MECOM permits pancreatic acinar cell dedifferentiation avoiding cell death under stress conditions

Maintenance of the pancreatic acinar cell phenotype suppresses tumor formation. Hence, repetitive acute or chronic pancreatitis, stress conditions in which the acinar cells dedifferentiate, predispose for cancer formation in the pancreas. Dedifferentiated acinar cells acquire a large panel of duct c...

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Autores principales: Backx, Elyne, Wauters, Elke, Baldan, Jonathan, Van Bulck, Mathias, Michiels, Ellis, Heremans, Yves, De Paep, Diedert Luc, Kurokawa, Mineo, Goyama, Susumu, Bouwens, Luc, Jacquemin, Patrick, Houbracken, Isabelle, Rooman, Ilse
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group UK 2021
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8408219/
https://www.ncbi.nlm.nih.gov/pubmed/33762742
http://dx.doi.org/10.1038/s41418-021-00771-6
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author Backx, Elyne
Wauters, Elke
Baldan, Jonathan
Van Bulck, Mathias
Michiels, Ellis
Heremans, Yves
De Paep, Diedert Luc
Kurokawa, Mineo
Goyama, Susumu
Bouwens, Luc
Jacquemin, Patrick
Houbracken, Isabelle
Rooman, Ilse
author_facet Backx, Elyne
Wauters, Elke
Baldan, Jonathan
Van Bulck, Mathias
Michiels, Ellis
Heremans, Yves
De Paep, Diedert Luc
Kurokawa, Mineo
Goyama, Susumu
Bouwens, Luc
Jacquemin, Patrick
Houbracken, Isabelle
Rooman, Ilse
author_sort Backx, Elyne
collection PubMed
description Maintenance of the pancreatic acinar cell phenotype suppresses tumor formation. Hence, repetitive acute or chronic pancreatitis, stress conditions in which the acinar cells dedifferentiate, predispose for cancer formation in the pancreas. Dedifferentiated acinar cells acquire a large panel of duct cell-specific markers. However, it remains unclear to what extent dedifferentiated acini differ from native duct cells and which genes are uniquely regulating acinar cell dedifferentiation. Moreover, most studies have been performed on mice since the availability of human cells is scarce. Here, we applied a non-genetic lineage tracing method of human pancreatic exocrine acinar and duct cells that allowed cell-type-specific gene expression profiling by RNA sequencing. Subsequent to this discovery analysis, one transcription factor that was unique for dedifferentiated acinar cells was functionally characterized. RNA sequencing analysis showed that human dedifferentiated acinar cells expressed genes in “Pathways of cancer” with a prominence of MECOM (EVI-1), a transcription factor that was not expressed by duct cells. During mouse embryonic development, pre-acinar cells also transiently expressed MECOM and in the adult mouse pancreas, MECOM was re-expressed when mice were subjected to acute and chronic pancreatitis, conditions in which acinar cells dedifferentiate. In human cells and in mice, MECOM expression correlated with and was directly regulated by SOX9. Mouse acinar cells that, by genetic manipulation, lose the ability to upregulate MECOM showed impaired cell adhesion, more prominent acinar cell death, and suppressed acinar cell dedifferentiation by limited ERK signaling. In conclusion, we transcriptionally profiled the two major human pancreatic exocrine cell types, acinar and duct cells, during experimental stress conditions. We provide insights that in dedifferentiated acinar cells, cancer pathways are upregulated in which MECOM is a critical regulator that suppresses acinar cell death by permitting cellular dedifferentiation.
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spelling pubmed-84082192021-09-16 MECOM permits pancreatic acinar cell dedifferentiation avoiding cell death under stress conditions Backx, Elyne Wauters, Elke Baldan, Jonathan Van Bulck, Mathias Michiels, Ellis Heremans, Yves De Paep, Diedert Luc Kurokawa, Mineo Goyama, Susumu Bouwens, Luc Jacquemin, Patrick Houbracken, Isabelle Rooman, Ilse Cell Death Differ Article Maintenance of the pancreatic acinar cell phenotype suppresses tumor formation. Hence, repetitive acute or chronic pancreatitis, stress conditions in which the acinar cells dedifferentiate, predispose for cancer formation in the pancreas. Dedifferentiated acinar cells acquire a large panel of duct cell-specific markers. However, it remains unclear to what extent dedifferentiated acini differ from native duct cells and which genes are uniquely regulating acinar cell dedifferentiation. Moreover, most studies have been performed on mice since the availability of human cells is scarce. Here, we applied a non-genetic lineage tracing method of human pancreatic exocrine acinar and duct cells that allowed cell-type-specific gene expression profiling by RNA sequencing. Subsequent to this discovery analysis, one transcription factor that was unique for dedifferentiated acinar cells was functionally characterized. RNA sequencing analysis showed that human dedifferentiated acinar cells expressed genes in “Pathways of cancer” with a prominence of MECOM (EVI-1), a transcription factor that was not expressed by duct cells. During mouse embryonic development, pre-acinar cells also transiently expressed MECOM and in the adult mouse pancreas, MECOM was re-expressed when mice were subjected to acute and chronic pancreatitis, conditions in which acinar cells dedifferentiate. In human cells and in mice, MECOM expression correlated with and was directly regulated by SOX9. Mouse acinar cells that, by genetic manipulation, lose the ability to upregulate MECOM showed impaired cell adhesion, more prominent acinar cell death, and suppressed acinar cell dedifferentiation by limited ERK signaling. In conclusion, we transcriptionally profiled the two major human pancreatic exocrine cell types, acinar and duct cells, during experimental stress conditions. We provide insights that in dedifferentiated acinar cells, cancer pathways are upregulated in which MECOM is a critical regulator that suppresses acinar cell death by permitting cellular dedifferentiation. Nature Publishing Group UK 2021-03-24 2021-09 /pmc/articles/PMC8408219/ /pubmed/33762742 http://dx.doi.org/10.1038/s41418-021-00771-6 Text en © The Author(s) 2021 https://creativecommons.org/licenses/by/4.0/Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Article
Backx, Elyne
Wauters, Elke
Baldan, Jonathan
Van Bulck, Mathias
Michiels, Ellis
Heremans, Yves
De Paep, Diedert Luc
Kurokawa, Mineo
Goyama, Susumu
Bouwens, Luc
Jacquemin, Patrick
Houbracken, Isabelle
Rooman, Ilse
MECOM permits pancreatic acinar cell dedifferentiation avoiding cell death under stress conditions
title MECOM permits pancreatic acinar cell dedifferentiation avoiding cell death under stress conditions
title_full MECOM permits pancreatic acinar cell dedifferentiation avoiding cell death under stress conditions
title_fullStr MECOM permits pancreatic acinar cell dedifferentiation avoiding cell death under stress conditions
title_full_unstemmed MECOM permits pancreatic acinar cell dedifferentiation avoiding cell death under stress conditions
title_short MECOM permits pancreatic acinar cell dedifferentiation avoiding cell death under stress conditions
title_sort mecom permits pancreatic acinar cell dedifferentiation avoiding cell death under stress conditions
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8408219/
https://www.ncbi.nlm.nih.gov/pubmed/33762742
http://dx.doi.org/10.1038/s41418-021-00771-6
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