Your search keyword '"Alfredo Fusco"' showing total 11 results

1. miR-130b-3p Upregulation Contributes to the Development of Thyroid Adenomas Targeting CCDC6 Gene

Author

Alfredo Fusco, Concetta Langella, Vincenza Leone, Gennaro Chiappetta, Myriam Decaussin-Petrucci, Francesco Esposito, Marco De Martino, and Antonio C. Bianco

Subjects

endocrine system, endocrine system diseases, biology, Adenoma, Endocrinology, Diabetes and Metabolism, Thyroid, Cell cycle, CREB, medicine.disease, medicine.anatomical_structure, Downregulation and upregulation, microRNA, biology.protein, medicine, Cancer research, CREB1, PAX8

Abstract

We have previously studied the function of microRNAs (miRNAs) in thyroid cells using the differentiated rat thyroid PC Cl 3 cells that need thyrotropin (TSH) for their growth. The miRNA expression profile examination allowed the detection of a set of miRNAs downregulated and upregulated by TSH. Here, we first demonstrated that upregulation of miR-130b-3p occurs through a protein kinase A-cAMP-responsive element binding protein (CREB)-dependent mechanism. Then, we analyzed its expression in human thyroid follicular adenomas, where a constitutive CREB activation is frequently present. miR-130b-3p results in upregulation with a high fold-change in most thyroid follicular adenomas. Then, we identified CCDC6, coding for a protein that interacts with CREB1 leading to the transcriptional repression of CREB1 target genes, as a target of this miRNA. The targeting of CCDC6 by miR-130b-3p likely accounts for the mechanism by which its upregulation contributes to the development of thyroid adenomas increasing CREB1 activity.

Published

2015

2. Role of the high mobility group A proteins in the regulation of pituitary cell cycle

Author

Alfredo Fusco, Monica Fedele, Fedele, M., and Fusco, Alfredo

Subjects

Adenoma, Adult, Male, Cell, FACTOR HMGI-C, DEPENDENT KINASES, Cell Cycle Proteins, Mice, Transgenic, Biology, Retinoblastoma Protein, Mice, Endocrinology, E2F1 ACTIVITY, CDK INHIBITORS, medicine, Animals, Humans, Cyclin D1, Pituitary Neoplasms, Cyclin D3, HMGA Proteins, Molecular Biology, Cyclin-Dependent Kinase Inhibitor p16, NATURAL-KILLER-CELL, Cyclin, SISTER-CHROMATID SEPARATION, TRANSGENIC MICE, DIFFERENTIAL GENE-EXPRESSION, Tumor Suppressor Proteins, Cell Cycle, Pituitary tumors, Retinoblastoma protein, HMGA, Cell cycle, medicine.disease, Cell biology, medicine.anatomical_structure, High-mobility group, Pituitary Gland, BENIGN MESENCHYMAL TUMORS, ADULT PITUITARY, biology.protein, Female, Cyclin-Dependent Kinase Inhibitor p27

Abstract

Pituitary cells are particularly sensitive to alterations of the cell cycle machinery. In fact, mutations affecting expression of proteins critical for cell cycle progression, including retinoblastoma protein, cyclins D1 and D3, p16INK4A, and p27kip1, are frequent in human pituitary adenomas. Similarly, both targeted disruption and overexpression of either cell cycle inhibitors or activators, respectively, lead to the development of pituitary adenomas in mice. Recent evidence has added the high mobility group A (HMGA) proteins as a new class of cell cycle regulators that play significant roles in the pathways that lead to pituitary tumor evolution in both humans and experimental animal models. Here, we first review the role of the cell cycle in pituitary tumorigenesis, as witnessed by human pathology and transgenic mice; and then, we focus on HMGA proteins and their cell cycle-related role in pituitary tumorigenesis.

