Your search keyword '"Nassa, Giovanni"' showing total 10 results

1. Functional Relationships between Long Non-Coding RNAs and Estrogen Receptor Alpha: A New Frontier in Hormone-Responsive Breast Cancer Management.

Author

Melone, Viola, Salvati, Annamaria, Brusco, Noemi, Alexandrova, Elena, D'Agostino, Ylenia, Palumbo, Domenico, Palo, Luigi, Terenzi, Ilaria, Nassa, Giovanni, Rizzo, Francesca, Giurato, Giorgio, Weisz, Alessandro, and Tarallo, Roberta

Subjects

ESTROGEN receptors, LINCRNA, NON-coding RNA, BREAST cancer, HORMONE therapy, HUMAN genome, NUCLEOTIDES

Abstract

In the complex and articulated machinery of the human genome, less than 2% of the transcriptome encodes for proteins, while at least 75% is actively transcribed into non-coding RNAs (ncRNAs). Among the non-coding transcripts, those ≥200 nucleotides long (lncRNAs) are receiving growing attention for their involvement in human diseases, particularly cancer. Genomic studies have revealed the multiplicity of processes, including neoplastic transformation and tumor progression, in which lncRNAs are involved by regulating gene expression at epigenetic, transcriptional, and post-transcriptional levels by mechanism(s) that still need to be clarified. In breast cancer, several lncRNAs were identified and demonstrated to have either oncogenic or tumor-suppressive roles. The functional understanding of the mechanisms of lncRNA action in this disease could represent a potential for translational applications, as these molecules may serve as novel biomarkers of clinical use and potential therapeutic targets. This review highlights the relationship between lncRNAs and the principal hallmark of the luminal breast cancer phenotype, estrogen receptor α (ERα), providing an overview of new potential ways to inhibit estrogenic signaling via this nuclear receptor toward escaping resistance to endocrine therapy. [ABSTRACT FROM AUTHOR]

Published

2023

2. Whole-Exome Sequencing Revealed New Candidate Genes for Human Dilated Cardiomyopathy.

Author

D'Agostino, Ylenia, Palumbo, Domenico, Rusciano, Maria Rosaria, Strianese, Oriana, Amabile, Sonia, Di Rosa, Domenico, De Angelis, Elena, Visco, Valeria, Russo, Fabio, Alexandrova, Elena, Salvati, Annamaria, Giurato, Giorgio, Nassa, Giovanni, Tarallo, Roberta, Galasso, Gennaro, Ciccarelli, Michele, Weisz, Alessandro, and Rizzo, Francesca

Subjects

DILATED cardiomyopathy, GENE ontology, RECESSIVE genes, ATP-binding cassette transporters, CONGENITAL heart disease, HUMAN genes, GENETIC variation, HEART failure

Abstract

Dilated cardiomyopathy (DCM) is a complex disease affecting young adults. It is a pathological condition impairing myocardium activity that leads to heart failure and, in the most severe cases, transplantation, which is currently the only possible therapy for the disease. DCM can be attributed to many genetic determinants interacting with environmental factors, resulting in a highly variable phenotype. Due to this complexity, the early identification of causative gene mutations is an important goal to provide a genetic diagnosis, implement pre-symptomatic interventions, and predict prognosis. The advent of next-generation sequencing (NGS) has opened a new path for mutation screening, and exome sequencing provides a promising approach for identifying causal variants in known genes and novel disease-associated candidates. We analyzed the whole-exome sequencing (WES) of 15 patients affected by DCM without overloading (hypertension, valvular, or congenital heart disease) or chronic ischemic conditions. We identified 70 pathogenic or likely pathogenic variants and 1240 variants of uncertain clinical significance. Gene ontology enrichment analysis was performed to assess the potential connections between affected genes and biological or molecular function, identifying genes directly related to extracellular matrix organization, transcellular movement through the solute carrier and ATP-binding cassette transporter, and vitamin B12 metabolism. We found variants in genes implicated to a different extent in cardiac function that may represent new players in the complex genetic scenario of DCM. [ABSTRACT FROM AUTHOR]

