Wnt ligands influence tumour initiation by controlling the number of intestinal stem cells

D. J. Huels; L. Bruens; M. C. Hodder; P. Cammareri; A. D. Campbell; R. A. Ridgway; D. M. Gay; M. Solar-Abboud; W. J. Faller; C. Nixon; L. B. Zeiger; M. E. McLaughlin; E. Morrissey; D. J. Winton; H. J. Snippert; J. Van Rheenen; O. J. Sansom

doi:10.1038/s41467-018-03426-2

Wnt ligands influence tumour initiation by controlling the number of intestinal stem cells

D. J. Huels, L. Bruens, M. C. Hodder, P. Cammareri, A. D. Campbell, R. A. Ridgway, D. M. Gay, M. Solar-Abboud, W. J. Faller, C. Nixon, L. B. Zeiger, M. E. McLaughlin, E. Morrissey, D. J. Winton, H. J. Snippert, J. Van Rheenen, O. J. Sansom^*

^*Corresponding author for this work

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Abstract

Many epithelial stem cell populations follow a pattern of stochastic stem cell divisions called 'neutral drift'. It is hypothesised that neutral competition between stem cells protects against the acquisition of deleterious mutations. Here we use a Porcupine inhibitor to reduce Wnt secretion at a dose where intestinal homoeostasis is maintained despite a reduction of Lgr5+ stem cells. Functionally, there is a marked acceleration in monoclonal conversion, so that crypts become rapidly derived from a single stem cell. Stem cells located further from the base are lost and the pool of competing stem cells is reduced. We tested whether this loss of stem cell competition would modify tumorigenesis. Reduction of Wnt ligand secretion accelerates fixation of Apc-deficient cells within the crypt leading to accelerated tumorigenesis. Therefore, ligand-based Wnt signalling influences the number of stem cells, fixation speed of Apc mutations and the speed and likelihood of adenoma formation.

Original language	English
Article number	1132
Journal	Nature Communications
Volume	9
Issue number	1
DOIs	https://doi.org/10.1038/s41467-018-03426-2
Publication status	Published - 1 Dec 2018

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Huels, D. J., Bruens, L., Hodder, M. C., Cammareri, P., Campbell, A. D., Ridgway, R. A., Gay, D. M., Solar-Abboud, M., Faller, W. J., Nixon, C., Zeiger, L. B., McLaughlin, M. E., Morrissey, E., Winton, D. J., Snippert, H. J., Van Rheenen, J., & Sansom, O. J. (2018). Wnt ligands influence tumour initiation by controlling the number of intestinal stem cells. Nature Communications, 9(1), Article 1132. https://doi.org/10.1038/s41467-018-03426-2

@article{eab64faaaed344d4b01741aceb7a0b29,

title = "Wnt ligands influence tumour initiation by controlling the number of intestinal stem cells",

abstract = "Many epithelial stem cell populations follow a pattern of stochastic stem cell divisions called 'neutral drift'. It is hypothesised that neutral competition between stem cells protects against the acquisition of deleterious mutations. Here we use a Porcupine inhibitor to reduce Wnt secretion at a dose where intestinal homoeostasis is maintained despite a reduction of Lgr5+ stem cells. Functionally, there is a marked acceleration in monoclonal conversion, so that crypts become rapidly derived from a single stem cell. Stem cells located further from the base are lost and the pool of competing stem cells is reduced. We tested whether this loss of stem cell competition would modify tumorigenesis. Reduction of Wnt ligand secretion accelerates fixation of Apc-deficient cells within the crypt leading to accelerated tumorigenesis. Therefore, ligand-based Wnt signalling influences the number of stem cells, fixation speed of Apc mutations and the speed and likelihood of adenoma formation.",

author = "Huels, {D. J.} and L. Bruens and Hodder, {M. C.} and P. Cammareri and Campbell, {A. D.} and Ridgway, {R. A.} and Gay, {D. M.} and M. Solar-Abboud and Faller, {W. J.} and C. Nixon and Zeiger, {L. B.} and McLaughlin, {M. E.} and E. Morrissey and Winton, {D. J.} and Snippert, {H. J.} and {Van Rheenen}, J. and Sansom, {O. J.}",

note = "Funding Information: The research was supported by Cancer Research UK core grant C596/A17196 and grant to OS A12481, and D.J.H. was funded by the European Union Seventh Framework Programme FP7/2007-2013 under grant agreement number 278568. O.J.S. is funded by an ERC Starting grant COLONCAN under agreement number 311301. This work was financially supported by European Research Council Grant CANCER-RECURRENCE 648804 (to J.v.R.), by the CancerGenomics.nl http://CancerGenomics.nl (Netherlands Organisation for Scientific Research) program (to J.v.R.), by the Doctor Josef Steiner Foundation (to J.v.R) and by the European Union{\textquoteright}s Horizon 2020 research and innovation program under Marie Sklodowska-Curie grant agreement no. 642866 (to J.v.R). Publisher Copyright: {\textcopyright} 2018 The Author(s).",

