Bone Morphogenetic Protein Pathway Antagonism by Grem1 Regulates Epithelial Cell Fate in Intestinal Regeneration

BACKGROUND & AIMS: In homeostasis, intestinal cell fate is controlled by balanced gradients of morphogen signaling. The bone morphogenetic protein (BMP) pathway has a physiological, prodifferentiation role, predominantly inferred through previous experimental pathway inactivation. Intestinal reg...

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Autores principales: Koppens, Martijn A. J., Davis, Hayley, Valbuena, Gabriel N., Mulholland, Eoghan J., Nasreddin, Nadia, Colombe, Mathilde, Antanaviciute, Agne, Biswas, Sujata, Friedrich, Matthias, Lee, Lennard, Wang, Lai Mun, Koelzer, Viktor H., East, James E., Simmons, Alison, Winton, Douglas J., Leedham, Simon J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2021
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7613733/
https://www.ncbi.nlm.nih.gov/pubmed/33819486
http://dx.doi.org/10.1053/j.gastro.2021.03.052
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author Koppens, Martijn A. J.
Davis, Hayley
Valbuena, Gabriel N.
Mulholland, Eoghan J.
Nasreddin, Nadia
Colombe, Mathilde
Antanaviciute, Agne
Biswas, Sujata
Friedrich, Matthias
Lee, Lennard
Wang, Lai Mun
Koelzer, Viktor H.
East, James E.
Simmons, Alison
Winton, Douglas J.
Leedham, Simon J.
author_facet Koppens, Martijn A. J.
Davis, Hayley
Valbuena, Gabriel N.
Mulholland, Eoghan J.
Nasreddin, Nadia
Colombe, Mathilde
Antanaviciute, Agne
Biswas, Sujata
Friedrich, Matthias
Lee, Lennard
Wang, Lai Mun
Koelzer, Viktor H.
East, James E.
Simmons, Alison
Winton, Douglas J.
Leedham, Simon J.
author_sort Koppens, Martijn A. J.
collection PubMed
description BACKGROUND & AIMS: In homeostasis, intestinal cell fate is controlled by balanced gradients of morphogen signaling. The bone morphogenetic protein (BMP) pathway has a physiological, prodifferentiation role, predominantly inferred through previous experimental pathway inactivation. Intestinal regeneration is underpinned by dedifferentiation and cell plasticity, but the signaling pathways that regulate this adaptive reprogramming are not well understood. We assessed the BMP signaling landscape and investigated the impact and therapeutic potential of pathway manipulation in homeostasis and regeneration. [Figure: see text] METHODS: A novel mouse model was generated to assess the effect of the autocrine Bmp4 ligand on individual secretory cell fate. We spatio-temporally mapped BMP signaling in mouse and human regenerating intestine. Transgenic models were used to explore the functional impact of pathway manipulation on stem cell fate and intestinal regeneration. RESULTS: In homeostasis, ligand exposure reduced proliferation, expedited terminal differentiation, abrogated secretory cell survival, and prevented dedifferentiation. After ulceration, physiological attenuation of BMP signaling arose through upregulation of the secreted antagonist Grem1 from topographically distinct populations of fibroblasts. Concomitant expression supported functional compensation after Grem1 deletion from tissue-resident cells. BMP pathway manipulation showed that antagonist-mediated BMP attenuation was obligatory but functionally submaximal, because regeneration was impaired or enhanced by epithelial overexpression of Bmp4 or Grem1, respectively. Mechanistically, Bmp4 abrogated regenerative stem cell reprogramming despite a convergent impact of YAP/TAZ on cell fate in remodeled wounds. CONCLUSIONS: BMP signaling prevents epithelial dedifferentiation, and pathway attenuation through stromal Grem1 upregulation was required for adaptive reprogramming in intestinal regeneration. This intercompartmental antagonism was functionally submaximal, raising the possibility of therapeutic pathway manipulation in inflammatory bowel disease.
