In vivo and in vitro invasion in relation to phenotypic characteristics of human colorectal carcinoma cells.

In this study we investigated the tumorigenicity, growth pattern and spontaneous metastatic ability of a series of nine human colorectal carcinoma cell lines after subcutaneous and intracaecal xenografting in nude mice. CaCo2 cells were found to be poorly tumorigenic to non-tumorigenic in either sit...

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Autores principales: de Vries, J. E., Dinjens, W. N., De Bruyne, G. K., Verspaget, H. W., van der Linden, E. P., de Bruïne, A. P., Mareel, M. M., Bosman, F. T., ten Kate, J.
Formato: Texto
Lenguaje:English
Publicado: Nature Publishing Group 1995
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2033572/
https://www.ncbi.nlm.nih.gov/pubmed/7841040
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author de Vries, J. E.
Dinjens, W. N.
De Bruyne, G. K.
Verspaget, H. W.
van der Linden, E. P.
de Bruïne, A. P.
Mareel, M. M.
Bosman, F. T.
ten Kate, J.
author_facet de Vries, J. E.
Dinjens, W. N.
De Bruyne, G. K.
Verspaget, H. W.
van der Linden, E. P.
de Bruïne, A. P.
Mareel, M. M.
Bosman, F. T.
ten Kate, J.
author_sort de Vries, J. E.
collection PubMed
description In this study we investigated the tumorigenicity, growth pattern and spontaneous metastatic ability of a series of nine human colorectal carcinoma cell lines after subcutaneous and intracaecal xenografting in nude mice. CaCo2 cells were found to be poorly tumorigenic to non-tumorigenic in either site; the other cell lines were tumorigenic in both sites. SW1116, SW480 and SW620 did not show local invasive in the NCI-H716 and LS174T cells were both invasive in the caecum, but only NCI-H716 was invasive in the subcutis. HT29 and 5583 (S and E) cells were invasive in the caecum and from that site metastatic to the lungs and/or the liver. HT29 and 5583S cells were both invasive in the subcutis, but 5583E cells were not. Of each category of in vivo behaviour in the caecum, one cell line was further investigated with regard to invasion in vitro (into embryonic chick heart fragments), E-cadherin expression in vivo and in vitro and in vitro production of u-PA and t-PA. These parameters were chosen in view of their purported role in extracellular matrix degradation and intercellular adhesion, which are all involved in the invasive and metastatic cascade. Invasion in vitro was not predictive for invasion or metastasis in vivo. In the cell line which showed invasion in embryonic chick heart tissue, heterogeneous E-cadherin expression was observed in vitro together with a relatively high production of u-PA. The non-invasive cell lines showed in vitro homogeneous expression of E-cadherin with a relatively low production of u-PA. In vivo expression of E-cadherin was either absent or heterogeneous. We conclude that: (1) colorectal carcinoma xenografts show site-specific modification of in vivo invasive and metastatic behaviour; (2) invasion in vitro does not correlate with invasion and metastasis in vivo; (3) in vitro non-invasion might be associated with homogeneous E-cadherin expression and low production of u-PA; (4) E-cadherin expression in vitro differs from E-cadherin expression in vivo. The results support the notion that the microenvironment in which cancer cells grow is one of the factors involved in the regulation of invasive and metastatic behaviour. IMAGES:
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spelling pubmed-20335722009-09-10 In vivo and in vitro invasion in relation to phenotypic characteristics of human colorectal carcinoma cells. de Vries, J. E. Dinjens, W. N. De Bruyne, G. K. Verspaget, H. W. van der Linden, E. P. de Bruïne, A. P. Mareel, M. M. Bosman, F. T. ten Kate, J. Br J Cancer Research Article In this study we investigated the tumorigenicity, growth pattern and spontaneous metastatic ability of a series of nine human colorectal carcinoma cell lines after subcutaneous and intracaecal xenografting in nude mice. CaCo2 cells were found to be poorly tumorigenic to non-tumorigenic in either site; the other cell lines were tumorigenic in both sites. SW1116, SW480 and SW620 did not show local invasive in the NCI-H716 and LS174T cells were both invasive in the caecum, but only NCI-H716 was invasive in the subcutis. HT29 and 5583 (S and E) cells were invasive in the caecum and from that site metastatic to the lungs and/or the liver. HT29 and 5583S cells were both invasive in the subcutis, but 5583E cells were not. Of each category of in vivo behaviour in the caecum, one cell line was further investigated with regard to invasion in vitro (into embryonic chick heart fragments), E-cadherin expression in vivo and in vitro and in vitro production of u-PA and t-PA. These parameters were chosen in view of their purported role in extracellular matrix degradation and intercellular adhesion, which are all involved in the invasive and metastatic cascade. Invasion in vitro was not predictive for invasion or metastasis in vivo. In the cell line which showed invasion in embryonic chick heart tissue, heterogeneous E-cadherin expression was observed in vitro together with a relatively high production of u-PA. The non-invasive cell lines showed in vitro homogeneous expression of E-cadherin with a relatively low production of u-PA. In vivo expression of E-cadherin was either absent or heterogeneous. We conclude that: (1) colorectal carcinoma xenografts show site-specific modification of in vivo invasive and metastatic behaviour; (2) invasion in vitro does not correlate with invasion and metastasis in vivo; (3) in vitro non-invasion might be associated with homogeneous E-cadherin expression and low production of u-PA; (4) E-cadherin expression in vitro differs from E-cadherin expression in vivo. The results support the notion that the microenvironment in which cancer cells grow is one of the factors involved in the regulation of invasive and metastatic behaviour. IMAGES: Nature Publishing Group 1995-02 /pmc/articles/PMC2033572/ /pubmed/7841040 Text en https://creativecommons.org/licenses/by/4.0/This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit https://creativecommons.org/licenses/by/4.0/.
spellingShingle Research Article
de Vries, J. E.
Dinjens, W. N.
De Bruyne, G. K.
Verspaget, H. W.
van der Linden, E. P.
de Bruïne, A. P.
Mareel, M. M.
Bosman, F. T.
ten Kate, J.
In vivo and in vitro invasion in relation to phenotypic characteristics of human colorectal carcinoma cells.
title In vivo and in vitro invasion in relation to phenotypic characteristics of human colorectal carcinoma cells.
title_full In vivo and in vitro invasion in relation to phenotypic characteristics of human colorectal carcinoma cells.
title_fullStr In vivo and in vitro invasion in relation to phenotypic characteristics of human colorectal carcinoma cells.
title_full_unstemmed In vivo and in vitro invasion in relation to phenotypic characteristics of human colorectal carcinoma cells.
title_short In vivo and in vitro invasion in relation to phenotypic characteristics of human colorectal carcinoma cells.
title_sort in vivo and in vitro invasion in relation to phenotypic characteristics of human colorectal carcinoma cells.
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2033572/
https://www.ncbi.nlm.nih.gov/pubmed/7841040
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