Your search keyword '"Muoio, Maria Grazia"' showing total 3 results

1. The G protein-coupled estrogen receptor (GPER) 2 expression correlates with pro-metastatic pathways in 3 ER-negative breast cancer: a bioinformatics analysis

Author

Talia, Marianna, De Francesco, Ernestina Marianna, Rigiracciolo, Damiano Cosimo, Muoio, Maria Grazia, Muglia, Lucia, Belfiore, Antonino, Maggiolini, Marcello, Sims, Andrew, and Lappano, Rosamaria

Subjects

cell adhesion molecules, Breast cancer, Bioinformatics, extracellular matrix, TCGA, METABRIC, focal adhesion, GPER

Abstract

The G protein-coupled estrogen receptor (GPER, formerly known as GPR30) is a seven-transmembrane receptor that mediates estrogen signals in both normal and malignant cells. In particular, GPER has been involved in the activation of diverse signaling pathways toward transcriptional and biological responses that characterize the progression of breast cancer (BC). In this context, a correlation between GPER expression and worse clinical-pathological features of BC has been suggested, although controversial data have been also reported. In order to better assess the biological significance of GPER in the aggressive estrogen receptor (ER)-negative BC, we performed a bioinformatics analysis using the information provided by The Invasive Breast Cancer Cohort of the The Cancer Genome Atlas (TCGA) project and the Molecular Taxonomy of Breast Cancer International Consortium (METABRIC) datasets. Gene expression correlation and the statistical analysis were carried out with R studio base functions and the tidyverse package. Pathway enrichment analysis was evaluated with KEGG pathway on DAVID website, whereas Gene Set Enrichment Analysis (GSEA) was performed with the R package phenoTest. The survival analysis was determined with the R package survivALL. Analyzing the expression data of more than 2500 primary BC, we ascertained that GPER levels are associated with pro-migratory and metastatic genes belonging to the cell adhesion molecules (CAMs), extracellular matrix (ECM)-receptor interaction and focal adhesion (FA) signaling pathways. Thereafter, evaluating the disease free interval (DFI) in ER-negative BC patients, we found that the subjects expressing high GPER levels exhibit a shorter DFI respect to those exhibiting low GPER levels. Overall, our results may pave the way to further dissect in the breast malignancies lacking ER the network triggered by GPER, toward a better assessment of its prognostic significance and the action elicited in mediating the aggressive features of the aforementioned BC subtype.

Published

2020

2. Activation of the S100A7/RAGE Pathway by IGF-1 Contributes to Angiogenesis in Breast Cancer.

Author

Muoio, Maria Grazia, Talia, Marianna, Lappano, Rosamaria, Sims, Andrew H., Vella, Veronica, Cirillo, Francesca, Manzella, Livia, Giuliano, Marika, Maggiolini, Marcello, Belfiore, Antonino, De Francesco, Ernestina Marianna, and Magklara, Angeliki

Subjects

*SOMATOMEDIN, *DISEASE progression, *CATHELICIDINS, *CARCINOGENESIS, *ONCOGENES, *INFLAMMATION, *CELL cycle proteins, *CELL receptors, *CELLULAR signal transduction, *ADVANCED glycation end-products, *BIOINFORMATICS, *GENE expression, *ESTROGEN receptors, *CALCIUM-binding proteins, *CELL lines, *BIOLOGICAL assay, *BREAST tumors