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spelling pubmed-76137332022-10-23 Bone Morphogenetic Protein Pathway Antagonism by Grem1 Regulates Epithelial Cell Fate in Intestinal Regeneration Koppens, Martijn A. J. Davis, Hayley Valbuena, Gabriel N. Mulholland, Eoghan J. Nasreddin, Nadia Colombe, Mathilde Antanaviciute, Agne Biswas, Sujata Friedrich, Matthias Lee, Lennard Wang, Lai Mun Koelzer, Viktor H. East, James E. Simmons, Alison Winton, Douglas J. Leedham, Simon J. Gastroenterology Article BACKGROUND & AIMS: In homeostasis, intestinal cell fate is controlled by balanced gradients of morphogen signaling. The bone morphogenetic protein (BMP) pathway has a physiological, prodifferentiation role, predominantly inferred through previous experimental pathway inactivation. Intestinal regeneration is underpinned by dedifferentiation and cell plasticity, but the signaling pathways that regulate this adaptive reprogramming are not well understood. We assessed the BMP signaling landscape and investigated the impact and therapeutic potential of pathway manipulation in homeostasis and regeneration. [Figure: see text] METHODS: A novel mouse model was generated to assess the effect of the autocrine Bmp4 ligand on individual secretory cell fate. We spatio-temporally mapped BMP signaling in mouse and human regenerating intestine. Transgenic models were used to explore the functional impact of pathway manipulation on stem cell fate and intestinal regeneration. RESULTS: In homeostasis, ligand exposure reduced proliferation, expedited terminal differentiation, abrogated secretory cell survival, and prevented dedifferentiation. After ulceration, physiological attenuation of BMP signaling arose through upregulation of the secreted antagonist Grem1 from topographically distinct populations of fibroblasts. Concomitant expression supported functional compensation after Grem1 deletion from tissue-resident cells. BMP pathway manipulation showed that antagonist-mediated BMP attenuation was obligatory but functionally submaximal, because regeneration was impaired or enhanced by epithelial overexpression of Bmp4 or Grem1, respectively. Mechanistically, Bmp4 abrogated regenerative stem cell reprogramming despite a convergent impact of YAP/TAZ on cell fate in remodeled wounds. CONCLUSIONS: BMP signaling prevents epithelial dedifferentiation, and pathway attenuation through stromal Grem1 upregulation was required for adaptive reprogramming in intestinal regeneration. This intercompartmental antagonism was functionally submaximal, raising the possibility of therapeutic pathway manipulation in inflammatory bowel disease. 2021-07-01 2021-04-02 /pmc/articles/PMC7613733/ /pubmed/33819486 http://dx.doi.org/10.1053/j.gastro.2021.03.052 Text en https://creativecommons.org/licenses/by/4.0/This work is licensed under a CC BY 4.0 (https://creativecommons.org/licenses/by/4.0/) International license.
spellingShingle Article
Koppens, Martijn A. J.
Davis, Hayley
Valbuena, Gabriel N.
Mulholland, Eoghan J.
Nasreddin, Nadia
Colombe, Mathilde
Antanaviciute, Agne
Biswas, Sujata
Friedrich, Matthias
Lee, Lennard
Wang, Lai Mun
Koelzer, Viktor H.
East, James E.
Simmons, Alison
Winton, Douglas J.
Leedham, Simon J.
Bone Morphogenetic Protein Pathway Antagonism by Grem1 Regulates Epithelial Cell Fate in Intestinal Regeneration
title Bone Morphogenetic Protein Pathway Antagonism by Grem1 Regulates Epithelial Cell Fate in Intestinal Regeneration
title_full Bone Morphogenetic Protein Pathway Antagonism by Grem1 Regulates Epithelial Cell Fate in Intestinal Regeneration
title_fullStr Bone Morphogenetic Protein Pathway Antagonism by Grem1 Regulates Epithelial Cell Fate in Intestinal Regeneration
title_full_unstemmed Bone Morphogenetic Protein Pathway Antagonism by Grem1 Regulates Epithelial Cell Fate in Intestinal Regeneration
title_short Bone Morphogenetic Protein Pathway Antagonism by Grem1 Regulates Epithelial Cell Fate in Intestinal Regeneration
title_sort bone morphogenetic protein pathway antagonism by grem1 regulates epithelial cell fate in intestinal regeneration
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7613733/
https://www.ncbi.nlm.nih.gov/pubmed/33819486
http://dx.doi.org/10.1053/j.gastro.2021.03.052
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