Published

2022

3. Regulation of Metabolic Reprogramming by Long Non-Coding RNAs in Cancer.

Author

Sellitto, Assunta, Pecoraro, Giovanni, Giurato, Giorgio, Nassa, Giovanni, Rizzo, Francesca, Saggese, Pasquale, Martinez, Cesar A., Scafoglio, Claudio, and Tarallo, Roberta

Subjects

LIPID metabolism, GLUTAMINE metabolism, GENETICS, RNA, TUMORS, GLYCOLYSIS

Abstract

Simple Summary: The molecular interplay between long non-coding RNAs (lncRNAs) and cancer metabolic reprogramming enables malignant cells to adjust metabolic reactions and nutrient uptake, supporting tumor growth and dissemination. Here, we summarize the current background on lncRNA-driven alterations of cell metabolic processes, with a particular emphasis on hypoxia-inducible pathways, glycolytic process, oxidative phosphorylation, lipid anabolic and catabolic reactions, amino acid metabolism and signal transduction pathways, with the main aim of elucidating the complex network of interactions between metabolism and lncRNA expression and activity. Indeed, due to their pleiotropic roles in cell physiology and cancer development and progression, lncRNAs are currently guarded as promising diagnostic and prognostic biomarkers and therapeutic targets, providing a novel approach for the early diagnosis and personalized therapy of multiple neoplasms. Metabolic reprogramming is a well described hallmark of cancer. Oncogenic stimuli and the microenvironment shape the metabolic phenotype of cancer cells, causing pathological modifications of carbohydrate, amino acid and lipid metabolism that support the uncontrolled growth and proliferation of cancer cells. Conversely, metabolic alterations in cancer can drive changes in genetic programs affecting cell proliferation and differentiation. In recent years, the role of non-coding RNAs in metabolic reprogramming in cancer has been extensively studied. Here, we review this topic, with a focus on glucose, glutamine, and lipid metabolism and point to some evidence that metabolic alterations occurring in cancer can drive changes in non-coding RNA expression, thus adding an additional level of complexity in the relationship between metabolism and genetic programs in cancer cells. [ABSTRACT FROM AUTHOR]

Published

2021

4. Metabolic Regulation of Epigenetic Modifications and Cell Differentiation in Cancer.

Author

Saggese, Pasquale, Sellitto, Assunta, Martinez, Cesar A., Giurato, Giorgio, Nassa, Giovanni, Rizzo, Francesca, Tarallo, Roberta, and Scafoglio, Claudio

Subjects

HYPOXEMIA, CELL differentiation, METABOLITES, MITOCHONDRIA, TUMORS, PHENOTYPES, EPIGENOMICS

Abstract

Simple Summary: Cancer cells change their metabolism to support a chaotic and uncontrolled growth. In addition to meeting the metabolic needs of the cell, these changes in metabolism also affect the patterns of gene activation, changing the identity of cancer cells. As a consequence, cancer cells become more aggressive and more resistant to treatments. In this article, we present a review of the literature on the interactions between metabolism and cell identity, and we explore the mechanisms by which metabolic changes affect gene regulation. This is important because recent therapies under active investigation target both metabolism and gene regulation. The interactions of these new therapies with existing chemotherapies are not known and need to be investigated. Metabolic reprogramming is a hallmark of cancer, with consistent rewiring of glucose, glutamine, and mitochondrial metabolism. While these metabolic alterations are adequate to meet the metabolic needs of cell growth and proliferation, the changes in critical metabolites have also consequences for the regulation of the cell differentiation state. Cancer evolution is characterized by progression towards a poorly differentiated, stem-like phenotype, and epigenetic modulation of the chromatin structure is an important prerequisite for the maintenance of an undifferentiated state by repression of lineage-specific genes. Epigenetic modifiers depend on intermediates of cellular metabolism both as substrates and as co-factors. Therefore, the metabolic reprogramming that occurs in cancer likely plays an important role in the process of the de-differentiation characteristic of the neoplastic process. Here, we review the epigenetic consequences of metabolic reprogramming in cancer, with particular focus on the role of mitochondrial intermediates and hypoxia in the regulation of cellular de-differentiation. We also discuss therapeutic implications. [ABSTRACT FROM AUTHOR]

