Genetic dissection of Nodal and Bmp signalling requirements during primordial germ cell development

AbstractThe essential roles played by Nodal and Bmp signalling during early mouse development have been extensively documented. Here we used conditional deletion strategies to investigate functional contributions made by Nodal, Bmp and Smad downstream effectors during primordial germ cell (PGC) development. We demonstrate that Nodal and its target gene Eomes provide early instructions during formation of the PGC lineage. We discovered that Smad2 inactivation in the visceral endoderm results in increased numbers of PGCs due to an expansion of the PGC niche. Smad1 is required for specification, whereas in contrast Smad4 controls the maintenance and migration of PGCs. Importantly we found that beside Blimp1, down-regulated phosphoSmad159 levels also distinguishes PGCs from their somatic neighbours so that emerging PGCs become refractory to Bmp signalling that otherwise promotes mesodermal development in the posterior epiblast. Thus balanced Nodal/Bmp signalling cues regulate germ cell versus somatic cell fate decisions in the early posterior epiblast.

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Single-cell transcriptional analysis to uncover regulatory circuits driving cell fate decisions in early mouse development

Bioinformatics ◽

10.1093/bioinformatics/btu777 ◽

2014 ◽

Vol 31 (7) ◽

pp. 1060-1066 ◽

Cited By ~ 31

Author(s):

Haifen Chen ◽

Jing Guo ◽

Shital K. Mishra ◽

Paul Robson ◽

Mahesan Niranjan ◽

...

Keyword(s):

Single Cell ◽

Cell Fate ◽

Transcriptional Analysis ◽

Mouse Development ◽

Cell Fate Decisions ◽

Regulatory Circuits ◽

Early Mouse

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Expression pattern of Motch, a mouse homolog of Drosophila Notch, suggests an important role in early postimplantation mouse development

Development ◽

10.1242/dev.115.3.737 ◽

1992 ◽

Vol 115 (3) ◽

pp. 737-744 ◽

Cited By ~ 22

Author(s):

F.F. Del Amo ◽

D.E. Smith ◽

P.J. Swiatek ◽

M. Gendron-Maguire ◽

R.J. Greenspan ◽

...

Keyword(s):

Cell Fate ◽

Mouse Embryo ◽

Transmembrane Protein ◽

Neuronal Cell ◽

Cell Types ◽

Drosophila Embryo ◽

Mouse Development ◽

Cell Fate Decisions ◽

Early Mouse ◽

Partial Cdna Clone

The Notch gene of Drosophila encodes a large transmembrane protein involved in cell-cell interactions and cell fate decisions in the Drosophila embryo. To determine if a gene homologous to Drosophila Notch plays a role in early mouse development, we screened a mouse embryo cDNA library with probes from the Xenopus Notch homolog, Xotch. A partial cDNA clone encoding the mouse Notch homolog, which we have termed Motch, was used to analyze expression of the Motch gene. Motch transcripts were detected in a wide variety of adult tissues, which included derivatives of all three germ layers. Differentiation of P19 embryonal carcinoma cells into neuronal cell types resulted in increased expression of Motch RNA. In the postimplantation mouse embryo Motch transcripts were first detected in mesoderm at 7.5 days post coitum (dpc). By 8.5 dpc, transcript levels were highest in presomitic mesoderm, mesenchyme and endothelial cells, while much lower levels were detected in neuroepithelium. In contrast, at 9.5 dpc, neuroepithelium was a major site of Motch expression. Transcripts were also abundant in cell types derived from neural crest. These data suggest that the Motch gene plays multiple roles in patterning and differentiation of the early postimplantation mouse embryo.

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Coordination between patterning and morphogenesis ensures robustness during mouse development

Philosophical Transactions of the Royal Society B Biological Sciences ◽

10.1098/rstb.2019.0562 ◽

2020 ◽

Vol 375 (1809) ◽

pp. 20190562 ◽

Cited By ~ 1

Author(s):

Néstor Saiz ◽

Anna-Katerina Hadjantonakis

Keyword(s):

Cell Fate ◽

Cell Types ◽

Biological Noise ◽

Mouse Development ◽

Lineage Specification ◽

Cell Fate Decisions ◽

The Past ◽

Early Mouse ◽

The Right ◽

External Signals

The mammalian preimplantation embryo is a highly tractable, self-organizing developmental system in which three cell types are consistently specified without the need for maternal factors or external signals. Studies in the mouse over the past decades have greatly improved our understanding of the cues that trigger symmetry breaking in the embryo, the transcription factors that control lineage specification and commitment, and the mechanical forces that drive morphogenesis and inform cell fate decisions. These studies have also uncovered how these multiple inputs are integrated to allocate the right number of cells to each lineage despite inherent biological noise, and as a response to perturbations. In this review, we summarize our current understanding of how these processes are coordinated to ensure a robust and precise developmental outcome during early mouse development. This article is part of a discussion meeting issue ‘Contemporary morphogenesis'.

