Your search keyword '"Carmine Del Giudice"' showing total 3 results

1. Targeting the CaMKII/ERK Interaction in the Heart Prevents Cardiac Hypertrophy.

Author

Ersilia Cipolletta, Maria Rosaria Rusciano, Angela Serena Maione, Gaetano Santulli, Daniela Sorriento, Carmine Del Giudice, Michele Ciccarelli, Antonietta Franco, Catherine Crola, Pietro Campiglia, Marina Sala, Isabel Gomez-Monterrey, Nicola De Luca, Bruno Trimarco, Guido Iaccarino, and Maddalena Illario

Subjects

Medicine, Science

Abstract

Activation of Ca2+/Calmodulin protein kinase II (CaMKII) is an important step in signaling of cardiac hypertrophy. The molecular mechanisms by which CaMKII integrates with other pathways in the heart are incompletely understood. We hypothesize that CaMKII association with extracellular regulated kinase (ERK), promotes cardiac hypertrophy through ERK nuclear localization.In H9C2 cardiomyoblasts, the selective CaMKII peptide inhibitor AntCaNtide, its penetratin conjugated minimal inhibitory sequence analog tat-CN17β, and the MEK/ERK inhibitor UO126 all reduce phenylephrine (PE)-mediated ERK and CaMKII activation and their interaction. Moreover, AntCaNtide or tat-CN17β pretreatment prevented PE induced CaMKII and ERK nuclear accumulation in H9C2s and reduced the hypertrophy responses. To determine the role of CaMKII in cardiac hypertrophy in vivo, spontaneously hypertensive rats were subjected to intramyocardial injections of AntCaNtide or tat-CN17β. Left ventricular hypertrophy was evaluated weekly for 3 weeks by cardiac ultrasounds. We observed that the treatment with CaMKII inhibitors induced similar but significant reduction of cardiac size, left ventricular mass, and thickness of cardiac wall. The treatment with CaMKII inhibitors caused a significant reduction of CaMKII and ERK phosphorylation levels and their nuclear localization in the heart.These results indicate that CaMKII and ERK interact to promote activation in hypertrophy; the inhibition of CaMKII-ERK interaction offers a novel therapeutic approach to limit cardiac hypertrophy.

Published

2015

2. Human glioblastoma multiforme: p53 reactivation by a novel MDM2 inhibitor.

Author

Barbara Costa, Sara Bendinelli, Pamela Gabelloni, Eleonora Da Pozzo, Simona Daniele, Fabrizio Scatena, Renato Vanacore, Pietro Campiglia, Alessia Bertamino, Isabel Gomez-Monterrey, Daniela Sorriento, Carmine Del Giudice, Guido Iaccarino, Ettore Novellino, and Claudia Martini

Subjects

Medicine, Science

Abstract

Cancer development and chemo-resistance are often due to impaired functioning of the p53 tumor suppressor through genetic mutation or sequestration by other proteins. In glioblastoma multiforme (GBM), p53 availability is frequently reduced because it binds to the Murine Double Minute-2 (MDM2) oncoprotein, which accumulates at high concentrations in tumor cells. The use of MDM2 inhibitors that interfere with the binding of p53 and MDM2 has become a valid approach to inhibit cell growth in a number of cancers; however little is known about the efficacy of these inhibitors in GBM. We report that a new small-molecule inhibitor of MDM2 with a spirooxoindolepyrrolidine core structure, named ISA27, effectively reactivated p53 function and inhibited human GBM cell growth in vitro by inducing cell cycle arrest and apoptosis. In immunoincompetent BALB/c nude mice bearing a human GBM xenograft, the administration of ISA27 in vivo activated p53, inhibited cell proliferation and induced apoptosis in tumor tissue. Significantly, ISA27 was non-toxic in an in vitro normal human cell model and an in vivo mouse model. ISA27 administration in combination with temozolomide (TMZ) produced a synergistic inhibitory effect on GBM cell viability in vitro, suggesting the possibility of lowering the dose of TMZ used in the treatment of GBM. In conclusion, our data show that ISA27 releases the powerful antitumor capacities of p53 in GBM cells. The use of this MDM2 inhibitor could become a novel therapy for the treatment of GBM patients.

Published

2013

3. Human Glioblastoma Multiforme: p53 Reactivation by a Novel MDM2 Inhibitor

Author

Guido Iaccarino, Daniela Sorriento, S Bendinelli, Eleonora Da Pozzo, P Gabelloni, Pietro Campiglia, Simona Daniele, Carmine Del Giudice, Alessia Bertamino, Fabrizio Scatena, Renato Vanacore, Claudia Martini, Barbara Costa, Isabel Gomez-Monterrey, Ettore Novellino, Costa, B, Bendinelli, S, Gabelloni, P, Da Pozzo, E, Daniele, S, Scatena, F, Vanacore, R, Campiglia, P, Bertamino, A, Gomez-Monterrey, I, Sorriento, D, Del Giudice, C, Iaccarino, G, Novellino, E, and Martini, C.

Subjects

Indoles, Cell cycle checkpoint, p53-MDM2 interaction, lcsh:Medicine, Apoptosis, Biochemistry, Mice, Drug Discovery, Molecular Cell Biology, Basic Cancer Research, lcsh:Science, Neurological Tumors, Mice, Inbred BALB C, Multidisciplinary, Cell Death, biology, Brain Neoplasms, Proto-Oncogene Proteins c-mdm2, Tumor Burden, Gene Expression Regulation, Neoplastic, Oncology, Medicine, Mdm2, Female, Signal transduction, Protein Binding, Signal Transduction, Research Article, medicine.drug, Drugs and Devices, Drug Research and Development, Mice, Nude, Antineoplastic Agents, Small Molecule Libraries, Inhibitory Concentration 50, In vivo, medicine, Animals, Humans, Spiro Compounds, Viability assay, Biology, Cell Proliferation, Temozolomide, Cell growth, lcsh:R, Cancers and Neoplasms, Xenograft Model Antitumor Assays, Molecular biology, Small Molecules, biology.protein, Cancer research, lcsh:Q, Tumor Suppressor Protein p53, Glioblastoma, Glioblastoma Multiforme

Abstract

Cancer development and chemo-resistance are often due to impaired functioning of the p53 tumor suppressor through genetic mutation or sequestration by other proteins. In glioblastoma multiforme (GBM), p53 availability is frequently reduced because it binds to the Murine Double Minute-2 (MDM2) oncoprotein, which accumulates at high concentrations in tumor cells. The use of MDM2 inhibitors that interfere with the binding of p53 and MDM2 has become a valid approach to inhibit cell growth in a number of cancers; however little is known about the efficacy of these inhibitors in GBM. We report that a new small-molecule inhibitor of MDM2 with a spirooxoindolepyrrolidine core structure, named ISA27, effectively reactivated p53 function and inhibited human GBM cell growth in vitro by inducing cell cycle arrest and apoptosis. In immunoincompetent BALB/c nude mice bearing a human GBM xenograft, the administration of ISA27 in vivo activated p53, inhibited cell proliferation and induced apoptosis in tumor tissue. Significantly, ISA27 was non-toxic in an in vitro normal human cell model and an in vivo mouse model. ISA27 administration in combination with temozolomide (TMZ) produced a synergistic inhibitory effect on GBM cell viability in vitro, suggesting the possibility of lowering the dose of TMZ used in the treatment of GBM. In conclusion, our data show that ISA27 releases the powerful antitumor capacities of p53 in GBM cells. The use of this MDM2 inhibitor could become a novel therapy for the treatment of GBM patients.

Published

2013