The Homeodomain-Containing Transcription Factors Arx and Pax4 Control Enteroendocrine Subtype Specification in Mice

Intestinal hormones are key regulators of digestion and energy homeostasis secreted by rare enteroendocrine cells. These cells produce over ten different hormones including GLP-1 and GIP peptides known to promote insulin secretion. To date, the molecular mechanisms controlling the specification of t...

Descripción completa

Detalles Bibliográficos
Autores principales: Beucher, Anthony, Gjernes, Elisabet, Collin, Caitlin, Courtney, Monica, Meunier, Aline, Collombat, Patrick, Gradwohl, Gérard
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3343025/
https://www.ncbi.nlm.nih.gov/pubmed/22570716
http://dx.doi.org/10.1371/journal.pone.0036449
_version_ 1782231764354203648
author Beucher, Anthony
Gjernes, Elisabet
Collin, Caitlin
Courtney, Monica
Meunier, Aline
Collombat, Patrick
Gradwohl, Gérard
author_facet Beucher, Anthony
Gjernes, Elisabet
Collin, Caitlin
Courtney, Monica
Meunier, Aline
Collombat, Patrick
Gradwohl, Gérard
author_sort Beucher, Anthony
collection PubMed
description Intestinal hormones are key regulators of digestion and energy homeostasis secreted by rare enteroendocrine cells. These cells produce over ten different hormones including GLP-1 and GIP peptides known to promote insulin secretion. To date, the molecular mechanisms controlling the specification of the various enteroendocrine subtypes from multipotent Neurog3(+) endocrine progenitor cells, as well as their number, remain largely unknown. In contrast, in the embryonic pancreas, the opposite activities of Arx and Pax4 homeodomain transcription factors promote islet progenitor cells towards the different endocrine cell fates. In this study, we thus investigated the role of Arx and Pax4 in enteroendocrine subtype specification. The small intestine and colon of Arx- and Pax4-deficient mice were analyzed using histological, molecular, and lineage tracing approaches. We show that Arx is expressed in endocrine progenitors (Neurog3(+)) and in early differentiating (ChromograninA(−)) GLP-1-, GIP-, CCK-, Sct- Gastrin- and Ghrelin-producing cells. We noted a dramatic reduction or a complete loss of all these enteroendocrine cell types in Arx mutants. Serotonin- and Somatostatin-secreting cells do not express Arx and, accordingly, the differentiation of Serotonin cells was not affected in Arx mutants. However, the number of Somatostatin-expressing D-cells is increased as Arx-deficient progenitor cells are redirected to the D-cell lineage. In Pax4-deficient mice, the differentiation of Serotonin and Somatostatin cells is impaired, as well as of GIP and Gastrin cells. In contrast, the number of GLP-1 producing L-cells is increased concomitantly with an upregulation of Arx. Thus, while Arx and Pax4 are necessary for the development of L- and D-cells respectively, they conversely restrict D- and L-cells fates suggesting antagonistic functions in D/L cell allocation. In conclusion, these finding demonstrate that, downstream of Neurog3, the specification of a subset of enteroendocrine subtypes relies on both Arx and Pax4, while others depend only on Arx or Pax4.
format Online
Article
Text
id pubmed-3343025
institution National Center for Biotechnology Information
language English
publishDate 2012
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-33430252012-05-08 The Homeodomain-Containing Transcription Factors Arx and Pax4 Control Enteroendocrine Subtype Specification in Mice Beucher, Anthony Gjernes, Elisabet Collin, Caitlin Courtney, Monica Meunier, Aline Collombat, Patrick Gradwohl, Gérard PLoS One Research Article Intestinal hormones are key regulators of digestion and energy homeostasis secreted by rare enteroendocrine cells. These cells produce over ten different hormones including GLP-1 and GIP peptides known to promote insulin secretion. To date, the molecular mechanisms controlling the specification of the various enteroendocrine subtypes from multipotent Neurog3(+) endocrine progenitor cells, as well as their number, remain largely unknown. In contrast, in the embryonic pancreas, the opposite activities of Arx and Pax4 homeodomain transcription factors promote islet progenitor cells towards the different endocrine cell fates. In this study, we thus investigated the role of Arx and Pax4 in enteroendocrine subtype specification. The