Vascularized Tissue-Engineered Model for Studying Drug Resistance in Neuroblastoma

Neuroblastoma is a vascularized pediatric tumor derived from neural crest stem cells that displays vasculogenic mimicry and can express a number of stemness markers, such as SOX2 and NANOG. Tumor relapse is the major cause of succumbing to this disease, and properties attributed to cancer stem-like...

Descripción completa

Detalles Bibliográficos
Autores principales: Villasante, A., Sakaguchi, K., Kim, J., Cheung, N.K., Nakayama, M., Parsa, H., Okano, T., Shimizu, T., Vunjak-Novakovic, G.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2017
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5695000/
https://www.ncbi.nlm.nih.gov/pubmed/29158813
http://dx.doi.org/10.7150/thno.20730
_version_ 1783280234725900288
author Villasante, A.
Sakaguchi, K.
Kim, J.
Cheung, N.K.
Nakayama, M.
Parsa, H.
Okano, T.
Shimizu, T.
Vunjak-Novakovic, G.
author_facet Villasante, A.
Sakaguchi, K.
Kim, J.
Cheung, N.K.
Nakayama, M.
Parsa, H.
Okano, T.
Shimizu, T.
Vunjak-Novakovic, G.
author_sort Villasante, A.
collection PubMed
description Neuroblastoma is a vascularized pediatric tumor derived from neural crest stem cells that displays vasculogenic mimicry and can express a number of stemness markers, such as SOX2 and NANOG. Tumor relapse is the major cause of succumbing to this disease, and properties attributed to cancer stem-like cells (CSLC), such as drug-resistance and cell plasticity, seem to be the key mechanisms. However, the lack of controllable models that recapitulate the features of human neuroblastoma limits our understanding of the process and impedes the development of new therapies. In response to these limitations, we engineered a perfusable, vascularized in vitro model of three-dimensional human neuroblastoma to study the effects of retinoid therapy on tumor vasculature and drug-resistance. METHODS: The in vitro model of neuroblastoma was generated using cell-sheet engineering and cultured in a perfusion bioreactor. Firstly, we stacked three cell sheets containing SKNBE(2) neuroblastoma cells and HUVEC. Then, a vascular bed made of fibrin, collagen I and HUVEC cells was placed onto a collagen-gel base with 8 microchannels. After gelling, the stacked cell sheets were placed on the vascular bed and cultured in the perfusion bioreactor (perfusion rate: 0.5 mL/min) for 4 days. Neuroblastoma models were treated with 10μM isotretionin in single daily doses for 5 days. RESULTS: The bioengineered model recapitulated vasculogenic mimicry (vessel-like structure formation and tumor-derived endothelial cells-TECs), and contained CSLC expressing SOX2 and NANOG. Treatment with Isotretinoin destabilized vascular networks but failed to target vasculogenic mimicry and augmented populations of CSLCs expressing high levels of SOX2. Our results suggest that CSLCs can transdifferentiate into drug resistant CD31(+)-TECs, and reveal the presence of an intermediate state STEC (stem tumor-derived endothelial cell) expressing both SOX2 and CD31. CONCLUSION: Our results reveal some roles of SOX2 in drug resistance and tumor relapse, and suggest that SOX2 could be a therapeutic target in neuroblastoma.
format Online
Article
Text
id pubmed-5695000
institution National Center for Biotechnology Information
language English
publishDate 2017
publisher Ivyspring International Publisher
record_format MEDLINE/PubMed