Published

2020

5. Insights into the Role of Estrogen Receptor β in Triple-Negative Breast Cancer.

Author

Sellitto, Assunta, D'Agostino, Ylenia, Alexandrova, Elena, Lamberti, Jessica, Pecoraro, Giovanni, Memoli, Domenico, Rocco, Domenico, Coviello, Elena, Giurato, Giorgio, Nassa, Giovanni, Tarallo, Roberta, Weisz, Alessandro, and Rizzo, Francesca

Subjects

BREAST tumors, CARCINOGENS, CELL lines, CELLULAR signal transduction, ESTROGEN receptors, GENE expression, ONCOGENES

Abstract

Estrogen receptors (ERα and ERβ) are ligand-activated transcription factors that play different roles in gene regulation and show both overlapping and specific tissue distribution patterns. ERβ, contrary to the oncogenic ERα, has been shown to act as an oncosuppressor in several instances. However, while the tumor-promoting actions of ERα are well-known, the exact role of ERβ in carcinogenesis and tumor progression is not yet fully understood. Indeed, to date, highly variable and even opposite effects have been ascribed to ERβ in cancer, including for example both proliferative and growth-inhibitory actions. Recently ERβ has been proposed as a potential target for cancer therapy, since it is expressed in a variety of breast cancers (BCs), including triple-negative ones (TNBCs). Because of the dependence of TNBCs on active cellular signaling, numerous studies have attempted to unravel the mechanism(s) behind ERβ-regulated gene expression programs but the scenario has not been fully revealed. We comprehensively reviewed the current state of knowledge concerning ERβ role in TNBC biology, focusing on the different signaling pathways and cellular processes regulated by this transcription factor, as they could be useful in identifying new diagnostic and therapeutic approaches for TNBC. [ABSTRACT FROM AUTHOR]

Published

2020

6. An Overview of Candidate Therapeutic Target Genes in Ovarian Cancer.

Author

Alexandrova, Elena, Pecoraro, Giovanni, Sellitto, Assunta, Melone, Viola, Ferravante, Carlo, Rocco, Teresa, Guacci, Anna, Giurato, Giorgio, Nassa, Giovanni, Rizzo, Francesca, Weisz, Alessandro, and Tarallo, Roberta

Subjects

CELLULAR signal transduction, DIAGNOSIS, GENES, MEDICAL errors, MOLECULAR diagnosis, NATURAL immunity, OVARIAN tumors, TUMOR markers, TREATMENT effectiveness, EARLY detection of cancer

Abstract

Ovarian cancer (OC) shows the highest mortality rate among gynecological malignancies and, because of the absence of specific symptoms, it is frequently diagnosed at an advanced stage, mainly due to the lack of specific and early biomarkers, such as those based on cancer molecular signature identification. Indeed, although significant progress has been made toward improving the clinical outcome of other cancers, rates of mortality for OC are essentially unchanged since 1980, suggesting the need of new approaches to identify and characterize the molecular mechanisms underlying pathogenesis and progression of these malignancies. In addition, due to the low response rate and the high frequency of resistance to current treatments, emerging therapeutic strategies against OC focus on targeting single factors and pathways specifically involved in tumor growth and metastasis. To date, loss-of-function screenings are extensively applied to identify key drug targets in cancer, seeking for more effective, disease-tailored treatments to overcome lack of response or resistance to current therapies. We review here the information relative to essential genes and functional pathways recently discovered in OC, often strictly interconnected with each other and representing promising biomarkers and molecular targets to treat these malignancies. [ABSTRACT FROM AUTHOR]

Published

2020

7. Global View of Candidate Therapeutic Target Genes in Hormone-Responsive Breast Cancer.

Author

Salvati, Annamaria, Gigantino, Valerio, Nassa, Giovanni, Mirici Cappa, Valeria, Ventola, Giovanna Maria, Cracas, Daniela Georgia Cristina, Mastrocinque, Raffaella, Rizzo, Francesca, Tarallo, Roberta, Weisz, Alessandro, and Giurato, Giorgio

