Utilize este identificador para referenciar este registo: https://hdl.handle.net/1822/49014

TítuloImpact of mesenchymal stem cells' secretome on glioblastoma pathophysiology
Autor(es)Castro, Joana Vieira de
Gomes, Eduardo Domingos Correia
Granja, Sara Costa
Anjo, Sandra I.
Baltazar, Fátima
Bruno Manadas
Salgado, A. J.
Costa, Bruno Marques
Palavras-chaveGlioblastoma
Mesenchymal stem cells
Human umbilical cord perivascular cells
Conditioned media
Secretome
Viability
Proliferation
Migration
Proteomics
Data2017
EditoraBioMed Central (BMC)
RevistaJournal of Translational Medicine
Resumo(s)Background: Glioblastoma (GBM) is a highly aggressive primary brain cancer, for which curative therapies are not available. An emerging therapeutic approach suggested to have potential to target malignant gliomas has been based on the use of multipotent mesenchymal stem cells (MSCs), either unmodified or engineered to deliver anticancer therapeutic agents, as these cells present an intrinsic capacity to migrate towards malignant tumors. Nevertheless, it is still controversial whether this innate tropism of MSCs towards the tumor area is associated with cancer promotion or suppression. Considering that one of the major mechanisms by which MSCs interact with and modulate tumor cells is via secreted factors, we studied how the secretome of MSCs modulates critical hallmark features of GBM cells. Methods: The effect of conditioned media (CM) from human umbilical cord perivascular cells (HUCPVCs, a MSC population present in the Wharton's jelly of the umbilical cord) on GBM cell viability, migration, proliferation and sensitivity to temozolomide treatment of U251 and SNB-19 GBM cells was evaluated. The in vivo chicken chorioallantoic membrane (CAM) assay was used to evaluate the effect of HUCPVCs CM on tumor growth and angiogenesis. The secretome of HUCPVCs was characterized by proteomic analyses. Results: We found that both tested GBM cell lines exposed to HUCPVCs CM presented significantly higher cellular viability, proliferation and migration. In contrast, resistance of GBM cells to temozolomide chemotherapy was not significantly affected by HUCPVCs CM. In the in vivo CAM assay, CM from HUCPVCs promoted U251 and SNB-19 tumor cells growth. Proteomic analysis to characterize the secretome of HUCPVCs identified several proteins involved in promotion of cell survival, proliferation and migration, revealing novel putative molecular mediators for the effects observed in GBM cells exposed to HUCPVCs CM. Conclusions: These findings provide novel insights to better understand the interplay between GBM cells and MSCs, raising awareness to potential safety issues regarding the use of MSCs as stem-cell based therapies for GBM.
TipoArtigo
URIhttps://hdl.handle.net/1822/49014
DOI10.1186/s12967-017-1303-8
ISSN1479-5876
Versão da editorahttps://www.ncbi.nlm.nih.gov/pmc/articles/PMC5625623/
Arbitragem científicayes
AcessoAcesso aberto
Aparece nas coleções:ICVS - Artigos em revistas internacionais / Papers in international journals

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