Published

2010

3. Deregulation of microRNA expression in follicular cell-derived human thyroid carcinomas

Author

Rosa Visone, Carlo M. Croce, Alfredo Fusco, and Pierlorenzo Pallante

Subjects

endocrine system, Cancer Research, Pathology, medicine.medical_specialty, Neoplasms, Radiation-Induced, endocrine system diseases, Endocrinology, Diabetes and Metabolism, Mice, Transgenic, Follicular cell, Diagnosis, Differential, Thyroid carcinoma, Mice, Endocrinology, Adenocarcinoma, Follicular, microRNA, Biomarkers, Tumor, Carcinoma, Animals, Humans, Medicine, RNA, Neoplasm, Thyroid Neoplasms, Anaplastic thyroid cancer, Oligonucleotide Array Sequence Analysis, business.industry, Gene Expression Profiling, Thyroid, Cancer, Oncogenes, MicroRNA Expression Profile, medicine.disease, Carcinoma, Papillary, Gene Expression Regulation, Neoplastic, MicroRNAs, Cell Transformation, Neoplastic, medicine.anatomical_structure, Oncology, Mutation, business

Abstract

Carcinoma of the thyroid gland is an uncommon cancer, but one of the most frequent malignancies of the endocrine system. Most thyroid cancers are derived from the follicular cells. Follicular carcinoma is considered more malignant than papillary thyroid carcinoma (PTC), and anaplastic thyroid cancer (ATC) is one of the most lethal human cancers. Even though several genetic lesions have been already described in human thyroid cancer, particularly in the papillary histotype, the mechanisms underlying the development of these neoplasias are still far from being completely elucidated. Some years ago, several studies were undertaken to analyze the expression of microRNAs (miRNAs or miRs) in thyroid carcinoma to evaluate a possible role of their deregulation in the process of carcinogenesis. These studies showed an aberrant microRNA expression profile that distinguishes unequivocally among PTC, ATC, and normal thyroid tissue. Here, other than summarizing the current findings on microRNA expression in human thyroid carcinomas, we discuss the mechanisms by which microRNA deregulation may play a role in thyroid carcinogenesis, and the possible use of microRNA knowledge in the diagnosis and therapy of thyroid neoplasms.

Published

2010

4. The insulin receptor: a new anticancer target for peroxisome proliferator-activated receptor- (PPAR ) and thiazolidinedione-PPAR agonists

Author

Eusebio Chiefari, Daniela Foti, L Palaia, G Brunetti, Elio Gulletta, Arturo Brunetti, Francesco Paonessa, V Costa, and Alfredo Fusco

Subjects

chemistry.chemical_classification, Cancer Research, Peroxisome proliferator-activated receptor gamma, Sp1 transcription factor, Activator (genetics), Endocrinology, Diabetes and Metabolism, Peroxisome proliferator-activated receptor, Biology, Receptor tyrosine kinase, Insulin receptor, Endocrinology, Oncology, Nuclear receptor, chemistry, Cancer research, biology.protein, Transcription factor

Abstract

The peroxisome proliferator-activated receptor-gamma (PPARgamma) is a member of the nuclear hormone receptor superfamily. Ligand activation of PPARgamma is associated with differentiation and inhibition of proliferation in the normal and malignant cells. Herein, we studied the effects of PPARgamma and the PPARgamma agonists thiazolidinediones (TZDs) on the insulin receptor (IR), a cell membrane tyrosine kinase receptor protein, whose role is of paramount importance in mediating the metabolic and growth-promoting effects of the peptide hormone insulin. Overexpression of the PPARgamma1 in human hepatocellular (HepG2) cells was associated with decreased IR gene transcription and protein expression levels, and these reductions were more evident in the presence of TZDs. Since no PPARgamma response elements were identified on the IR promoter, we postulated that PPARgamma adversely affects the IR gene transcription by perturbing the assembly and stability of the transcriptionally active multiprotein-DNA complex identified previously, which includes the high-mobility group A1 protein, the ubiquitously expressed transcription factor (Sp1), the CAAT enhancer-binding protein (C/EBPbeta), and, in some cell lines, the developmentally regulated activator protein-2 (AP-2) transcription factor. Using glutathione S-transferase pull-down assays combined with electrophoretic mobility shift assay and chromatin immunoprecipitation, we demonstrated that by interacting with Sp1, C/EBPbeta, and AP-2, PPARgamma can prevent Sp1/AP-2 protein-protein association and inhibit binding of Sp1 and C/EBPbeta to DNA, thus reducing IR gene transcription. Our results demonstrate that IR is a new target gene of PPARgamma, and support a potential use of TZDs as anti-proliferative agents in selected neoplastic tissues overexpressing IRs.

