Tumorigenic fragments of APC cause dominant defects in directional cell migration in multiple model systems

Nonsense mutations that result in the expression of truncated, N-terminal, fragments of the adenomatous polyposis coli (APC) tumour suppressor protein are found in most sporadic and some hereditary colorectal cancers. These mutations can cause tumorigenesis by eliminating β-catenin-binding sites fro...

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Autores principales: Nelson, Scott A., Li, Zhouyu, Newton, Ian P., Fraser, David, Milne, Rachel E., Martin, David M. A., Schiffmann, David, Yang, Xuesong, Dormann, Dirk, Weijer, Cornelis J., Appleton, Paul L., Näthke, Inke S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Company of Biologists Limited 2012
Materias:
Research Report
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3484875/
https://www.ncbi.nlm.nih.gov/pubmed/22563063
http://dx.doi.org/10.1242/dmm.008607
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author Nelson, Scott A.
Li, Zhouyu
Newton, Ian P.
Fraser, David
Milne, Rachel E.
Martin, David M. A.
Schiffmann, David
Yang, Xuesong
Dormann, Dirk
Weijer, Cornelis J.
Appleton, Paul L.
Näthke, Inke S.
author_facet Nelson, Scott A.
Li, Zhouyu
Newton, Ian P.
Fraser, David
Milne, Rachel E.
Martin, David M. A.
Schiffmann, David
Yang, Xuesong
Dormann, Dirk
Weijer, Cornelis J.
Appleton, Paul L.
Näthke, Inke S.
author_sort Nelson, Scott A.
collection PubMed
description Nonsense mutations that result in the expression of truncated, N-terminal, fragments of the adenomatous polyposis coli (APC) tumour suppressor protein are found in most sporadic and some hereditary colorectal cancers. These mutations can cause tumorigenesis by eliminating β-catenin-binding sites from APC, which leads to upregulation of β-catenin and thereby results in the induction of oncogenes such as MYC. Here we show that, in three distinct experimental model systems, expression of an N-terminal fragment of APC (N-APC) results in loss of directionality, but not speed, of cell motility independently of changes in β-catenin regulation. We developed a system to culture and fluorescently label live pieces of gut tissue to record high-resolution three-dimensional time-lapse movies of cells in situ. This revealed an unexpected complexity of normal gut cell migration, a key process in gut epithelial maintenance, with cells moving with spatial and temporal discontinuity. Quantitative comparison of gut tissue from wild-type mice and APC heterozygotes (APC(Min/+); multiple intestinal neoplasia model) demonstrated that cells in precancerous epithelia lack directional preference when moving along the crypt-villus axis. This effect was reproduced in diverse experimental systems: in developing chicken embryos, mesoderm cells expressing N-APC failed to migrate normally; in amoeboid Dictyostelium, which lack endogenous APC, expressing an N-APC fragment maintained cell motility, but the cells failed to perform directional chemotaxis; and multicellular Dictyostelium slug aggregates similarly failed to perform phototaxis. We propose that N-terminal fragments of APC represent a gain-of-function mutation that causes cells within tissue to fail to migrate directionally in response to relevant guidance cues. Consistent with this idea, crypts in histologically normal tissues of APC(Min/+) intestines are overpopulated with cells, suggesting that a lack of migration might cause cell accumulation in a precancerous state.
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spelling pubmed-34848752012-11-16 Tumorigenic fragments of APC cause dominant defects in directional cell migration in multiple model systems Nelson, Scott A. Li, Zhouyu Newton, Ian P. Fraser, David Milne, Rachel E. Martin, David M. A. Schiffmann, David Yang, Xuesong Dormann, Dirk Weijer, Cornelis J. Appleton, Paul L. Näthke, Inke S. Dis Model Mech Research Report Nonsense mutations that result in the expression of truncated, N-terminal, fragments of the adenomatous polyposis coli (APC) tumour suppressor protein are found in most sporadic and some hereditary colorectal cancers. These mutations can cause tumorigenesis by eliminating β-catenin-binding sites from APC, which leads to upregulation of β-catenin and thereby results in the induction of oncogenes such as MYC. Here we show that, in three distinct experimental model systems, expression of an N-terminal fragment of APC (N-APC) results in loss of directionality, but not speed, of cell motility independently of changes in β-catenin regulation. We developed a system to culture and fluorescently label live pieces of gut tissue to record high-resolution three-dimensional time-lapse movies of cells in situ. This revealed an unexpected complexity of normal gut cell migration, a key process in gut epithelial maintenance, with cells moving with spatial and temporal discontinuity. Quantitative comparison of gut tissue from wild-type mice and APC heterozygotes (APC(Min/+); multiple intestinal neoplasia model) demonstrated that cells in precancerous epithelia lack directional preference when moving along the crypt-villus axis. This effect was reproduced in diverse experimental systems: in developing chicken embryos, mesoderm cells expressing N-APC failed to migrate normally; in amoeboid Dictyostelium, which lack endogenous APC, expressing an N-APC fragment maintained cell motility, but the cells failed to perform directional chemotaxis; and multicellular Dictyostelium slug aggregates similarly failed to perform phototaxis. We propose that N-terminal fragments of APC represent a gain-of-function mutation that causes cells within tissue to fail to migrate directionally in response to relevant guidance cues. Consistent with this idea, crypts in histologically normal tissues of APC(Min/+) intestines are overpopulated with cells, suggesting that a lack of migration might cause cell accumulation in a precancerous state. The Company of Biologists Limited 2012-11 2012-04-05 /pmc/articles/PMC3484875/ /pubmed/22563063 http://dx.doi.org/10.1242/dmm.008607 Text en © 2012. Published by The Company of Biologists Ltd This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial Share Alike License (http://creativecommons.org/licenses/by-nc-sa/3.0), which permits unrestricted non-commercial use, distribution and reproduction in any medium provided that the original work is properly cited and all further distributions of the work or adaptation are subject to the same Creative Commons License terms.
spellingShingle Research Report
Nelson, Scott A.
Li, Zhouyu
Newton, Ian P.
Fraser, David
Milne, Rachel E.
Martin, David M. A.
Schiffmann, David
Yang, Xuesong
Dormann, Dirk
Weijer, Cornelis J.
Appleton, Paul L.
Näthke, Inke S.
Tumorigenic fragments of APC cause dominant defects in directional cell migration in multiple model systems
title Tumorigenic fragments of APC cause dominant defects in directional cell migration in multiple model systems
title_full Tumorigenic fragments of APC cause dominant defects in directional cell migration in multiple model systems
title_fullStr Tumorigenic fragments of APC cause dominant defects in directional cell migration in multiple model systems
title_full_unstemmed Tumorigenic fragments of APC cause dominant defects in directional cell migration in multiple model systems
title_short Tumorigenic fragments of APC cause dominant defects in directional cell migration in multiple model systems
title_sort tumorigenic fragments of apc cause dominant defects in directional cell migration in multiple model systems
topic Research Report
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3484875/
https://www.ncbi.nlm.nih.gov/pubmed/22563063
http://dx.doi.org/10.1242/dmm.008607
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