spelling pubmed-56950002017-11-20 Vascularized Tissue-Engineered Model for Studying Drug Resistance in Neuroblastoma Villasante, A. Sakaguchi, K. Kim, J. Cheung, N.K. Nakayama, M. Parsa, H. Okano, T. Shimizu, T. Vunjak-Novakovic, G. Theranostics Research Paper Neuroblastoma is a vascularized pediatric tumor derived from neural crest stem cells that displays vasculogenic mimicry and can express a number of stemness markers, such as SOX2 and NANOG. Tumor relapse is the major cause of succumbing to this disease, and properties attributed to cancer stem-like cells (CSLC), such as drug-resistance and cell plasticity, seem to be the key mechanisms. However, the lack of controllable models that recapitulate the features of human neuroblastoma limits our understanding of the process and impedes the development of new therapies. In response to these limitations, we engineered a perfusable, vascularized in vitro model of three-dimensional human neuroblastoma to study the effects of retinoid therapy on tumor vasculature and drug-resistance. METHODS: The in vitro model of neuroblastoma was generated using cell-sheet engineering and cultured in a perfusion bioreactor. Firstly, we stacked three cell sheets containing SKNBE(2) neuroblastoma cells and HUVEC. Then, a vascular bed made of fibrin, collagen I and HUVEC cells was placed onto a collagen-gel base with 8 microchannels. After gelling, the stacked cell sheets were placed on the vascular bed and cultured in the perfusion bioreactor (perfusion rate: 0.5 mL/min) for 4 days. Neuroblastoma models were treated with 10μM isotretionin in single daily doses for 5 days. RESULTS: The bioengineered model recapitulated vasculogenic mimicry (vessel-like structure formation and tumor-derived endothelial cells-TECs), and contained CSLC expressing SOX2 and NANOG. Treatment with Isotretinoin destabilized vascular networks but failed to target vasculogenic mimicry and augmented populations of CSLCs expressing high levels of SOX2. Our results suggest that CSLCs can transdifferentiate into drug resistant CD31(+)-TECs, and reveal the presence of an intermediate state STEC (stem tumor-derived endothelial cell) expressing both SOX2 and CD31. CONCLUSION: Our results reveal some roles of SOX2 in drug resistance and tumor relapse, and suggest that SOX2 could be a therapeutic target in neuroblastoma. Ivyspring International Publisher 2017-09-21 /pmc/articles/PMC5695000/ /pubmed/29158813 http://dx.doi.org/10.7150/thno.20730 Text en © Ivyspring International Publisher This is an open access article distributed under the terms of the Creative Commons Attribution (CC BY-NC) license (https://creativecommons.org/licenses/by-nc/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Villasante, A.
Sakaguchi, K.
Kim, J.
Cheung, N.K.
Nakayama, M.
Parsa, H.
Okano, T.
Shimizu, T.
Vunjak-Novakovic, G.
Vascularized Tissue-Engineered Model for Studying Drug Resistance in Neuroblastoma
title Vascularized Tissue-Engineered Model for Studying Drug Resistance in Neuroblastoma
title_full Vascularized Tissue-Engineered Model for Studying Drug Resistance in Neuroblastoma
title_fullStr Vascularized Tissue-Engineered Model for Studying Drug Resistance in Neuroblastoma
title_full_unstemmed Vascularized Tissue-Engineered Model for Studying Drug Resistance in Neuroblastoma
title_short Vascularized Tissue-Engineered Model for Studying Drug Resistance in Neuroblastoma
title_sort vascularized tissue-engineered model for studying drug resistance in neuroblastoma
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5695000/
https://www.ncbi.nlm.nih.gov/pubmed/29158813
http://dx.doi.org/10.7150/thno.20730
work_keys_str_mv AT villasantea vascularizedtissueengineeredmodelforstudyingdrugresistanceinneuroblastoma
AT sakaguchik vascularizedtissueengineeredmodelforstudyingdrugresistanceinneuroblastoma
AT kimj vascularizedtissueengineeredmodelforstudyingdrugresistanceinneuroblastoma
AT cheungnk vascularizedtissueengineeredmodelforstudyingdrugresistanceinneuroblastoma
AT nakayamam vascularizedtissueengineeredmodelforstudyingdrugresistanceinneuroblastoma
AT parsah vascularizedtissueengineeredmodelforstudyingdrugresistanceinneuroblastoma
AT okanot vascularizedtissueengineeredmodelforstudyingdrugresistanceinneuroblastoma
AT shimizut vascularizedtissueengineeredmodelforstudyingdrugresistanceinneuroblastoma
AT vunjaknovakovicg vascularizedtissueengineeredmodelforstudyingdrugresistanceinneuroblastoma

Ejemplares similares