Subjects

BRCA genes, HORMONE therapy, ESTROGEN, ESTROGEN receptors, CANCER invasiveness, TUMOR growth

Abstract

Breast cancer (BC) is a heterogeneous disease characterized by different biopathological features, differential response to therapy and substantial variability in long-term-survival. BC heterogeneity recapitulates genetic and epigenetic alterations affecting transformed cell behavior. The estrogen receptor alpha positive (ERα+) is the most common BC subtype, generally associated with a better prognosis and improved long-term survival, when compared to ERα-tumors. This is mainly due to the efficacy of endocrine therapy, that interfering with estrogen biosynthesis and actions blocks ER-mediated cell proliferation and tumor spread. Acquired resistance to endocrine therapy, however, represents a great challenge in the clinical management of ERα+ BC, causing tumor growth and recurrence irrespective of estrogen blockade. Improving overall survival in such cases requires new and effective anticancer drugs, allowing adjuvant treatments able to overcome resistance to first-line endocrine therapy. To date, several studies focus on the application of loss-of-function genome-wide screenings to identify key (hub) "fitness" genes essential for BC progression and representing candidate drug targets to overcome lack of response, or acquired resistance, to current therapies. Here, we review the biological significance of essential genes and relative functional pathways affected in ERα+ BC, most of which are strictly interconnected with each other and represent potential effective targets for novel molecular therapies. [ABSTRACT FROM AUTHOR]

Published

2020

8. Small Non-Coding RNA Profiling Identifies miR-181a-5p as a Mediator of Estrogen Receptor Beta-Induced Inhibition of Cholesterol Biosynthesis in Triple-Negative Breast Cancer.

Author

Alexandrova, Elena, Lamberti, Jessica, Saggese, Pasquale, Pecoraro, Giovanni, Memoli, Domenico, Mirici Cappa, Valeria, Ravo, Maria, Iorio, Roberta, Tarallo, Roberta, Rizzo, Francesca, Collina, Francesca, Cantile, Monica, Di Bonito, Maurizio, Botti, Gerardo, Nassa, Giovanni, Weisz, Alessandro, and Giurato, Giorgio

Subjects

TRIPLE-negative breast cancer, ESTROGEN receptors, NON-coding RNA, BIOSYNTHESIS, PROGESTERONE receptors, GENETIC regulation, TRANSFER RNA

Abstract

Triple-negative breast cancer (TNBC) is a highly heterogeneous disease, representing the most aggressive breast cancer (BC) subtype with limited treatment options due to a lack of estrogen receptor alpha (ERα), progesterone receptor (PR), and Erb-B2 receptor tyrosine kinase 2 (HER2/neu) expression. Estrogen receptor beta (ERβ) is present in a fraction of TNBC patients, where its expression correlates with improved patient outcomes, supported by the fact that it exerts oncosuppressive effects in TNBC cell models in vitro. ERβ is involved in microRNA-mediated regulation of gene expression in hormone-responsive BC cells and could mediate its actions through small noncoding RNAs (sncRNAs) in TNBCs also. To verify this possibility, smallRNA sequencing was performed on three ERβ-expressing cell lines from different TNBC molecular subtypes. Several sncRNAs resulted modulated by ERβ, with a subset being regulated in a tumor subtype-independent manner. Interestingly, sncRNA profiling of 12 ERβ+and 32 ERβ− primary TNBC biopsies identified 7 microRNAs, 1 PIWI-interacting RNA (piRNA), and 1 transfer RNA (tRNA) differentially expressed in ERβ+ compared to ERβ− tumors and cell lines. Among them, miR-181a-5p was found to be overexpressed in ERβ+ tumors and predicted target key components of the cholesterol biosynthesis pathway previously found to be inhibited by ERβ in TNBC cells. [ABSTRACT FROM AUTHOR]

