Intestinal tumorigenesis initiated by dedifferentiation and acquisition of stem-cell-like properties

Sarah Schwitalla; Alexander A. Fingerle; Patrizia Cammareri; Tim Nebelsiek; Serkan I. Göktuna; Paul K. Ziegler; Ozge Canli; Jarom Heijmans; David J. Huels; Guenievre Moreaux; Rudolf A. Rupec; Markus Gerhard; Roland Schmid; Nick Barker; Hans Clevers; Roland Lang; Jens Neumann; Thomas Kirchner; Makoto M. Taketo; Gijs R. van den Brink; Owen J. Sansom; Melek C. Arkan; Florian R. Greten

doi:https://doi.org/10.1016/j.cell.2012.12.012

Intestinal tumorigenesis initiated by dedifferentiation and acquisition of stem-cell-like properties

Sarah Schwitalla, Alexander A. Fingerle, Patrizia Cammareri, Tim Nebelsiek, Serkan I. Göktuna, Paul K. Ziegler, Ozge Canli, Jarom Heijmans, David J. Huels, Guenievre Moreaux, Rudolf A. Rupec, Markus Gerhard, Roland Schmid, Nick Barker, Hans Clevers, Roland Lang, Jens Neumann, Thomas Kirchner, Makoto M. Taketo, Gijs R. van den BrinkOwen J. Sansom, Melek C. Arkan, Florian R. Greten

Research output: Contribution to journal › Article › Academic › peer-review

828 Citations (Scopus)

Abstract

Cell-type plasticity within a tumor has recently been suggested to cause a bidirectional conversion between tumor-initiating stem cells and nonstem cells triggered by an inflammatory stroma. NF-κB represents a key transcription factor within the inflammatory tumor microenvironment. However, NF-κB's function in tumor-initiating cells has not been examined yet. Using a genetic model of intestinal epithelial cell (IEC)-restricted constitutive Wnt-activation, which comprises the most common event in the initiation of colon cancer, we demonstrate that NF-κB modulates Wnt signaling and show that IEC-specific ablation of RelA/p65 retards crypt stem cell expansion. In contrast, elevated NF-κB signaling enhances Wnt activation and induces dedifferentiation of nonstem cells that acquire tumor-initiating capacity. Thus, our data support the concept of bidirectional conversion and highlight the importance of inflammatory signaling for dedifferentiation and generation of tumor-initiating cells in vivo

Original language	English
Pages (from-to)	25-38
Journal	Cell
Volume	152
Issue number	1-2
DOIs	https://doi.org/10.1016/j.cell.2012.12.012
Publication status	Published - 2013

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https://doi.org/10.1016/j.cell.2012.12.012

Cite this

Schwitalla, S., Fingerle, A. A., Cammareri, P., Nebelsiek, T., Göktuna, S. I., Ziegler, P. K., Canli, O., Heijmans, J., Huels, D. J., Moreaux, G., Rupec, R. A., Gerhard, M., Schmid, R., Barker, N., Clevers, H., Lang, R., Neumann, J., Kirchner, T., Taketo, M. M., ... Greten, F. R. (2013). Intestinal tumorigenesis initiated by dedifferentiation and acquisition of stem-cell-like properties. Cell, 152(1-2), 25-38. https://doi.org/10.1016/j.cell.2012.12.012

@article{921a2eb4c5bd4dda8babade6507c0630,

title = "Intestinal tumorigenesis initiated by dedifferentiation and acquisition of stem-cell-like properties",

abstract = "Cell-type plasticity within a tumor has recently been suggested to cause a bidirectional conversion between tumor-initiating stem cells and nonstem cells triggered by an inflammatory stroma. NF-κB represents a key transcription factor within the inflammatory tumor microenvironment. However, NF-κB's function in tumor-initiating cells has not been examined yet. Using a genetic model of intestinal epithelial cell (IEC)-restricted constitutive Wnt-activation, which comprises the most common event in the initiation of colon cancer, we demonstrate that NF-κB modulates Wnt signaling and show that IEC-specific ablation of RelA/p65 retards crypt stem cell expansion. In contrast, elevated NF-κB signaling enhances Wnt activation and induces dedifferentiation of nonstem cells that acquire tumor-initiating capacity. Thus, our data support the concept of bidirectional conversion and highlight the importance of inflammatory signaling for dedifferentiation and generation of tumor-initiating cells in vivo",