Published

2008

5. A differential proteomic approach to identify proteins associated with thyroid cell transformation

Author

Nicoletta Bivi, Maria Teresa Berlingieri, Chiara D'Ambrosio, Andrea Scaloni, Igor Paron, Gianluca Tell, Giuseppe Damante, Pierlorenzo Pallante, Alfredo Fusco, Paron, I., D'Ambrosio, C., Scaloni, A., Berlingieri, . M. T., Pallante, P. L., Fusco, Alfredo, Bivi, N., Tell, G., and Damante, G.

Subjects

p53, Cell type, Galectin 1, Proteome, Mutant, Thyroid Gland, Biology, medicine.disease_cause, Endocrinology, medicine, Humans, Vimentin, Electrophoresis, Gel, Two-Dimensional, HSP90 Heat-Shock Proteins, Allele, DNA-binding domain, Molecular Biology, Gene, Transcription factor, Mutation, Transfection, Molecular biology, Neoplasm Proteins, Cell Transformation, Neoplastic, Cell culture, Tumor Suppressor Protein p53, Calreticulin, Tumour suppressor

Abstract

Tumour suppressor p53 is a transcription factor essential for DNA damage checkpoints during cellular response to stress. Mutations in the p53 gene are the most common genetic alterations found in human tumours; most pathogenetic modifications are missense mutations that abolish the p53 DNA-binding function. In the same cell type, distinct p53 missense mutations may determine different phenotypes. The PC Cl3 cell line retains several markers of thyroid differentiation in vitro. Introduction of the V143A mutant p53 allele, which abolishes the p53 DNA-binding function, leads to loss of differentiation markers as well as TSH dependency for growth. Conversely, PC Cl3 cells transfected with the S392A mutant p53 allele, presenting the mutation located outside the DNA-binding domain, show only loss of TSH dependency for growth. To identify molecular differences existing between PC Cl3 cell lines transformed by the V143A and the S392A mutant alleles, a differential proteomic approach was used. Two-dimensional gel electrophoresis analyses indicated that expression of a significant portion of protein species was modified by both p53 mutants. In fact, compared with wild-type PC Cl3 cells, modification of expression in V143A mutant cells occurred in 23.6% of the entire protein species. Conversely, modification of S392A mutant cells affected 14.0% of total proteins. Among these components, 8.3% were common to both mutants. Several of these proteins were identified by mass spectrometry procedures; some proteins, such as HSP90 and T-complex proteins, are already known to be related to p53 function.

Published

2005

6. Contents Vol. 3, 2014

Author

Minoru Kihara, Mitsuhiro Fukushima, Michel Depierreux, Kaoru Kobayashi, P. Martin van Hagen, Willem A. Dik, Luís Lopes, R Wright-Pascoe, Max Richardson, Jonah Robinson, Leendert van Steensel, Akira Miyauchi, Mafalda Marcelino, Druckerei Stückle, Karen Phillips, Hiroo Masuoka, Petros Perros, Pierlorenzo Pallante, Dion Paridaens, Margaret Miller, Richard Quinton, Andy James, Takuya Higashiyama, Marianna Di Frenna, Alfredo Fusco, Sita Virakul, Romina Sepe, Federica Marelli, Christophe Ghys, Osamu Yamada, S. G. Ball, Fabián Pitoia, Maria João Bugalho, Giovanna Weber, Yasuhiro Ito, Simon H. S. Pearce, Johannes Järhult, Antonella Federico, Tiziana de Filippis, Nadine Johnson, Mario Monaco, Erika Abelleira, Ramtin Vedad, Brigitte Velkeniers, Tomonori Yabuta, Maria Cristina Vigone, Choo-Kang E, Valeriano Leite, Monica Smikle, Virgil A. S. H. Dalm, Gennaro Chiappetta, Pedro Marques, Vikash Chatrani, Janis Hickey, Hiroshi Yoshida, Marvin Reid, Luca Persani, Margaret A. Morris, Akihiro Miya, Daniela Russo, Elçin Ozalp, Concetta Aiello, Anna-Kay Taylor-Christmas, Graciela Cross, and João Jácome de Castro

