Identification of p130Cas/ErbB2-dependent invasive signatures in transformed mammary epithelial cells

Pincini, Alessandra; Tornillo, Giusy; Orso, Francesca; Sciortino, Marianna; Bisarò, Brigitte; Leal, Maria del Pilar Camacho; Lembo, Antonio; Brizzi, Maria Felice; Turco, Emilia; Pittà, Cristiano De; Provero, Paolo; Medico, Enzo; Defilippi, Paola; Taverna, Daniela; Cabodi, Sara

doi:10.4161/cc.25415

Cited by 19 publications

(25 citation statements)

References 61 publications

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“…Our current finding that Smad7 and Smurf2 protein levels are simultaneously and directly suppressed by overexpressed miR424-503 cluster in metastatic breast cancer cells without alterations in their mRNA levels, therefore, represents a novel posttranscriptional model for a coordinated regulation of these 2 factors. Although miRNAs have been reported to target Smad7 (36,37), and miR424 or miR503 overexpression has been separately found to be associated with poor prognosis in breast cancer (38,39), our results provides the first demonstration for miRNA Importantly, this newly identified mode of action is clinically relevant, as shown by our human specimens' data. Thus, a coordinated miRNA modulation of both Smad7 and Smurf2 appears to be an importantly new layer of TGFb signaling in breast cancer metastasis.…”

Section: Discussionmentioning

confidence: 54%

Metastatic Heterogeneity of Breast Cancer Cells Is Associated with Expression of a Heterogeneous TGFβ-Activating miR424–503 Gene Cluster

Ying

et al. 2014

Cancer Research

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TGFb signaling is known to drive metastasis in human cancer. Under physiologic conditions, the level of TGFb activity is tightly controlled by a regulatory network involving multiple negative regulators. At metastasis, however, these inhibitory mechanisms are usually overridden so that oncogenic TGFb signaling can be overactivated and sustained. To better understand how the TGFb inhibitors are suppressed in metastatic breast cancer cells, we compared miRNA expression profiles between breast cancers with or without metastasis and found that the miR424-503 cluster was markedly overexpressed in metastatic breast cancer. Mechanistic studies revealed that miR424 and miR503 simultaneously suppressed Smad7 and Smurf2, two key inhibitory factors of TGFb signaling, leading to enhanced TGFb signaling and metastatic capability of breast cancer cells. Moreover, antagonizing miR424-503 in breast cancer cells suppressed metastasis in vivo and increased overall host survival. Interestingly, our study also found that heterogeneous expression of the miR424-503 cluster contributed to the heterogeneity of TGFb activity levels in, and metastatic potential of, breast cancer cell subsets. Overall, our findings demonstrate a novel mechanism, mediated by elevated expression of the miR424-503 cluster, underlying TGFb activation and metastasis of human breast cancer. Cancer Res; 74(21); 6107-18. Ó2014 AACR.

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Section: Discussionmentioning

confidence: 54%

Metastatic Heterogeneity of Breast Cancer Cells Is Associated with Expression of a Heterogeneous TGFβ-Activating miR424–503 Gene Cluster

Ying

et al. 2014

Cancer Research

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“…Consistent with this result, 21 years later Pincini et al (2013) [50] showed that ITPKA belongs to the invasive signature of p130Cas/ErbB2 transformed MCF10A.B2 breast cancer cells. In addition to ErbB2, also the v-scr oncogene seems to be sufficient to induce expression of ITPKA.…”

Section: Regulation Of Itpka Expression In Tumor Cellsmentioning

confidence: 59%

Inositol-1,4,5-trisphosphate 3-kinase-A (ITPKA) is frequently over-expressed and functions as an oncogene in several tumor types

Windhorst

Song

Gazdar

2017

Biochemical Pharmacology

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At present targeted tumor therapy is based on inhibition of proteins or protein mutants that are up-regulated in tumor but not in corresponding normal cells. The actin bundling Inositol-trisphosphate 3-kinase A (ITPKA) belongs to such molecular targets. ITPKA is expressed in a broad range of tumor types but shows limited expression in normal cells. In lung and breast cancer expression of ITPKA is stimulated by gene body methylation which increases with increasing malignancy of these tumors but is not detectable in the corresponding normal tissues. Since ITPKA gene body methylation occurs early in tumor development, it could serve as biomarker for early detection of lung cancer. Detailed mechanistic studies revealed that down-regulation of ITPKA in lung adenocarcinoma cancers reduced both, tumor growth and metastasis. It is assumed that tumor growth is stimulated by the InsP3Kinase activity of ITPKA and metastasis by its actin bundling activity. A selective inhibitor against the InsP3Kinase activity of ITPKA has been identified but compounds inhibiting the actin bundling activity are not available yet. Since no curative therapy option for metastatic lung or breast tumors exist, therapies that block activities of ITPKA may offer new options for patients with these tumors. Thus, efforts should be made to develop clinical drugs that selectively target InsP3Kinase activity as well as actin bundling activity of ITPKA.

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“…It was therefore decided that we evaluate the possible interactions of miR-23b in this context, as it has previously been demonstrated to be downmodulated in invasive acini 4 , and that Blimp1 was predicted to be one of its putative targets (TargetScan v. 6.2).…”

Section: Resultsmentioning

confidence: 99%

Dysregulation of Blimp1 transcriptional repressor unleashes p130Cas/ErbB2 breast cancer invasion

Sciortino

Camacho-Leal

Orso

et al. 2017

Sci Rep

Self Cite

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ErbB2 overexpression is detected in approximately 20% of breast cancers and is correlated with poor survival. It was previously shown that the adaptor protein p130Cas/BCAR1 is a crucial mediator of ErbB2 transformation and that its overexpression confers invasive properties to ErbB2-positive human mammary epithelial cells. We herein prove, for the first time, that the transcriptional repressor Blimp1 is a novel mediator of p130Cas/ErbB2-mediated invasiveness. Indeed, high Blimp1 expression levels are detected in invasive p130Cas/ErbB2 cells and correlate with metastatic status in human breast cancer patients. The present study, by using 2D and 3D breast cancer models, shows that the increased Blimp1 expression depends on both MAPK activation and miR-23b downmodulation. Moreover, we demonstrate that Blimp1 triggers cell invasion and metastasis formation via its effects on focal adhesion and survival signaling. These findings unravel the previously unidentified role that transcriptional repressor Blimp1 plays in the control of breast cancer invasiveness.

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Identification of p130Cas/ErbB2-dependent invasive signatures in transformed mammary epithelial cells

Cited by 19 publications

References 61 publications

Metastatic Heterogeneity of Breast Cancer Cells Is Associated with Expression of a Heterogeneous TGFβ-Activating miR424–503 Gene Cluster

Metastatic Heterogeneity of Breast Cancer Cells Is Associated with Expression of a Heterogeneous TGFβ-Activating miR424–503 Gene Cluster

Inositol-1,4,5-trisphosphate 3-kinase-A (ITPKA) is frequently over-expressed and functions as an oncogene in several tumor types

Dysregulation of Blimp1 transcriptional repressor unleashes p130Cas/ErbB2 breast cancer invasion

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