Colorectal cancer derived organotypic spheroids maintain essential tissue characteristics but adapt their metabolism in culture

BACKGROUND: Organotypic tumor spheroids, a 3D in vitro model derived from patient tumor material, preserve tissue heterogeneity and retain structural tissue elements, thus replicating the in vivo tumor more closely than commonly used 2D and 3D cell line models. Such structures harbour tumorigenic ce...

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Autores principales: Rajcevic, Uros, Knol, Jaco C, Piersma, Sander, Bougnaud, Sébastien, Fack, Fred, Sundlisaeter, Eirik, Søndenaa, Karl, Myklebust, Reidar, Pham, Thang V, Niclou, Simone P, Jiménez, Connie R
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2014
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4114130/
https://www.ncbi.nlm.nih.gov/pubmed/25075203
http://dx.doi.org/10.1186/1477-5956-12-39
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author Rajcevic, Uros
Knol, Jaco C
Piersma, Sander
Bougnaud, Sébastien
Fack, Fred
Sundlisaeter, Eirik
Søndenaa, Karl
Myklebust, Reidar
Pham, Thang V
Niclou, Simone P
Jiménez, Connie R
author_facet Rajcevic, Uros
Knol, Jaco C
Piersma, Sander
Bougnaud, Sébastien
Fack, Fred
Sundlisaeter, Eirik
Søndenaa, Karl
Myklebust, Reidar
Pham, Thang V
Niclou, Simone P
Jiménez, Connie R
author_sort Rajcevic, Uros
collection PubMed
description BACKGROUND: Organotypic tumor spheroids, a 3D in vitro model derived from patient tumor material, preserve tissue heterogeneity and retain structural tissue elements, thus replicating the in vivo tumor more closely than commonly used 2D and 3D cell line models. Such structures harbour tumorigenic cells, as revealed by xenograft implantation studies in animal models and maintain the genetic makeup of the original tumor material. The aim of our work was a morphological and proteomic characterization of organotypic spheroids derived from colorectal cancer tissue in order to get insight into their composition and associated biology. RESULTS: Morphological analysis showed that spheroids were of about 250 μm in size and varied in structure, while the spheroid cells differed in shape and size and were tightly packed together by desmosomes and tight junctions. Our proteomic data revealed significant alterations in protein expression in organotypic tumor spheroids cultured as primary explants compared to primary colorectal cancer tissue. Components underlying cellular and tissue architecture were changed; nuclear DNA/ chromatin maintenance systems were up-regulated, whereas various mitochondrial components were down-regulated in spheroids. Most interestingly, the mesenchymal cells appear to be substantial component in such cellular assemblies. Thus the observed changes may partly occur in this cellular compartment. Finally, in the proteomics analysis stem cell-like characteristics were observed within the spheroid cellular assembly, reflected by accumulation of Alcam, Ctnnb1, Aldh1, Gpx2, and CD166. These findings were underlined by IHC analysis of Ctnnb1, CD24 and CD44, therefore warranting closer investigation of the tumorigenic compartment in this 3D culture model for tumor tissue. CONCLUSIONS: Our analysis of organotypic CRC tumor spheroids has identified biological processes associated with a mixture of cell types and states, including protein markers for mesenchymal and stem-like cells. This 3D tumor model in which tumor heterogeneity is preserved may represent an advantageous model system to investigate novel therapeutic approaches.
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spelling pubmed-41141302014-07-30 Colorectal cancer derived organotypic spheroids maintain essential tissue characteristics but adapt their metabolism in culture Rajcevic, Uros Knol, Jaco C Piersma, Sander Bougnaud, Sébastien Fack, Fred Sundlisaeter, Eirik Søndenaa, Karl Myklebust, Reidar Pham, Thang V Niclou, Simone P Jiménez, Connie R Proteome Sci Research BACKGROUND: Organotypic tumor spheroids, a 3D in vitro model derived from patient tumor material, preserve tissue heterogeneity and retain structural tissue elements, thus replicating the in vivo tumor more closely than commonly used 2D and 3D cell line models. Such structures harbour tumorigenic cells, as revealed by xenograft implantation studies in animal models and maintain the genetic makeup of the original tumor material. The aim of our work was a morphological and proteomic characterization of organotypic spheroids derived from colorectal cancer tissue in order to get insight into their composition and associated biology. RESULTS: Morphological analysis showed that spheroids were of about 250 μm in size and varied in structure, while the spheroid cells differed in shape and size and were tightly packed together by desmosomes and tight junctions. Our proteomic data revealed significant alterations in protein expression in organotypic tumor spheroids cultured as primary explants compared to primary colorectal cancer tissue. Components underlying cellular and tissue architecture were changed; nuclear DNA/ chromatin maintenance systems were up-regulated, whereas various mitochondrial components were down-regulated in spheroids. Most interestingly, the mesenchymal cells appear to be substantial component in such cellular assemblies. Thus the observed changes may partly occur in this cellular compartment. Finally, in the proteomics analysis stem cell-like characteristics were observed within the spheroid cellular assembly, reflected by accumulation of Alcam, Ctnnb1, Aldh1, Gpx2, and CD166. These findings were underlined by IHC analysis of Ctnnb1, CD24 and CD44, therefore warranting closer investigation of the tumorigenic compartment in this 3D culture model for tumor tissue. CONCLUSIONS: Our analysis of organotypic CRC tumor spheroids has identified biological processes associated with a mixture of cell types and states, including protein markers for mesenchymal and stem-like cells. This 3D tumor model in which tumor heterogeneity is preserved may represent an advantageous model system to investigate novel therapeutic approaches. BioMed Central 2014-07-11 /pmc/articles/PMC4114130/ /pubmed/25075203 http://dx.doi.org/10.1186/1477-5956-12-39 Text en Copyright © 2014 Rajcevic et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly credited. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research
Rajcevic, Uros
Knol, Jaco C
Piersma, Sander
Bougnaud, Sébastien
Fack, Fred
Sundlisaeter, Eirik
Søndenaa, Karl
Myklebust, Reidar
Pham, Thang V
Niclou, Simone P
Jiménez, Connie R
Colorectal cancer derived organotypic spheroids maintain essential tissue characteristics but adapt their metabolism in culture
title Colorectal cancer derived organotypic spheroids maintain essential tissue characteristics but adapt their metabolism in culture
title_full Colorectal cancer derived organotypic spheroids maintain essential tissue characteristics but adapt their metabolism in culture
title_fullStr Colorectal cancer derived organotypic spheroids maintain essential tissue characteristics but adapt their metabolism in culture
title_full_unstemmed Colorectal cancer derived organotypic spheroids maintain essential tissue characteristics but adapt their metabolism in culture
title_short Colorectal cancer derived organotypic spheroids maintain essential tissue characteristics but adapt their metabolism in culture
title_sort colorectal cancer derived organotypic spheroids maintain essential tissue characteristics but adapt their metabolism in culture
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4114130/
https://www.ncbi.nlm.nih.gov/pubmed/25075203
http://dx.doi.org/10.1186/1477-5956-12-39
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