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Chromatin dynamics and the role of G9a in gene regulation and enhancer silencing during early mouse development

eLife ◽

10.7554/elife.09571 ◽

2015 ◽

Vol 4 ◽

Cited By ~ 56

Author(s):

Jan J Zylicz ◽

Sabine Dietmann ◽

Ufuk Günesdogan ◽

Jamie A Hackett ◽

Delphine Cougot ◽

...

Keyword(s):

Cell Fate ◽

Regulatory Networks ◽

Histone H3 ◽

Epigenetic Mechanism ◽

Mouse Development ◽

Germline Development ◽

Chromatin Dynamics ◽

Cell Fate Decisions ◽

Active Enhancer ◽

Early Mouse

Early mouse development is accompanied by dynamic changes in chromatin modifications, including G9a-mediated histone H3 lysine 9 dimethylation (H3K9me2), which is essential for embryonic development. Here we show that genome-wide accumulation of H3K9me2 is crucial for postimplantation development, and coincides with redistribution of enhancer of zeste homolog 2 (EZH2)-dependent histone H3 lysine 27 trimethylation (H3K27me3). Loss of G9a or EZH2 results in upregulation of distinct gene sets involved in cell cycle regulation, germline development and embryogenesis. Notably, the H3K9me2 modification extends to active enhancer elements where it promotes developmentally-linked gene silencing and directly marks promoters and gene bodies. This epigenetic mechanism is important for priming gene regulatory networks for critical cell fate decisions in rapidly proliferating postimplantation epiblast cells.

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Genetic dissection of Nodal and Bmp signalling requirements during primordial germ cell development in mouse

Nature Communications ◽

10.1038/s41467-019-09052-w ◽

2019 ◽

Vol 10 (1) ◽

Cited By ~ 4

Author(s):

Anna D. Senft ◽

Elizabeth K. Bikoff ◽

Elizabeth J. Robertson ◽

Ita Costello

Keyword(s):

Germ Cell ◽

Primordial Germ Cell ◽

Cell Development ◽

Genetic Dissection ◽

Germ Cell Development ◽

Bmp Signalling

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Loss of Kallmann syndrome-associated gene WDR11 disrupts primordial germ cell development by affecting canonical and non-canonical Hedgehog signalling

10.1101/2020.09.06.284927 ◽

2020 ◽

Author(s):

Jiyoung Lee ◽

Yeonjoo Kim ◽

Paris Ataliotis ◽

Hyung-Goo Kim ◽

Dae-Won Kim ◽

...

Keyword(s):

Germ Cell ◽

Germ Cells ◽

Primary Cilia ◽

Primordial Germ Cell ◽

Kallmann Syndrome ◽

Loss Of Function ◽

Downstream Effectors ◽

Cell Components ◽

Underlying Mechanisms ◽

And Migration

ABSTRACTMutations of WDR11 are associated with Kallmann syndrome (KS) and congenital hypogonadotrophic hypogonadism (CHH), typically caused by defective functions of gonadotrophin-releasing hormone (GnRH) neurones in the brain. We previously reported that Wdr11 knockout mice show profound infertility with significantly fewer germ cells present in the gonads. To understand the underlying mechanisms mediated by WDR11 in these processes, we investigated the effects of Wdr11 deletion on primordial germ cell (PGC) development. Using live-tracking of PGCs and primary co-cultures of genital ridges (GR), we demonstrated that Wdr11-deficient embryos contained reduced numbers of PGCs which had delayed migration due to significantly decreased proliferation and motility. We found primary cilia-dependent canonical Hedgehog (Hh) signalling was required for proliferation of the somatic mesenchymal cells of GR, while primary cilia-independent non-canonical Hh signalling mediated by Ptch2/Gas1 and downstream effectors Src and Creb was required for PGC proliferation and migration, which was disrupted by the loss of function mutations of WDR11. Therefore, canonical and non-canonical Hh signalling are differentially involved in the development of somatic and germ cell components of the gonads, and WDR11 is required for both of these pathways operating in parallel in GR and PGCs, respectively, during normal PGC development. Our study provides a mechanistic link between the development of GnRH neurones and germ cells mediated by WDR11, which may underlie some cases of KS/CHH and ciliopathies.

