene is not expressed in most normal tissues but when activated by oncogenic stress signals engages a p53-dependent transcriptional program that prevents tumor formation. Surprisingly, expression of the p19 Arf protein in mouse embryoid bodies is required for the timely formation of extraembryonic endoderm (ExEn). Inactivation of Arf down-regulates a single microRNA, miR-205, which can “rescue” ExEn formation in Arf -null embryonic or induced pluripotent stem cells. During ExEn formation, miR-205 regulates a suite of genes that govern cell migration and adhesion, suggesting a conceptual basis for linking the roles of Arf in ExEn differentiation and tumor metastasis.

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Section: Discussionmentioning

confidence: 55%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Significancementioning

confidence: 99%

See 2 more Smart Citations

Arf tumor suppressor and miR-205 regulate cell adhesion and formation of extraembryonic endoderm from pluripotent stem cells

Finkelstein

Sherr

2013

Proc. Natl. Acad. Sci. U.S.A.

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“…There is accumulating evidence that downregulation of miR-205-5p occurs in several cancers, e.g., breast, lung, esophageal and prostate cancers, and that it acts as an antitumor miRNA [33]. Downregulation of miR-205-5p in PCa tissues and its antitumor roles in PCa cells have been observed in past studies, including data from our laboratory [22,34]. Androgen signaling through AR is an essential pathway in PCa progression and aggressiveness [35].…”

Section: Discussionmentioning

confidence: 99%

Regulation of HMGB3 by antitumor miR-205-5p inhibits cancer cell aggressiveness and is involved in prostate cancer pathogenesis

et al. 2017

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Our recent determination of a microRNA (miRNA) expression signature in prostate cancer (PCa) revealed that miR-205-5p was significantly reduced in PCa tissues and that it acted as an antitumor miRNA. The aim of this study was to identify oncogenic genes and pathways in PCa cells that were regulated by antitumor miR-205-5p. Genome-wide gene expression analyses and in silico miRNA database searches showed that 37 genes were putative targets of miR-205-5p regulation. Among those genes, elevated expression levels of seven in particular (HMGB3, SPARC, MKI67, CENPF, CDK1, RHOU, and POLR2D) were associated with a shorter disease-free survival in a large number of patients in the The Cancer Genome Atlas (TCGA) database. We focused on high-mobility group box 3 (HMGB3) because it was the most downregulated by ectopic expression of miR-205-5p in PC3 cells and its expression was involved in PCa pathogenesis. Luciferase reporter assays showed that HMGB3 was directly regulated by miR-205-5p in PCa cells. Knockdown studies using si-HMGB3 showed that expression of HMGB3 enhanced PCa cell aggressiveness. Overexpression of HMGB3/HMGB3 was confirmed in naive PCa and castration-resistant PCa (CRPC) clinical specimens. Novel approaches to analysis of antitumor miRNAregulated RNA networks in PCa cells may provide new insights into the pathogenic mechanisms of the disease.

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The strong propensity of Cadherin‐23 for aggregation inhibits cell migration

et al. 2019

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Cadherin‐23 (Cdh23), a long‐chain non‐classical cadherin, exhibits strong homophilic and heterophilic binding. The physiological relevance of strong heterophilic binding with protocadherin‐15 at neuroepithelial tip links is well‐studied. However, the role of Cdh23 homodimers in physiology is less understood, despite its widespread expression at the cell boundaries of various human and mouse tissues, including kidney, muscle, testes, and heart. Here, we performed immunofluorescence studies that revealed that Cdh23 is present as distinct puncta at the cell–cell boundaries of cancer cells. Analysis of patient data and quantitative estimation of Cdh23 in human tissues (normal and tumor) also indicated that Cdh23 is down‐regulated via promoter methylation in lung adenocarcinoma (AD) and esophageal squamous cell carcinoma (SCC) cells; we also observed a clear inverse correlation between Cdh23 expression and cancer metastasis. Using HEK 293T cells and four types of cancer cells differentially expressing Cdh23, we observed that cell migration was faster in cells with reduced levels of Cdh23 expression. The cell migration rate in cancer cells is further accelerated by the presence of excretory isoforms of Cdh23, which loosen its cell‐adhesion ability by competitive binding. Overall, our data indicate the role of Cdh23 as a suppressor of cell migration.

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Loss of p63 and its microRNA-205 target results in enhanced cell migration and metastasis in prostate cancer

Cited by 249 publications

References 27 publications

Arf tumor suppressor and miR-205 regulate cell adhesion and formation of extraembryonic endoderm from pluripotent stem cells

Arf tumor suppressor and miR-205 regulate cell adhesion and formation of extraembryonic endoderm from pluripotent stem cells

Regulation of HMGB3 by antitumor miR-205-5p inhibits cancer cell aggressiveness and is involved in prostate cancer pathogenesis

The strong propensity of Cadherin‐23 for aggregation inhibits cell migration

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