year = "2018",

month = dec,

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doi = "10.1038/s41467-018-03426-2",

language = "English",

volume = "9",

journal = "Nature Communications",

issn = "2041-1723",

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Huels, DJ, Bruens, L, Hodder, MC, Cammareri, P, Campbell, AD, Ridgway, RA, Gay, DM, Solar-Abboud, M, Faller, WJ, Nixon, C, Zeiger, LB, McLaughlin, ME, Morrissey, E, Winton, DJ, Snippert, HJ , Van Rheenen, J & Sansom, OJ 2018, 'Wnt ligands influence tumour initiation by controlling the number of intestinal stem cells', Nature Communications, vol. 9, no. 1, 1132. https://doi.org/10.1038/s41467-018-03426-2

TY - JOUR

T1 - Wnt ligands influence tumour initiation by controlling the number of intestinal stem cells

AU - Huels, D. J.

AU - Bruens, L.

AU - Hodder, M. C.

AU - Cammareri, P.

AU - Campbell, A. D.

AU - Ridgway, R. A.

AU - Gay, D. M.

AU - Solar-Abboud, M.

AU - Faller, W. J.

AU - Nixon, C.

AU - Zeiger, L. B.

AU - McLaughlin, M. E.

AU - Morrissey, E.

AU - Winton, D. J.

AU - Snippert, H. J.

AU - Van Rheenen, J.

AU - Sansom, O. J.

N1 - Funding Information: The research was supported by Cancer Research UK core grant C596/A17196 and grant to OS A12481, and D.J.H. was funded by the European Union Seventh Framework Programme FP7/2007-2013 under grant agreement number 278568. O.J.S. is funded by an ERC Starting grant COLONCAN under agreement number 311301. This work was financially supported by European Research Council Grant CANCER-RECURRENCE 648804 (to J.v.R.), by the CancerGenomics.nl http://CancerGenomics.nl (Netherlands Organisation for Scientific Research) program (to J.v.R.), by the Doctor Josef Steiner Foundation (to J.v.R) and by the European Union’s Horizon 2020 research and innovation program under Marie Sklodowska-Curie grant agreement no. 642866 (to J.v.R). Publisher Copyright: © 2018 The Author(s).

PY - 2018/12/1

Y1 - 2018/12/1

N2 - Many epithelial stem cell populations follow a pattern of stochastic stem cell divisions called 'neutral drift'. It is hypothesised that neutral competition between stem cells protects against the acquisition of deleterious mutations. Here we use a Porcupine inhibitor to reduce Wnt secretion at a dose where intestinal homoeostasis is maintained despite a reduction of Lgr5+ stem cells. Functionally, there is a marked acceleration in monoclonal conversion, so that crypts become rapidly derived from a single stem cell. Stem cells located further from the base are lost and the pool of competing stem cells is reduced. We tested whether this loss of stem cell competition would modify tumorigenesis. Reduction of Wnt ligand secretion accelerates fixation of Apc-deficient cells within the crypt leading to accelerated tumorigenesis. Therefore, ligand-based Wnt signalling influences the number of stem cells, fixation speed of Apc mutations and the speed and likelihood of adenoma formation.

AB - Many epithelial stem cell populations follow a pattern of stochastic stem cell divisions called 'neutral drift'. It is hypothesised that neutral competition between stem cells protects against the acquisition of deleterious mutations. Here we use a Porcupine inhibitor to reduce Wnt secretion at a dose where intestinal homoeostasis is maintained despite a reduction of Lgr5+ stem cells. Functionally, there is a marked acceleration in monoclonal conversion, so that crypts become rapidly derived from a single stem cell. Stem cells located further from the base are lost and the pool of competing stem cells is reduced. We tested whether this loss of stem cell competition would modify tumorigenesis. Reduction of Wnt ligand secretion accelerates fixation of Apc-deficient cells within the crypt leading to accelerated tumorigenesis. Therefore, ligand-based Wnt signalling influences the number of stem cells, fixation speed of Apc mutations and the speed and likelihood of adenoma formation.

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U2 - 10.1038/s41467-018-03426-2

DO - 10.1038/s41467-018-03426-2

M3 - Article

AN - SCOPUS:85044193464

SN - 2041-1723

VL - 9

JO - Nature Communications

JF - Nature Communications

IS - 1

M1 - 1132

ER -

Wnt ligands influence tumour initiation by controlling the number of intestinal stem cells

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