Subjects

Traditional medicine, business.industry, Endocrinology, Diabetes and Metabolism, Physiology, Medicine, business

Published

2014

7. Subject Index Vol. 4, 2015

Author

Martina Tavarelli, Birte Nygaard, Marina Morais, Hosahalli Mohan, Christian De Gennes, Linda M. Thienpont, Alfredo Fusco, Myriam Decaussin-Petrucci, Gabriele D'Hauw, Fausta Sestini, Sandro Cardinale, Rania Mehanna, Marco De Martino, Valeria Cenci, C. Ghander, Vincenza Leone, Furio Pacini, Luís Matos-Lima, Concetta Langella, Julie McCarthy, G H Beastall, Carla Fioravanti, Maria Regina Calsolari, Silvia Cantara, Gennaro Chiappetta, Gabriele Cevenini, J. Simon, Tania Pilli, Matthew S. Murphy, Antoinette Tuthill, Catherine Brophy, Gabriela Franco Mourão, Fahim U. Hassan, Eike C. Kühn, Patrick Sheahan, Julien Haroche, Pedro Weslley Rosario, James D. Faix, José Costa-Maia, Laurence Leenhardt, Camille Buffet, Druckerei Stückle, Fabrice Menegaux, Julie Sarfati, João Capela-Costa, Sofie Jespersen, Lutz Schomburg, Francesco Esposito, Antonio Bianco, Lars Østergaard Kristensen, and Ellen C.D. Heid

Subjects

Gerontology, Index (economics), business.industry, Endocrinology, Diabetes and Metabolism, Medicine, Subject (documents), business

Published

2015

8. Horst Schleusener, 1933-2015

Author

Furio Pacini, Marina Morais, Linda M. Thienpont, Eike C. Kühn, Fausta Sestini, Julien Haroche, Ellen C.D. Heid, Myriam Decaussin-Petrucci, Valeria Cenci, Vincenza Leone, Maria Regina Calsolari, Birte Nygaard, João Capela-Costa, Catherine Brophy, Fabrice Menegaux, Gabriele Cevenini, Fahim U. Hassan, Pedro Weslley Souza Rosario, Antonio Bianco, J. Simon, Camille Buffet, Matthew S. Murphy, Lars Østergaard Kristensen, Julie Sarfati, Antoinette Tuthill, Sofie Jespersen, Lutz Schomburg, Julie McCarthy, Marco De Martino, Laurence Leenhardt, Carla Fioravanti, Francesco Esposito, Patrick Sheahan, Luís Matos-Lima, Concetta Langella, Sandro Cardinale, C. Ghander, James D. Faix, José Costa-Maia, Gabriela Franco Mourão, Druckerei Stückle, Gennaro Chiappetta, Silvia Cantara, Hosahalli Mohan, Christian De Gennes, Tania Pilli, Graham Beastall, Gabriele D'Hauw, Rania Mehanna, Martina Tavarelli, and Alfredo Fusco

Subjects

business.industry, Endocrinology, Diabetes and Metabolism, Medicine, business, Classics

