Derivation of pluripotent epiblast stem cells from mammalian embryos

Brons, I. G. M.; Smithers, Lucy; Trotter, Matthew; Rugg‐Gunn, Peter J.; Sun, Bowen; Lopes, Susana M. Chuva de Sousa; Howlett, Sarah; Clarkson, Amanda; Ährlund‐Richter, Lars; Pedersen, Roger A.; Vallier, Ludovic

doi:10.1038/nature05950

Cited by 1,839 publications

(1,988 citation statements)

References 26 publications

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“…S1B). Lines E3, T9, and C1a1 have previously been characterized using this assay [2][3][4]. Taken together, these data demonstrate that these six cell lines were pluripotent EpiSC lines.…”

Section: Characterization Of Episc Linessupporting

confidence: 59%

“…For example, mESCs undergo self-renewal in the presence of leukemia inhibitory factor (LIF) and inhibitors of fibroblast growth factor (FGF) signaling [1]. In contrast, EpiSCs require FGF and Activin signaling to sustain self-renewal [2][3][4]. Intriguingly, human embryonic stem cells (hESCs), although derived from preimplantation embryos, appear to share more characteristics with EpiSCs than with mESCs.…”

Section: Introductionmentioning

confidence: 99%

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Distinct Developmental Ground States of Epiblast Stem Cell Lines Determine Different Pluripotency Features

et al. 2011

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Epiblast stem cells (EpiSCs) are pluripotent stem cells derived from mouse postimplantation embryos at embryonic day (E) 5.5-E7.5 at the onset of gastrulation, which makes them a valuable tool for studying mammalian postimplantation development in vitro. EpiSCs can also be reprogrammed into a mouse embryonic stem cell (mESC)-like state. Some reports have shown that the reversion of EpiSCs requires transcription factor overexpression, whereas others have suggested that use of stringent mESC culture conditions alone is sufficient for the reversion of EpiSCs. To clarify these discrepancies, we systematically compared a panel of independent EpiSC lines. We found that-regardless of the embryonic day of derivation-the different EpiSC lines shared a number of defining characteristics such as the ability to form teratomas. However, despite use of standard EpiSC culture conditions, some lines exhibited elevated expression of genes associated with mesendodermal differentiation. Pluripotency (Oct4) and mesodermal (Brachyury) marker genes were coexpressed in this subset of lines. Interestingly, the expression of mesendodermal marker genes was negatively correlated with the cells' ability to efficiently undergo neural induction. Moreover, these mesodermal marker gene-expressing cell lines could not be efficiently reverted to an mESC-like state by using stringent mESC culture conditions. Conversely, Brachyury overexpression diminished the reversion efficiency in otherwise Brachyury-negative lines. Overall, our data suggest that different EpiSC lines may undergo self-renewal into distinct developmental states, a finding with important implications for functional readouts such as reversion of EpiSCs to an mESC-like state as well as directed differentiation. STEM CELLS

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“…S1B). Lines E3, T9, and C1a1 have previously been characterized using this assay [2][3][4]. Taken together, these data demonstrate that these six cell lines were pluripotent EpiSC lines.…”

Section: Characterization Of Episc Linessupporting

confidence: 59%

Section: Introductionmentioning

confidence: 99%

Distinct Developmental Ground States of Epiblast Stem Cell Lines Determine Different Pluripotency Features

et al. 2011

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“…Indeed, ESCs cultured in LIF/FCS have been proposed to contain a mixture of pluripotent cells that have progressed to different extents toward a primed state (Hackett & Surani, 2014). Such a primed state can also be captured in vitro as EpiSC, by explantation and culture of post‐implantation epiblast cells (Brons et al , 2007; Tesar et al , 2007). In contrast, ESCs cultured in LIF supplemented with inhibitors of both MEK and GSK3b (two inhibitors or 2i; Ying et al , 2008) may represent the opposite end of the range of pluripotent states that can be maintained in vitro (Hackett & Surani, 2014).…”

Section: Introductionmentioning

confidence: 99%

Esrrb extinction triggers dismantling of naïve pluripotency and marks commitment to differentiation

et al. 2018

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Self‐renewal of embryonic stem cells (ESCs) cultured in LIF/fetal calf serum (FCS) is incomplete with some cells initiating differentiation. While this is reflected in heterogeneous expression of naive pluripotency transcription factors (TFs), the link between TF heterogeneity and differentiation is not fully understood. Here, we purify ESCs with distinct TF expression levels from LIF/FCS cultures to uncover early events during commitment from naïve pluripotency. ESCs carrying fluorescent Nanog and Esrrb reporters show Esrrb downregulation only in Nanoglow cells. Independent Esrrb reporter lines demonstrate that Esrrbnegative ESCs cannot effectively self‐renew. Upon Esrrb loss, pre‐implantation pluripotency gene expression collapses. ChIP‐Seq identifies different regulatory element classes that bind both OCT4 and NANOG in Esrrbpositive cells. Class I elements lose NANOG and OCT4 binding in Esrrbnegative ESCs and associate with genes expressed preferentially in naïve ESCs. In contrast, Class II elements retain OCT4 but not NANOG binding in ESRRB‐negative cells and associate with more broadly expressed genes. Therefore, mechanistic differences in TF function act cumulatively to restrict potency during exit from naïve pluripotency.

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“…Epiblast stem cells present the next stage in development and therefore have a more limited developmental potential. They show poor success in generating chimeras and can manifest expression of early lineage commitment markers [20,21]. Thus, the similarity of mouse EpiESC to human ESC/iPSC, together with the limited pluripotency tests available in human lines, raise questions on whether those cells are capable of producing whole embryos and about their general level of pluripotency.…”

Section: Introductionmentioning

confidence: 99%

Concise Review: Induced Pluripotent Stem Cells Versus Embryonic Stem Cells: Close Enough or Yet Too Far Apart?

2011

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Derivation of pluripotent epiblast stem cells from mammalian embryos

Cited by 1,839 publications

References 26 publications

Distinct Developmental Ground States of Epiblast Stem Cell Lines Determine Different Pluripotency Features

Distinct Developmental Ground States of Epiblast Stem Cell Lines Determine Different Pluripotency Features

Esrrb extinction triggers dismantling of naïve pluripotency and marks commitment to differentiation

Concise Review: Induced Pluripotent Stem Cells Versus Embryonic Stem Cells: Close Enough or Yet Too Far Apart?

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