Published

2020

9. Molecular and Functional Characterization of the Somatic PIWIL1/piRNA Pathway in Colorectal Cancer Cells.

Author

Sellitto, Assunta, Geles, Konstantinos, D'Agostino, Ylenia, Conte, Marisa, Alexandrova, Elena, Rocco, Domenico, Nassa, Giovanni, Giurato, Giorgio, Tarallo, Roberta, Weisz, Alessandro, and Rizzo, Francesca

Subjects

COLORECTAL cancer, CANCER cells, CYTOLOGY, NUCLEOTIDE sequence, GENE expression

Abstract

PIWI-like (PIWIL) proteins and small non-coding piRNAs, involved in genome regulation in germline cells, are found aberrantly expressed in human tumors. Gene expression data from The Cancer Genome Atlas (TCGA), the Genotype-Tissue Expression (GTEx) project, and the European Genome-Phenome Archive (EGA) indicate that the PIWIL1 gene is ectopically activated in a significant fraction of colorectal cancers (CRCs), where this is accompanied by promoter demethylation, together with germline factors required for piRNA production. Starting from this observation, the PIWIL/piRNA pathway was studied in detail in COLO 205 CRC cells, which express significant levels of this protein, to investigate role and significance of ectopic PIWIL1 expression in human tumors. RNA sequencing and cell and computational biology led to the demonstration that PIWIL1 localizes in a nuage-like structure located in the perinuclear region of the cell and that a significant fraction of the piRNAs expressed in these cells are methylated, and, therefore, present in an active form. This was further supported by RNA immunoprecipitation, which revealed how several piRNAs can be found loaded into PIWIL1 to form complexes also comprising their target mRNAs. The mature transcripts associated with the PIWIL–piRNA complex encode key regulatory proteins involved in the molecular mechanisms sustaining colorectal carcinogenesis, suggesting that the PIWI/piRNA pathway may actively contribute to the establishment and/or maintenance of clinico-pathological features of CRCs. [ABSTRACT FROM AUTHOR]

Published

2019

10. The Histone Methyltransferase DOT1L Is a Functional Component of Estrogen Receptor Alpha Signaling in Ovarian Cancer Cells.

Author

Salvati, Annamaria, Gigantino, Valerio, Nassa, Giovanni, Giurato, Giorgio, Alexandrova, Elena, Rizzo, Francesca, Tarallo, Roberta, and Weisz, Alessandro

Subjects

CELL proliferation, CELL cycle, CELL lines, CELLULAR signal transduction, EPITHELIAL cells, ESTROGEN receptors, GENE expression, HISTONES, OVARIAN tumors, RNA, TRANSFERASES, GENETIC testing, SEQUENCE analysis

Abstract

Although a large fraction of high-grade serous epithelial ovarian cancers (OCs) expresses Estrogen Receptor alpha (ERα), anti-estrogen-based therapies are still not widely used against these tumors due to a lack of sufficient evidence. The histone methyltransferase Disruptor of telomeric silencing-1-like (DOT1L), which is a modulator of ERα transcriptional activity in breast cancer, controls chromatin functions involved in tumor initiation and progression and has been proposed as a prognostic OC biomarker. As molecular and clinico-pathological data from TCGA suggest a correlation between ERα and DOT1L expression and OC prognosis, the presence and significance of ERα/DOT1L association was investigated in chemotherapy-sensitive and chemotherapy-resistant ER+ OC cells. RNA sequencing before and after inhibition of these factors showed that their activity is implicated in OC cell proliferation and that they functionally cooperate with each other to control the transcription of genes involved in key cancer cell features, such as the cell cycle, epithelial-mesenchymal transition (EMT), drug metabolism, and cell-to-cell signaling, as well as expression of the ERα gene itself. Together with evidence from loss-of-function genetic screens showing that ERα and DOT1L behave as core fitness factors in OC cells, these results suggest that combined inhibition of their activity might be effective against ERα-expressing, chemotherapy-resistant ovarian tumors. [ABSTRACT FROM AUTHOR]

Published

2019