In vitro and in vivo analysis of RTK inhibitor efficacy and identification of its novel targets in glioblastomas

Detalhes bibliográficos
Autor(a) principal: Martinho, Olga
Data de Publicação: 2013
Outros Autores: Oliveira, Renato José Silva, Gonçalves, Vera M., Clara, Carlos, Almeida, José Reynaldo, Carvalho, André Lopes, Barata, João Taborda, Reis, R. M.
Tipo de documento: Artigo
Idioma: eng
Título da fonte: Repositório Científico de Acesso Aberto de Portugal (Repositórios Cientìficos)
Texto Completo: http://hdl.handle.net/1822/25541
Resumo: Treatment for glioblastoma consists of radiotherapy and temozolomide-based chemotherapy. However, virtually all patients recur, leading to a fatal outcome. Receptor tyrosine kinase (RTK)-targeted therapy has been the focus of attention in novel treatment options for these patients. Here, we compared the efficacy of imatinib, sunitinib, and cediranib in glioblastoma models. In the present work, the biologic effect of the drugs was screened by viability, cell cycle, apoptosis, migration, and invasion in vitro assays or in vivo by chick chorioallantoic membrane assay. Intracellular signaling was assessed by Western blot and the RTK targets were identified using phospho-RTK arrays. The amplified status of KIT, PDGFRA, and VEGFR2 genes was assessed by quantitative polymerase chain reaction. In a panel of 10 glioblastoma cell lines, we showed that cediranib was the most potent. In addition, cediranib and sunitinib synergistically sensitize the cells to temozolomide. Cediranib efficacy was shown to associate with higher cytostatic and unique cytotoxic effects in vitro and both antitumoral and antiangiogenic activity in vivo, which could associate with its great capacity to inhibit mitogen-activated protein kinase (MAPK) and AKT pathways. The molecular status of KIT, PDGFRA, and VEGFR2 did not predict glioblastoma cell responsiveness to any of the RTK inhibitors. Importantly, phospho-RTK arrays revealed novel targets for cediranib and sunitinib therapy. In conclusion, the novel targets found may be of value as future biomarkers for therapy response in glioblastoma and lead to the rational selection of patients for effective molecular targeted treatment.
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spelling In vitro and in vivo analysis of RTK inhibitor efficacy and identification of its novel targets in glioblastomasScience & TechnologyTreatment for glioblastoma consists of radiotherapy and temozolomide-based chemotherapy. However, virtually all patients recur, leading to a fatal outcome. Receptor tyrosine kinase (RTK)-targeted therapy has been the focus of attention in novel treatment options for these patients. Here, we compared the efficacy of imatinib, sunitinib, and cediranib in glioblastoma models. In the present work, the biologic effect of the drugs was screened by viability, cell cycle, apoptosis, migration, and invasion in vitro assays or in vivo by chick chorioallantoic membrane assay. Intracellular signaling was assessed by Western blot and the RTK targets were identified using phospho-RTK arrays. The amplified status of KIT, PDGFRA, and VEGFR2 genes was assessed by quantitative polymerase chain reaction. In a panel of 10 glioblastoma cell lines, we showed that cediranib was the most potent. In addition, cediranib and sunitinib synergistically sensitize the cells to temozolomide. Cediranib efficacy was shown to associate with higher cytostatic and unique cytotoxic effects in vitro and both antitumoral and antiangiogenic activity in vivo, which could associate with its great capacity to inhibit mitogen-activated protein kinase (MAPK) and AKT pathways. The molecular status of KIT, PDGFRA, and VEGFR2 did not predict glioblastoma cell responsiveness to any of the RTK inhibitors. Importantly, phospho-RTK arrays revealed novel targets for cediranib and sunitinib therapy. In conclusion, the novel targets found may be of value as future biomarkers for therapy response in glioblastoma and lead to the rational selection of patients for effective molecular targeted treatment.This work was funded by Fundacao para a Ciencia e Tecnologia (FCT, Portugal; Project PTDC/SAU-TOX/114549/2009) and by Pfizer/Sociedade de Ciencias Medicas de Lisboa with the award "Research in Oncology Diseases, Prof. Francisco Gentil." Olga Martinho is a recipient of a PhD fellowship (SFRH/BD/36463/2007), and Vera Miranda-Goncalves is a recipient of a research fellowship (SFRH/BI/33503/2008), both from FCT. Andre Lopes Carvalho has a Brazilian National Council for Scientific and Technological Development Scholarship (CNPq, 313181/2009-8).TransoncUniversidade do