Published

2015

9. Targeting ofPATZ1by miR-29b is a downstream effect of oncogenic Ras signalling in thyroid cells

Author

Sonia Mansueto, Alfredo Fusco, Menna Marta De, Luigia Serpico, Teresa Valentino, Gabriella De Vita, Michela Vitiello, and Monica Fedele

Subjects

Signalling, Downstream (manufacturing), Chemistry, Anti-apoptotic Ras signalling cascade, Thyroid cells, Cell biology

Published

2013

10. Subject Index Vol. 3, 2014

Author

Monica Smikle, Ramtin Vedad, Valeriano Leite, Romina Sepe, Karen Phillips, Choo-Kang E, Luís Lopes, Andy James, Maria Cristina Vigone, S. G. Ball, Margaret A. Morris, Yasuhiro Ito, P. Martin van Hagen, Michel Depierreux, Kaoru Kobayashi, Mario Monaco, Petros Perros, Osamu Yamada, Takuya Higashiyama, Hiroo Masuoka, Nadine Johnson, Richard Quinton, Tomonori Yabuta, Erika Abelleira, Margaret Miller, Jonah Robinson, Akihiro Miya, Anna-Kay Taylor-Christmas, Akira Miyauchi, Christophe Ghys, Federica Marelli, Mafalda Marcelino, Marianna Di Frenna, R Wright-Pascoe, Fabián Pitoia, Max Richardson, Daniela Russo, Simon H. S. Pearce, Druckerei Stückle, Pierlorenzo Pallante, Gennaro Chiappetta, Pedro Marques, Johannes Järhult, Giovanna Weber, Marvin Reid, Sita Virakul, Dion Paridaens, Virgil A. S. H. Dalm, Alfredo Fusco, Antonella Federico, Tiziana de Filippis, Willem A. Dik, Vikash Chatrani, Janis Hickey, Hiroshi Yoshida, Luca Persani, Brigitte Velkeniers, Concetta Aiello, Leendert van Steensel, Graciela Cross, Maria João Bugalho, João Jácome de Castro, Elçin Ozalp, Minoru Kihara, and Mitsuhiro Fukushima

Subjects

Gerontology, Index (economics), business.industry, Endocrinology, Diabetes and Metabolism, Medicine, Subject (documents), business

Published

2014

11. Impairment of the p27kip1 function enhances thyroid carcinogenesis in TRK-T1 transgenic mice.

Author

Monica Fedele, Dario Palmieri, Gennaro Chiappetta, Rosa Pasquinelli, Ivana De Martino, Claudio Arra, Giuseppe Palma, Teresa Valentino, Giovanna M Pierantoni, Giuseppe Viglietto, Jay L Rothstein, Massimo Santoro, and Alfredo Fusco

Subjects

CYCLIN-dependent kinases, CARCINOGENESIS, TRANSGENIC mice, CELL proliferation, THYROGLOBULIN, THYROID cancer, GENE expression, ONCOGENES

Abstract

Impairment of the p27(kip1) function, caused by a drastic reduction of its expression or cytoplasmic mislocalization, has been frequently observed in thyroid carcinomas. To understand the role of p27(kip1) impairment in thyroid carcinogenesis, we investigated the consequences of the loss of p27(kip1) expression in the context of a mouse modeling of papillary thyroid cancer, expressing the TRK-T1 oncogene under the transcriptional control of thyroglobulin promoter. We found that double mutant mice homozygous for a p27(kip1) null allele (TRK-T1/p27(-/-)) display a higher incidence of papillary thyroid carcinomas, with a shorter latency period and increased proliferation index, compared with p27(kip1) wild-type compounds (TRK-T1/p27(+/+)). Consistently, double mutant mice heterozygous for a p27(kip1) null allele (TRK-T1/p27(+/-)) show an incidence of thyroid carcinomas that is intermediate between TRK-T1/p27(-/-) and TRK-T1/p27(+/+) mice. Therefore, our findings suggest a dose-dependent role of p27(kip1) function in papillary thyroid cancer development. [ABSTRACT FROM AUTHOR]

Published

2009