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

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

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) oncopr...

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Main Authors: 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, Claudia Martini
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3747081?pdf=render
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spelling doaj-ac32b651c0df4a3b83aaca38b9579f5e2020-11-25T01:45:49ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0188e7228110.1371/journal.pone.0072281Human glioblastoma multiforme: p53 reactivation by a novel MDM2 inhibitor.Barbara CostaSara BendinelliPamela GabelloniEleonora Da PozzoSimona DanieleFabrizio ScatenaRenato VanacorePietro CampigliaAlessia BertaminoIsabel Gomez-MonterreyDaniela SorrientoCarmine Del GiudiceGuido IaccarinoEttore NovellinoClaudia MartiniCancer 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.http://europepmc.org/articles/PMC3747081?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
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
Claudia Martini
spellingShingle 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
Claudia Martini
Human glioblastoma multiforme: p53 reactivation by a novel MDM2 inhibitor.
PLoS ONE
author_facet 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
Claudia Martini
author_sort Barbara Costa
title Human glioblastoma multiforme: p53 reactivation by a novel MDM2 inhibitor.
title_short Human glioblastoma multiforme: p53 reactivation by a novel MDM2 inhibitor.
title_full Human glioblastoma multiforme: p53 reactivation by a novel MDM2 inhibitor.
title_fullStr Human glioblastoma multiforme: p53 reactivation by a novel MDM2 inhibitor.
title_full_unstemmed Human glioblastoma multiforme: p53 reactivation by a novel MDM2 inhibitor.
title_sort human glioblastoma multiforme: p53 reactivation by a novel mdm2 inhibitor.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description 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.
url http://europepmc.org/articles/PMC3747081?pdf=render
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