MinhoMartinho, OlgaOliveira, Renato José SilvaGonçalves, Vera M.Clara, CarlosAlmeida, José ReynaldoCarvalho, André LopesBarata, João TabordaReis, R. M.2013-10-042013-10-04T00:00:00Zinfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/articleapplication/pdfhttp://hdl.handle.net/1822/25541eng1936-523310.1593/tlo.12400http://www.transonc.com/index.phpinfo:eu-repo/semantics/openAccessreponame:Repositório Científico de Acesso Aberto de Portugal (Repositórios Cientìficos)instname:Agência para a Sociedade do Conhecimento (UMIC) - FCT - Sociedade da Informaçãoinstacron:RCAAP2023-07-21T12:08:03Zoai:repositorium.sdum.uminho.pt:1822/25541Portal AgregadorONGhttps://www.rcaap.pt/oai/openaireopendoar:71602024-03-19T18:59:09.927857Repositório Científico de Acesso Aberto de Portugal (Repositórios Cientìficos) - Agência para a Sociedade do Conhecimento (UMIC) - FCT - Sociedade da Informaçãofalse
dc.title.none.fl_str_mv In vitro and in vivo analysis of RTK inhibitor efficacy and identification of its novel targets in glioblastomas
title In vitro and in vivo analysis of RTK inhibitor efficacy and identification of its novel targets in glioblastomas
spellingShingle In vitro and in vivo analysis of RTK inhibitor efficacy and identification of its novel targets in glioblastomas
Martinho, Olga
Science & Technology
title_short In vitro and in vivo analysis of RTK inhibitor efficacy and identification of its novel targets in glioblastomas
title_full In vitro and in vivo analysis of RTK inhibitor efficacy and identification of its novel targets in glioblastomas
title_fullStr In vitro and in vivo analysis of RTK inhibitor efficacy and identification of its novel targets in glioblastomas
title_full_unstemmed In vitro and in vivo analysis of RTK inhibitor efficacy and identification of its novel targets in glioblastomas
title_sort In vitro and in vivo analysis of RTK inhibitor efficacy and identification of its novel targets in glioblastomas
author Martinho, Olga
author_facet Martinho, Olga
Oliveira, Renato José Silva
Gonçalves, Vera M.
Clara, Carlos
Almeida, José Reynaldo
Carvalho, André Lopes
Barata, João Taborda
Reis, R. M.
author_role author
author2 Oliveira, Renato José Silva
Gonçalves, Vera M.
Clara, Carlos
Almeida, José Reynaldo
Carvalho, André Lopes
Barata, João Taborda
Reis, R. M.
author2_role author
author
author
author
author
author
author
dc.contributor.none.fl_str_mv Universidade do Minho
dc.contributor.author.fl_str_mv Martinho, Olga
Oliveira, Renato José Silva
Gonçalves, Vera M.
Clara, Carlos
Almeida, José Reynaldo
Carvalho, André Lopes
Barata, João Taborda
Reis, R. M.
dc.subject.por.fl_str_mv Science & Technology
topic Science & Technology
description Treatment for glioblastoma consists of radiotherapy and temozolomide-based chemotherapy. However, virtually all patients recur, leading to a fatal outcome. Receptor tyrosine kinase (RTK)-targeted therapy has been the focus of attention in novel treatment options for these patients. Here, we compared the efficacy of imatinib, sunitinib, and cediranib in glioblastoma models. In the present work, the biologic effect of the drugs was screened by viability, cell cycle, apoptosis, migration, and invasion in vitro assays or in vivo by chick chorioallantoic membrane assay. Intracellular signaling was assessed by Western blot and the RTK targets were identified using phospho-RTK arrays. The amplified status of KIT, PDGFRA, and VEGFR2 genes was assessed by quantitative polymerase chain reaction. In a panel of 10 glioblastoma cell lines, we showed that cediranib was the most potent. In addition, cediranib and sunitinib synergistically sensitize the cells to temozolomide. Cediranib efficacy was shown to associate with higher cytostatic and unique cytotoxic effects in vitro and both antitumoral and antiangiogenic activity in vivo, which could associate with its great capacity to inhibit mitogen-activated protein kinase (MAPK) and AKT pathways. The molecular status of KIT, PDGFRA, and VEGFR2 did not predict glioblastoma cell responsiveness to any of the RTK inhibitors. Importantly, phospho-RTK arrays revealed novel targets for cediranib and sunitinib therapy. In conclusion, the novel targets found may be of value as future biomarkers for therapy response in glioblastoma and lead to the rational selection of patients for effective molecular targeted treatment.
publishDate 2013
dc.date.none.fl_str_mv 2013-10-04
2013-10-04T00:00:00Z
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publisher.none.fl_str_mv Transonc
dc.source.none.fl_str_mv reponame:Repositório Científico de Acesso Aberto de Portugal (Repositórios Cientìficos)
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