MCL1 Is Required for Maintenance of Intestinal Homeostasis and Prevention of Carcinogenesis in Mice

BACKGROUND & AIMS: Intestinal epithelial homeostasis depends on a tightly regulated balance between intestinal epithelial cell (IEC) death and proliferation. While the disruption of several IEC death regulating factors result in intestinal inflammation, the loss of the anti-apoptotic BCL2 family...

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Autores principales: Healy, Marc E., Boege, Yannick, Hodder, Michael C., Böhm, Friederike, Malehmir, Mohsen, Scherr, Anna-Lena, Jetzer, Jasna, Chan, Lap Kwan, Parrotta, Rossella, Jacobs, Kurt, Clerbaux, Laure-Alix, Kreutzer, Susanne, Campbell, Andrew, Gilchrist, Ella, Gilroy, Kathryn, Rodewald, Ann-Katrin, Honcharova-Biletska, Hanna, Schimmer, Roman, Vélez, Karelia, Büeler, Simone, Cammareri, Patrizia, Kalna, Gabriela, Wenning, Anna S., McCoy, Kathy D., Gomez de Agüero, Mercedes, Schulze-Bergkamen, Henning, Klose, Christoph S.N., Unger, Kristian, Macpherson, Andrew J., Moor, Andreas E., Köhler, Bruno, Sansom, Owen J., Heikenwälder, Mathias, Weber, Achim
Formato: Online Artículo Texto
Lenguaje:English
Publicado: W.B. Saunders 2020
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7397524/
https://www.ncbi.nlm.nih.gov/pubmed/32179094
http://dx.doi.org/10.1053/j.gastro.2020.03.017
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author Healy, Marc E.
Boege, Yannick
Hodder, Michael C.
Böhm, Friederike
Malehmir, Mohsen
Scherr, Anna-Lena
Jetzer, Jasna
Chan, Lap Kwan
Parrotta, Rossella
Jacobs, Kurt
Clerbaux, Laure-Alix
Kreutzer, Susanne
Campbell, Andrew
Gilchrist, Ella
Gilroy, Kathryn
Rodewald, Ann-Katrin
Honcharova-Biletska, Hanna
Schimmer, Roman
Vélez, Karelia
Büeler, Simone
Cammareri, Patrizia
Kalna, Gabriela
Wenning, Anna S.
McCoy, Kathy D.
Gomez de Agüero, Mercedes
Schulze-Bergkamen, Henning
Klose, Christoph S.N.
Unger, Kristian
Macpherson, Andrew J.
Moor, Andreas E.
Köhler, Bruno
Sansom, Owen J.
Heikenwälder, Mathias
Weber, Achim
author_facet Healy, Marc E.
Boege, Yannick
Hodder, Michael C.
Böhm, Friederike
Malehmir, Mohsen
Scherr, Anna-Lena
Jetzer, Jasna
Chan, Lap Kwan
Parrotta, Rossella
Jacobs, Kurt
Clerbaux, Laure-Alix
Kreutzer, Susanne
Campbell, Andrew
Gilchrist, Ella
Gilroy, Kathryn
Rodewald, Ann-Katrin
Honcharova-Biletska, Hanna
Schimmer, Roman
Vélez, Karelia
Büeler, Simone
Cammareri, Patrizia
Kalna, Gabriela
Wenning, Anna S.
McCoy, Kathy D.
Gomez de Agüero, Mercedes
Schulze-Bergkamen, Henning
Klose, Christoph S.N.
Unger, Kristian
Macpherson, Andrew J.
Moor, Andreas E.
Köhler, Bruno
Sansom, Owen J.
Heikenwälder, Mathias
Weber, Achim
author_sort Healy, Marc E.
collection PubMed
description BACKGROUND & AIMS: Intestinal epithelial homeostasis depends on a tightly regulated balance between intestinal epithelial cell (IEC) death and proliferation. While the disruption of several IEC death regulating factors result in intestinal inflammation, the loss of the anti-apoptotic BCL2 family members BCL2 and BCL2L1 has no effect on intestinal homeostasis in mice. We investigated the functions of the antiapoptotic protein MCL1, another member of the BCL2 family, in intestinal homeostasis in mice. METHODS: We generated mice with IEC-specific disruption of Mcl1 (Mcl1(ΔIEC) mice) or tamoxifen-inducible IEC-specific disruption of Mcl1 (i-Mcl1(ΔIEC) mice); these mice and mice with full-length Mcl1 (controls) were raised under normal or germ-free conditions. Mice were analyzed by endoscopy and for intestinal epithelial barrier permeability. Intestinal tissues were analyzed by histology, in situ hybridization, proliferation assays, and immunoblots. Levels of calprotectin, a marker of intestinal inflammation, were measured in intestinal tissues and feces. RESULTS: Mcl1(ΔIEC) mice spontaneously developed apoptotic enterocolopathy, characterized by increased IEC apoptosis, hyperproliferative crypts, epithelial barrier dysfunction, and chronic inflammation. Loss of MCL1 retained intestinal crypts in a hyperproliferated state and prevented the differentiation of intestinal stem cells. Proliferation of intestinal stem cells in MCL1-deficient mice required WNT signaling and was associated with DNA damage accumulation. By 1 year of age, Mcl1(ΔIEC) mice developed intestinal tumors with morphologic and genetic features of human adenomas and carcinomas. Germ-free housing of Mcl1(ΔIEC) mice reduced markers of microbiota-induced intestinal inflammation but not tumor development. CONCLUSION: The antiapoptotic protein MCL1, a member of the BCL2 family, is required for maintenance of intestinal homeostasis and prevention of carcinogenesis in mice. Loss of MCL1 results in development of intestinal carcinomas, even under germ-free conditions, and therefore does not involve microbe-induced chronic inflammation. Mcl1(ΔIEC) mice might be used to study apoptotic enterocolopathy and inflammatory bowel diseases.
