Cell lineage specific distribution of H3K27 trimethylation accumulation in an in vitro model for human implantation.

Cell lineage specific distribution of H3K27 trimethylation accumulation in an in vitro model for human implantation.

Female mammals inactivate one of their two X-chromosomes to compensate for the difference in gene-dosage with males that have just one X-chromosome. X-chromosome inactivation is initiated by the expression of the non-coding RNA Xist, which coats the X-chromosome in cis and triggers gene silencing. I...

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Main Authors: Gijs Teklenburg, Charlotte H E Weimar, Bart C J M Fauser, Nick Macklon, Niels Geijsen, Cobi J Heijnen, Susana M Chuva de Sousa Lopes, Ewart W Kuijk
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3296731?pdf=render
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spelling doaj-0ad0cfa30b7a42f4a6e3dfb568287ca12020-11-25T02:15:44ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-0173e3270110.1371/journal.pone.0032701Cell lineage specific distribution of H3K27 trimethylation accumulation in an in vitro model for human implantation.Gijs TeklenburgCharlotte H E WeimarBart C J M FauserNick MacklonNiels GeijsenCobi J HeijnenSusana M Chuva de Sousa LopesEwart W KuijkFemale mammals inactivate one of their two X-chromosomes to compensate for the difference in gene-dosage with males that have just one X-chromosome. X-chromosome inactivation is initiated by the expression of the non-coding RNA Xist, which coats the X-chromosome in cis and triggers gene silencing. In early mouse development the paternal X-chromosome is initially inactivated in all cells of cleavage stage embryos (imprinted X-inactivation) followed by reactivation of the inactivated paternal X-chromosome exclusively in the epiblast precursors of blastocysts, resulting temporarily in the presence of two active X-chromosomes in this specific lineage. Shortly thereafter, epiblast cells randomly inactivate either the maternal or the paternal X-chromosome. XCI is accompanied by the accumulation of histone 3 lysine 27 trimethylation (H3K27me3) marks on the condensed X-chromosome. It is still poorly understood how XCI is regulated during early human development. Here we have investigated lineage development and the distribution of H3K27me3 foci in human embryos derived from an in-vitro model for human implantation. In this system, embryos are co-cultured on decidualized endometrial stromal cells up to day 8, which allows the culture period to be extended for an additional two days. We demonstrate that after the co-culture period, the inner cell masses have relatively high cell numbers and that the GATA4-positive hypoblast lineage and OCT4-positive epiblast cell lineage in these embryos have segregated. H3K27me3 foci were observed in ∼25% of the trophectoderm cells and in ∼7.5% of the hypoblast cells, but not in epiblast cells. In contrast with day 8 embryos derived from the co-cultures, foci of H3K27me3 were not observed in embryos at day 5 of development derived from regular IVF-cultures. These findings indicate that the dynamics of H3K27me3 accumulation on the X-chromosome in human development is regulated in a lineage specific fashion.http://europepmc.org/articles/PMC3296731?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Gijs Teklenburg
Charlotte H E Weimar
Bart C J M Fauser
Nick Macklon
Niels Geijsen
Cobi J Heijnen
Susana M Chuva de Sousa Lopes
Ewart W Kuijk
spellingShingle Gijs Teklenburg
Charlotte H E Weimar
Bart C J M Fauser
Nick Macklon
Niels Geijsen
Cobi J Heijnen
Susana M Chuva de Sousa Lopes
Ewart W Kuijk
Cell lineage specific distribution of H3K27 trimethylation accumulation in an in vitro model for human implantation.
PLoS ONE
author_facet Gijs Teklenburg
Charlotte H E Weimar
Bart C J M Fauser
Nick Macklon
Niels Geijsen
Cobi J Heijnen
Susana M Chuva de Sousa Lopes
Ewart W Kuijk
author_sort Gijs Teklenburg
title Cell lineage specific distribution of H3K27 trimethylation accumulation in an in vitro model for human implantation.
title_short Cell lineage specific distribution of H3K27 trimethylation accumulation in an in vitro model for human implantation.
title_full Cell lineage specific distribution of H3K27 trimethylation accumulation in an in vitro model for human implantation.
title_fullStr Cell lineage specific distribution of H3K27 trimethylation accumulation in an in vitro model for human implantation.
title_full_unstemmed Cell lineage specific distribution of H3K27 trimethylation accumulation in an in vitro model for human implantation.
title_sort cell lineage specific distribution of h3k27 trimethylation accumulation in an in vitro model for human implantation.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description Female mammals inactivate one of their two X-chromosomes to compensate for the difference in gene-dosage with males that have just one X-chromosome. X-chromosome inactivation is initiated by the expression of the non-coding RNA Xist, which coats the X-chromosome in cis and triggers gene silencing. In early mouse development the paternal X-chromosome is initially inactivated in all cells of cleavage stage embryos (imprinted X-inactivation) followed by reactivation of the inactivated paternal X-chromosome exclusively in the epiblast precursors of blastocysts, resulting temporarily in the presence of two active X-chromosomes in this specific lineage. Shortly thereafter, epiblast cells randomly inactivate either the maternal or the paternal X-chromosome. XCI is accompanied by the accumulation of histone 3 lysine 27 trimethylation (H3K27me3) marks on the condensed X-chromosome. It is still poorly understood how XCI is regulated during early human development. Here we have investigated lineage development and the distribution of H3K27me3 foci in human embryos derived from an in-vitro model for human implantation. In this system, embryos are co-cultured on decidualized endometrial stromal cells up to day 8, which allows the culture period to be extended for an additional two days. We demonstrate that after the co-culture period, the inner cell masses have relatively high cell numbers and that the GATA4-positive hypoblast lineage and OCT4-positive epiblast cell lineage in these embryos have segregated. H3K27me3 foci were observed in ∼25% of the trophectoderm cells and in ∼7.5% of the hypoblast cells, but not in epiblast cells. In contrast with day 8 embryos derived from the co-cultures, foci of H3K27me3 were not observed in embryos at day 5 of development derived from regular IVF-cultures. These findings indicate that the dynamics of H3K27me3 accumulation on the X-chromosome in human development is regulated in a lineage specific fashion.
url http://europepmc.org/articles/PMC3296731?pdf=render
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