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Genomic insights into chromatin reprogramming to totipotency in embryos

The Journal of Cell Biology ◽

10.1083/jcb.201807044 ◽

2018 ◽

Vol 218 (1) ◽

pp. 70-82 ◽

Cited By ~ 10

Author(s):

Sabrina Ladstätter ◽

Kikuë Tachibana

Keyword(s):

Cell Fate ◽

Regulatory Networks ◽

Chromatin Accessibility ◽

Early Embryo ◽

Epigenetic Reprogramming ◽

Mammalian Embryo ◽

Cell Fate Decisions ◽

A Cell ◽

Early Mouse ◽

Chromatin Reprogramming

The early embryo is the natural prototype for the acquisition of totipotency, which is the potential of a cell to produce a whole organism. Generation of a totipotent embryo involves chromatin reorganization and epigenetic reprogramming that alter DNA and histone modifications. Understanding embryonic chromatin architecture and how this is related to the epigenome and transcriptome will provide invaluable insights into cell fate decisions. Recently emerging low-input genomic assays allow the exploration of regulatory networks in the sparsely available mammalian embryo. Thus, the field of developmental biology is transitioning from microscopy to genome-wide chromatin descriptions. Ultimately, the prototype becomes a unique model for studying fundamental principles of development, epigenetic reprogramming, and cellular plasticity. In this review, we discuss chromatin reprogramming in the early mouse embryo, focusing on DNA methylation, chromatin accessibility, and higher-order chromatin structure.

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Hypersensitivity to DNA damage leads to increased apoptosis during early mouse development

Genes & Development ◽

10.1101/gad.14.16.2072 ◽

2000 ◽

Vol 14 (16) ◽

pp. 2072-2084

Author(s):

Babette S. Heyer ◽

Alasdair MacAuley ◽

Ole Behrendtsen ◽

Zena Werb

Keyword(s):

Dna Damage ◽

Cell Fate ◽

Genotoxic Stress ◽

Embryonic Cells ◽

Mouse Development ◽

Potential Cost ◽

Proliferation And Differentiation ◽

A Cell ◽

Early Mouse ◽

Surveillance Mechanism

Gastrulation in mice is associated with the start of extreme proliferation and differentiation. The potential cost to the embryo of a very rapid proliferation rate is a high production of damaged cells. We demonstrate a novel surveillance mechanism for the elimination of cells damaged by ionizing radiation during mouse gastrulation. During this restricted developmental window, the embryo becomes hypersensitive to DNA damage induced by low dose irradiation (<0.5 Gy) and undergoes apoptosis without cell cycle arrest. Intriguingly, embryonic cells, including germ cell progenitors, but not extraembryonic cells, become hypersensitive to genotoxic stress and undergo Atm- and p53-dependent apoptosis. Thus, hypersensitivity to apoptosis in the early mouse embryo is a cell fate-dependent mechanism to ensure genomic integrity during a period of extreme proliferation and differentiation.

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Nodal signaling regulates endodermal cell motility and actin dynamics via Rac1 and Prex1

The Journal of Cell Biology ◽

10.1083/jcb.201203012 ◽

2012 ◽

Vol 198 (5) ◽

pp. 941-952 ◽

Cited By ~ 30

Author(s):

Stephanie Woo ◽

Michael P. Housley ◽

Orion D. Weiner ◽

Didier Y.R. Stainier

Keyword(s):

Cell Fate ◽

Actin Dynamics ◽

Migration Behavior ◽

Nodal Signaling ◽

Nucleotide Exchange ◽

Random Motility ◽

Cell Behaviors ◽

Cell Fate Decisions ◽

And Migration ◽

Endodermal Cells

Embryo morphogenesis is driven by dynamic cell behaviors, including migration, that are coordinated with fate specification and differentiation, but how such coordination is achieved remains poorly understood. During zebrafish gastrulation, endodermal cells sequentially exhibit first random, nonpersistent migration followed by oriented, persistent migration and finally collective migration. Using a novel transgenic line that labels the endodermal actin cytoskeleton, we found that these stage-dependent changes in migratory behavior correlated with changes in actin dynamics. The dynamic actin and random motility exhibited during early gastrulation were dependent on both Nodal and Rac1 signaling. We further identified the Rac-specific guanine nucleotide exchange factor Prex1 as a Nodal target and showed that it mediated Nodal-dependent random motility. Reducing Rac1 activity in endodermal cells caused them to bypass the random migration phase and aberrantly contribute to mesodermal tissues. Together, our results reveal a novel role for Nodal signaling in regulating actin dynamics and migration behavior, which are crucial for endodermal morphogenesis and cell fate decisions.

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