author = "Sarah Schwitalla and Fingerle, {Alexander A.} and Patrizia Cammareri and Tim Nebelsiek and G{\"o}ktuna, {Serkan I.} and Ziegler, {Paul K.} and Ozge Canli and Jarom Heijmans and Huels, {David J.} and Guenievre Moreaux and Rupec, {Rudolf A.} and Markus Gerhard and Roland Schmid and Nick Barker and Hans Clevers and Roland Lang and Jens Neumann and Thomas Kirchner and Taketo, {Makoto M.} and {van den Brink}, {Gijs R.} and Sansom, {Owen J.} and Arkan, {Melek C.} and Greten, {Florian R.}",

year = "2013",

doi = "https://doi.org/10.1016/j.cell.2012.12.012",

language = "English",

volume = "152",

pages = "25--38",

journal = "Cell",

issn = "0092-8674",

publisher = "Cell Press",

number = "1-2",

}

Schwitalla, S, Fingerle, AA, Cammareri, P, Nebelsiek, T, Göktuna, SI, Ziegler, PK, Canli, O, Heijmans, J , Huels, DJ, Moreaux, G, Rupec, RA, Gerhard, M, Schmid, R, Barker, N, Clevers, H, Lang, R, Neumann, J, Kirchner, T, Taketo, MM, van den Brink, GR, Sansom, OJ, Arkan, MC & Greten, FR 2013, 'Intestinal tumorigenesis initiated by dedifferentiation and acquisition of stem-cell-like properties', Cell, vol. 152, no. 1-2, pp. 25-38. https://doi.org/10.1016/j.cell.2012.12.012

TY - JOUR

T1 - Intestinal tumorigenesis initiated by dedifferentiation and acquisition of stem-cell-like properties

AU - Schwitalla, Sarah

AU - Fingerle, Alexander A.

AU - Cammareri, Patrizia

AU - Nebelsiek, Tim

AU - Göktuna, Serkan I.

AU - Ziegler, Paul K.

AU - Canli, Ozge

AU - Heijmans, Jarom

AU - Huels, David J.

AU - Moreaux, Guenievre

AU - Rupec, Rudolf A.

AU - Gerhard, Markus

AU - Schmid, Roland

AU - Barker, Nick

AU - Clevers, Hans

AU - Lang, Roland

AU - Neumann, Jens

AU - Kirchner, Thomas

AU - Taketo, Makoto M.

AU - van den Brink, Gijs R.

AU - Sansom, Owen J.

AU - Arkan, Melek C.

AU - Greten, Florian R.

PY - 2013

Y1 - 2013

N2 - Cell-type plasticity within a tumor has recently been suggested to cause a bidirectional conversion between tumor-initiating stem cells and nonstem cells triggered by an inflammatory stroma. NF-κB represents a key transcription factor within the inflammatory tumor microenvironment. However, NF-κB's function in tumor-initiating cells has not been examined yet. Using a genetic model of intestinal epithelial cell (IEC)-restricted constitutive Wnt-activation, which comprises the most common event in the initiation of colon cancer, we demonstrate that NF-κB modulates Wnt signaling and show that IEC-specific ablation of RelA/p65 retards crypt stem cell expansion. In contrast, elevated NF-κB signaling enhances Wnt activation and induces dedifferentiation of nonstem cells that acquire tumor-initiating capacity. Thus, our data support the concept of bidirectional conversion and highlight the importance of inflammatory signaling for dedifferentiation and generation of tumor-initiating cells in vivo

AB - Cell-type plasticity within a tumor has recently been suggested to cause a bidirectional conversion between tumor-initiating stem cells and nonstem cells triggered by an inflammatory stroma. NF-κB represents a key transcription factor within the inflammatory tumor microenvironment. However, NF-κB's function in tumor-initiating cells has not been examined yet. Using a genetic model of intestinal epithelial cell (IEC)-restricted constitutive Wnt-activation, which comprises the most common event in the initiation of colon cancer, we demonstrate that NF-κB modulates Wnt signaling and show that IEC-specific ablation of RelA/p65 retards crypt stem cell expansion. In contrast, elevated NF-κB signaling enhances Wnt activation and induces dedifferentiation of nonstem cells that acquire tumor-initiating capacity. Thus, our data support the concept of bidirectional conversion and highlight the importance of inflammatory signaling for dedifferentiation and generation of tumor-initiating cells in vivo

U2 - https://doi.org/10.1016/j.cell.2012.12.012

DO - https://doi.org/10.1016/j.cell.2012.12.012

M3 - Article

C2 - 23273993

SN - 0092-8674

VL - 152

SP - 25

EP - 38

JO - Cell

JF - Cell

IS - 1-2

ER -