small intestine and colon of Arx- and Pax4-deficient mice were analyzed using histological, molecular, and lineage tracing approaches. We show that Arx is expressed in endocrine progenitors (Neurog3(+)) and in early differentiating (ChromograninA(−)) GLP-1-, GIP-, CCK-, Sct- Gastrin- and Ghrelin-producing cells. We noted a dramatic reduction or a complete loss of all these enteroendocrine cell types in Arx mutants. Serotonin- and Somatostatin-secreting cells do not express Arx and, accordingly, the differentiation of Serotonin cells was not affected in Arx mutants. However, the number of Somatostatin-expressing D-cells is increased as Arx-deficient progenitor cells are redirected to the D-cell lineage. In Pax4-deficient mice, the differentiation of Serotonin and Somatostatin cells is impaired, as well as of GIP and Gastrin cells. In contrast, the number of GLP-1 producing L-cells is increased concomitantly with an upregulation of Arx. Thus, while Arx and Pax4 are necessary for the development of L- and D-cells respectively, they conversely restrict D- and L-cells fates suggesting antagonistic functions in D/L cell allocation. In conclusion, these finding demonstrate that, downstream of Neurog3, the specification of a subset of enteroendocrine subtypes relies on both Arx and Pax4, while others depend only on Arx or Pax4. Public Library of Science 2012-05-03 /pmc/articles/PMC3343025/ /pubmed/22570716 http://dx.doi.org/10.1371/journal.pone.0036449 Text en Beucher et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Beucher, Anthony
Gjernes, Elisabet
Collin, Caitlin
Courtney, Monica
Meunier, Aline
Collombat, Patrick
Gradwohl, Gérard
The Homeodomain-Containing Transcription Factors Arx and Pax4 Control Enteroendocrine Subtype Specification in Mice
title The Homeodomain-Containing Transcription Factors Arx and Pax4 Control Enteroendocrine Subtype Specification in Mice
title_full The Homeodomain-Containing Transcription Factors Arx and Pax4 Control Enteroendocrine Subtype Specification in Mice
title_fullStr The Homeodomain-Containing Transcription Factors Arx and Pax4 Control Enteroendocrine Subtype Specification in Mice
title_full_unstemmed The Homeodomain-Containing Transcription Factors Arx and Pax4 Control Enteroendocrine Subtype Specification in Mice
title_short The Homeodomain-Containing Transcription Factors Arx and Pax4 Control Enteroendocrine Subtype Specification in Mice
title_sort homeodomain-containing transcription factors arx and pax4 control enteroendocrine subtype specification in mice
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3343025/
https://www.ncbi.nlm.nih.gov/pubmed/22570716
http://dx.doi.org/10.1371/journal.pone.0036449
work_keys_str_mv AT beucheranthony thehomeodomaincontainingtranscriptionfactorsarxandpax4controlenteroendocrinesubtypespecificationinmice
AT gjerneselisabet thehomeodomaincontainingtranscriptionfactorsarxandpax4controlenteroendocrinesubtypespecificationinmice
AT collincaitlin thehomeodomaincontainingtranscriptionfactorsarxandpax4controlenteroendocrinesubtypespecificationinmice
AT courtneymonica thehomeodomaincontainingtranscriptionfactorsarxandpax4controlenteroendocrinesubtypespecificationinmice
AT meunieraline thehomeodomaincontainingtranscriptionfactorsarxandpax4controlenteroendocrinesubtypespecificationinmice
AT collombatpatrick thehomeodomaincontainingtranscriptionfactorsarxandpax4controlenteroendocrinesubtypespecificationinmice
AT gradwohlgerard thehomeodomaincontainingtranscriptionfactorsarxandpax4controlenteroendocrinesubtypespecificationinmice
AT beucheranthony homeodomaincontainingtranscriptionfactorsarxandpax4controlenteroendocrinesubtypespecificationinmice
AT gjerneselisabet homeodomaincontainingtranscriptionfactorsarxandpax4controlenteroendocrinesubtypespecificationinmice
AT collincaitlin homeodomaincontainingtranscriptionfactorsarxandpax4controlenteroendocrinesubtypespecificationinmice
AT courtneymonica homeodomaincontainingtranscriptionfactorsarxandpax4controlenteroendocrinesubtypespecificationinmice
AT meunieraline homeodomaincontainingtranscriptionfactorsarxandpax4controlenteroendocrinesubtypespecificationinmice
AT collombatpatrick homeodomaincontainingtranscriptionfactorsarxandpax4controlenteroendocrinesubtypespecificationinmice
AT gradwohlgerard homeodomaincontainingtranscriptionfactorsarxandpax4controlenteroendocrinesubtypespecificationinmice

Ejemplares similares