No evidence of involvement of E-cadherin in cell fate specification or the segregation of Epi and PrE in mouse blastocysts.

During preimplantation mouse development stages, emerging pluripotent epiblast (Epi) and extraembryonic primitive endoderm (PrE) cells are first distributed in the blastocyst in a "salt-and-pepper" manner before they segregate into separate layers. As a result of segregation, PrE cells bec...

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Main Authors: Katarzyna Filimonow, Nestor Saiz, Aneta Suwińska, Tomasz Wyszomirski, Joanna B Grabarek, Elisabetta Ferretti, Anna Piliszek, Berenika Plusa, Marek Maleszewski
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2019-01-01
Series:PLoS ONE
Online Access:https://doi.org/10.1371/journal.pone.0212109
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spelling doaj-95c664d5842c4bcf9538f9612d0063a62021-03-04T12:39:05ZengPublic Library of Science (PLoS)PLoS ONE1932-62032019-01-01142e021210910.1371/journal.pone.0212109No evidence of involvement of E-cadherin in cell fate specification or the segregation of Epi and PrE in mouse blastocysts.Katarzyna FilimonowNestor SaizAneta SuwińskaTomasz WyszomirskiJoanna B GrabarekElisabetta FerrettiAnna PiliszekBerenika PlusaMarek MaleszewskiDuring preimplantation mouse development stages, emerging pluripotent epiblast (Epi) and extraembryonic primitive endoderm (PrE) cells are first distributed in the blastocyst in a "salt-and-pepper" manner before they segregate into separate layers. As a result of segregation, PrE cells become localised on the surface of the inner cell mass (ICM), and the Epi is enclosed by the PrE on one side and by the trophectoderm on the other. During later development, a subpopulation of PrE cells migrates away from the ICM and forms the parietal endoderm (PE), while cells remaining in contact with the Epi form the visceral endoderm (VE). Here, we asked: what are the mechanisms mediating Epi and PrE cell segregation and the subsequent VE vs PE specification? Differences in cell adhesion have been proposed; however, we demonstrate that the levels of plasma membrane-bound E-cadherin (CDH1, cadherin 1) in Epi and PrE cells only differ after the segregation of these lineages within the ICM. Moreover, manipulating E-cadherin levels did not affect lineage specification or segregation, thus failing to confirm its role during these processes. Rather, we report changes in E-cadherin localisation during later PrE-to-PE transition which are accompanied by the presence of Vimentin and Twist, supporting the hypothesis that an epithelial-to-mesenchymal transition process occurs in the mouse peri-implantation blastocyst.https://doi.org/10.1371/journal.pone.0212109
collection DOAJ
language English
format Article
sources DOAJ
author Katarzyna Filimonow
Nestor Saiz
Aneta Suwińska
Tomasz Wyszomirski
Joanna B Grabarek
Elisabetta Ferretti
Anna Piliszek
Berenika Plusa
Marek Maleszewski
spellingShingle Katarzyna Filimonow
Nestor Saiz
Aneta Suwińska
Tomasz Wyszomirski
Joanna B Grabarek
Elisabetta Ferretti
Anna Piliszek
Berenika Plusa
Marek Maleszewski
No evidence of involvement of E-cadherin in cell fate specification or the segregation of Epi and PrE in mouse blastocysts.
PLoS ONE
author_facet Katarzyna Filimonow
Nestor Saiz
Aneta Suwińska
Tomasz Wyszomirski
Joanna B Grabarek
Elisabetta Ferretti
Anna Piliszek
Berenika Plusa
Marek Maleszewski
author_sort Katarzyna Filimonow
title No evidence of involvement of E-cadherin in cell fate specification or the segregation of Epi and PrE in mouse blastocysts.
title_short No evidence of involvement of E-cadherin in cell fate specification or the segregation of Epi and PrE in mouse blastocysts.
title_full No evidence of involvement of E-cadherin in cell fate specification or the segregation of Epi and PrE in mouse blastocysts.
title_fullStr No evidence of involvement of E-cadherin in cell fate specification or the segregation of Epi and PrE in mouse blastocysts.
title_full_unstemmed No evidence of involvement of E-cadherin in cell fate specification or the segregation of Epi and PrE in mouse blastocysts.
title_sort no evidence of involvement of e-cadherin in cell fate specification or the segregation of epi and pre in mouse blastocysts.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2019-01-01
description During preimplantation mouse development stages, emerging pluripotent epiblast (Epi) and extraembryonic primitive endoderm (PrE) cells are first distributed in the blastocyst in a "salt-and-pepper" manner before they segregate into separate layers. As a result of segregation, PrE cells become localised on the surface of the inner cell mass (ICM), and the Epi is enclosed by the PrE on one side and by the trophectoderm on the other. During later development, a subpopulation of PrE cells migrates away from the ICM and forms the parietal endoderm (PE), while cells remaining in contact with the Epi form the visceral endoderm (VE). Here, we asked: what are the mechanisms mediating Epi and PrE cell segregation and the subsequent VE vs PE specification? Differences in cell adhesion have been proposed; however, we demonstrate that the levels of plasma membrane-bound E-cadherin (CDH1, cadherin 1) in Epi and PrE cells only differ after the segregation of these lineages within the ICM. Moreover, manipulating E-cadherin levels did not affect lineage specification or segregation, thus failing to confirm its role during these processes. Rather, we report changes in E-cadherin localisation during later PrE-to-PE transition which are accompanied by the presence of Vimentin and Twist, supporting the hypothesis that an epithelial-to-mesenchymal transition process occurs in the mouse peri-implantation blastocyst.
url https://doi.org/10.1371/journal.pone.0212109
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