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spelling pubmed-73975242020-08-06 MCL1 Is Required for Maintenance of Intestinal Homeostasis and Prevention of Carcinogenesis in Mice Healy, Marc E. Boege, Yannick Hodder, Michael C. Böhm, Friederike Malehmir, Mohsen Scherr, Anna-Lena Jetzer, Jasna Chan, Lap Kwan Parrotta, Rossella Jacobs, Kurt Clerbaux, Laure-Alix Kreutzer, Susanne Campbell, Andrew Gilchrist, Ella Gilroy, Kathryn Rodewald, Ann-Katrin Honcharova-Biletska, Hanna Schimmer, Roman Vélez, Karelia Büeler, Simone Cammareri, Patrizia Kalna, Gabriela Wenning, Anna S. McCoy, Kathy D. Gomez de Agüero, Mercedes Schulze-Bergkamen, Henning Klose, Christoph S.N. Unger, Kristian Macpherson, Andrew J. Moor, Andreas E. Köhler, Bruno Sansom, Owen J. Heikenwälder, Mathias Weber, Achim Gastroenterology Article BACKGROUND & AIMS: Intestinal epithelial homeostasis depends on a tightly regulated balance between intestinal epithelial cell (IEC) death and proliferation. While the disruption of several IEC death regulating factors result in intestinal inflammation, the loss of the anti-apoptotic BCL2 family members BCL2 and BCL2L1 has no effect on intestinal homeostasis in mice. We investigated the functions of the antiapoptotic protein MCL1, another member of the BCL2 family, in intestinal homeostasis in mice. METHODS: We generated mice with IEC-specific disruption of Mcl1 (Mcl1(ΔIEC) mice) or tamoxifen-inducible IEC-specific disruption of Mcl1 (i-Mcl1(ΔIEC) mice); these mice and mice with full-length Mcl1 (controls) were raised under normal or germ-free conditions. Mice were analyzed by endoscopy and for intestinal epithelial barrier permeability. Intestinal tissues were analyzed by histology, in situ hybridization, proliferation assays, and immunoblots. Levels of calprotectin, a marker of intestinal inflammation, were measured in intestinal tissues and feces. RESULTS: Mcl1(ΔIEC) mice spontaneously developed apoptotic enterocolopathy, characterized by increased IEC apoptosis, hyperproliferative crypts, epithelial barrier dysfunction, and chronic inflammation. Loss of MCL1 retained intestinal crypts in a hyperproliferated state and prevented the differentiation of intestinal stem cells. Proliferation of intestinal stem cells in MCL1-deficient mice required WNT signaling and was associated with DNA damage accumulation. By 1 year of age, Mcl1(ΔIEC) mice developed intestinal tumors with morphologic and genetic features of human adenomas and carcinomas. Germ-free housing of Mcl1(ΔIEC) mice reduced markers of microbiota-induced intestinal inflammation but not tumor development. CONCLUSION: The antiapoptotic protein MCL1, a member of the BCL2 family, is required for maintenance of intestinal homeostasis and prevention of carcinogenesis in mice. Loss of MCL1 results in development of intestinal carcinomas, even under germ-free conditions, and therefore does not involve microbe-induced chronic inflammation. Mcl1(ΔIEC) mice might be used to study apoptotic enterocolopathy and inflammatory bowel diseases. W.B. Saunders 2020-07 /pmc/articles/PMC7397524/ /pubmed/32179094 http://dx.doi.org/10.1053/j.gastro.2020.03.017 Text en © 2020 The Authors http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Article
Healy, Marc E.
Boege, Yannick
Hodder, Michael C.
Böhm, Friederike
Malehmir, Mohsen
Scherr, Anna-Lena
Jetzer, Jasna
Chan, Lap Kwan
Parrotta, Rossella
Jacobs, Kurt
Clerbaux, Laure-Alix
Kreutzer, Susanne
Campbell, Andrew
Gilchrist, Ella
Gilroy, Kathryn
Rodewald, Ann-Katrin
Honcharova-Biletska, Hanna
Schimmer, Roman
Vélez, Karelia
Büeler, Simone
Cammareri, Patrizia
Kalna, Gabriela
Wenning, Anna S.
McCoy, Kathy D.
Gomez de Agüero, Mercedes
Schulze-Bergkamen, Henning
Klose, Christoph S.N.
Unger, Kristian
Macpherson, Andrew J.
Moor, Andreas E.
Köhler, Bruno
Sansom, Owen J.
Heikenwälder, Mathias
Weber, Achim
MCL1 Is Required for Maintenance of Intestinal Homeostasis and Prevention of Carcinogenesis in Mice
title MCL1 Is Required for Maintenance of Intestinal Homeostasis and Prevention of Carcinogenesis in Mice
title_full MCL1 Is Required for Maintenance of Intestinal Homeostasis and Prevention of Carcinogenesis in Mice
title_fullStr MCL1 Is Required for Maintenance of Intestinal Homeostasis and Prevention of Carcinogenesis in Mice
title_full_unstemmed MCL1 Is Required for Maintenance of Intestinal Homeostasis and Prevention of Carcinogenesis in Mice
title_short MCL1 Is Required for Maintenance of Intestinal Homeostasis and Prevention of Carcinogenesis in Mice
title_sort mcl1 is required for maintenance of intestinal homeostasis and prevention of carcinogenesis in mice
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7397524/
https://www.ncbi.nlm.nih.gov/pubmed/32179094
http://dx.doi.org/10.1053/j.gastro.2020.03.017
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