Glutathione depletion sensitizes cisplatin- and temozolomide-resistant glioma cells in vitro and in vivo.

dc.contributor.authorRocha, Clarissa Ribeiro Reily
dc.contributor.authorGarcia, Camila Carrião Machado
dc.contributor.authorVieira, Debora Braga
dc.contributor.authorQuinet, Annabel
dc.contributor.authorLima, Leonardo Carmo de Andrade
dc.contributor.authorMunford, Veridiana
dc.contributor.authorBelizário, José Ernesto
dc.contributor.authorMenck, Carlos Frederico Martins
dc.date.accessioned2015-09-22T19:06:46Z
dc.date.available2015-09-22T19:06:46Z
dc.date.issued2014
dc.description.abstractMalignant glioma is a severe type of brain tumor with a poor prognosis and few options for therapy. The main chemotherapy protocol for this type of tumor is based on temozolomide (TMZ), albeit with limited success. Cisplatin is widely used to treat several types of tumor and, in association with TMZ, is also used to treat recurrent glioma. However, several mechanisms of cellular resistance to cisplatin restrict therapy efficiency. In that sense, enhanced DNA repair, high glutathione levels and functional p53 have a critical role on cisplatin resistance. In this work, we explored several mechanisms of cisplatin resistance in human glioma. We showed that cellular survival was independent of the p53 status of those cells. In addition, in a host-cell reactivation assay using cisplatin-treated plasmid, we did not detect any difference in DNA repair capacity. We demonstrated that cisplatin-treated U138MG cells suffered fewer DNA double-strand breaks and DNA platination. Interestingly, the resistant cells carried higher levels of intracellular glutathione. Thus, preincubation with the glutathione inhibitor buthionine sulfoximine (BSO) induced massive cell death, whereas N-acetyl cysteine, a precursor of glutathione synthesis, improved the resistance to cisplatin treatment. In addition, BSO sensitized glioma cells to TMZ alone or in combination with cisplatin. Furthermore, using an in vivo model the combination of BSO, cisplatin and TMZ activated the caspase 3–7 apoptotic pathway. Remarkably, the combined treatment did not lead to severe side effects, while causing a huge impact on tumor progression. In fact, we noted a remarkable threefold increase in survival rate compared with other treatment regimens. Thus, the intracellular glutathione concentration is a potential molecular marker for cisplatin resistance in glioma, and the use of glutathione inhibitors, such as BSO, in association with cisplatin and TMZ seems a promising approach for the therapy of such devastating tumors.pt_BR
dc.identifier.citationROCHA, C. R. R. et al. Glutathione depletion sensitizes cisplatin- and temozolomide-resistant glioma cells in vitro and in vivo. Cell Death & Disease, v. 5, p. e1505, 2014. Disponível em: <https://www.nature.com/articles/cddis2014465>. Acesso em: 22 maio 2015.pt_BR
dc.identifier.doihttps://doi.org/10.1038/cddis.2014.465
dc.identifier.issn2041-4889
dc.identifier.urihttp://www.repositorio.ufop.br/handle/123456789/5611
dc.language.isoen_USpt_BR
dc.rights.licenseThis work is licensed under a Creative Commons Attribution 4.0 International Licence. Fonte: o próprio artigo.pt_BR
dc.titleGlutathione depletion sensitizes cisplatin- and temozolomide-resistant glioma cells in vitro and in vivo.pt_BR
dc.typeArtigo publicado em periodicopt_BR

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