Abstract

Simple Summary: Breast cancer mortality is increased in patients affected by metabolic disorders associated with dysregulation of the Insulin-like growth factor-1 (IGF-1) axis, like obesity and type-2 diabetes. Despite the oncogenic role of this complex signaling system is widely known, the clinical targeting of IGF-1 and its receptor (IGF-1R) has provided valuable benefit only on small sub-populations of cancer patients, thus suggesting that a further characterization of the biological effects of the IGF-1/IGF-1R pathway could pave the way for a better manipulation of this crucial signaling system at the clinical level. In this study, we have identified the protein S100A7 as novel molecular target of IGF-1 action in the breast tumor microenvironment, toward increased cancer-associated angiogenesis. Targeting the IGF-1/IGF-1R/S100A7 pathway may therefore represent a further useful approach for blocking disease progression in breast cancer patients with dysregulated IGF-1 signaling. Background: Breast cancer (BC) mortality is increased among obese and diabetic patients. Both obesity and diabetes are associated with dysregulation of both the IGF-1R and the RAGE (Receptor for Advanced Glycation End Products) pathways, which contribute to complications of these disorders. The alarmin S100A7, signaling through the receptor RAGE, prompts angiogenesis, inflammation, and BC progression. Methods: We performed bioinformatic analysis of BC gene expression datasets from published studies. We then used Estrogen Receptor (ER)-positive BC cells, CRISPR-mediated IGF-1R KO BC cells, and isogenic S100A7-transduced BC cells to investigate the role of IGF-1/IGF-1R in the regulation of S100A7 expression and tumor angiogenesis. To this aim, we also used gene silencing and pharmacological inhibitors, and we performed gene expression and promoter studies, western blotting analysis, ChIP and ELISA assays, endothelial cell proliferation and tube formation assay. Results: S100A7 expression correlates with worse prognostic outcomes in human BCs. In BC cells, the IGF-1/IGF-1R signaling engages STAT3 activation and its recruitment to the S100A7 promoter toward S100A7 increase. In human vascular endothelial cells, S100A7 activates RAGE signaling and prompts angiogenic effects. Conclusions: In ER-positive BCs the IGF-1 dependent activation of the S100A7/RAGE signaling in adjacent endothelial cells may serve as a previously unidentified angiocrine effector. Targeting S100A7 may pave the way for a better control of BC, particularly in conditions of unopposed activation of the IGF-1/IGF-1R axis. [ABSTRACT FROM AUTHOR]

Published

2021

3. The G Protein-Coupled Estrogen Receptor (GPER) Expression Correlates with Pro-Metastatic Pathways in ER-Negative Breast Cancer: A Bioinformatics Analysis.

Author

Talia, Marianna, De Francesco, Ernestina Marianna, Rigiracciolo, Damiano Cosimo, Muoio, Maria Grazia, Muglia, Lucia, Belfiore, Antonino, Maggiolini, Marcello, Sims, Andrew H., and Lappano, Rosamaria

Subjects

G protein coupled receptors, CELL adhesion molecules, BREAST cancer, FOCAL adhesions, ESTROGEN receptors

Abstract

The G protein-coupled estrogen receptor (GPER, formerly known as GPR30) is a seven-transmembrane receptor that mediates estrogen signals in both normal and malignant cells. In particular, GPER has been involved in the activation of diverse signaling pathways toward transcriptional and biological responses that characterize the progression of breast cancer (BC). In this context, a correlation between GPER expression and worse clinical-pathological features of BC has been suggested, although controversial data have also been reported. In order to better assess the biological significance of GPER in the aggressive estrogen receptor (ER)-negative BC, we performed a bioinformatics analysis using the information provided by The Invasive Breast Cancer Cohort of The Cancer Genome Atlas (TCGA) project and Molecular Taxonomy of Breast Cancer International Consortium (METABRIC) datasets. Gene expression correlation and the statistical analysis were carried out with R studio base functions and the tidyverse package. Pathway enrichment analysis was evaluated with Kyoto Encyclopedia of Genes and Genomes (KEGG) pathway on the Database for Annotation, Visualization and Integrated Discovery (DAVID) website, whereas gene set enrichment analysis (GSEA) was performed with the R package phenoTest. The survival analysis was determined with the R package survivALL. Analyzing the expression data of more than 2500 primary BC, we ascertained that GPER levels are associated with pro-migratory and metastatic genes belonging to cell adhesion molecules (CAMs), extracellular matrix (ECM)-receptor interaction, and focal adhesion (FA) signaling pathways. Thereafter, evaluating the disease-free interval (DFI) in ER-negative BC patients, we found that the subjects expressing high GPER levels exhibited a shorter DFI in respect to those exhibiting low GPER levels. Overall, our results may pave the way to further dissect the network triggered by GPER in the breast malignancies lacking ER toward a better assessment of its prognostic significance and the action elicited in mediating the aggressive features of the aforementioned BC subtype. [ABSTRACT FROM AUTHOR]

Published

2020