Tpbpa mediated deletion of Tfap2c leads to deregulation of MAPK, P21, AKT and subsequent placental growth arrest

Sharma, Neha; Kubaczka, Caroline; Kaiser, Stéphanie; Nettersheim, Daniel; Mughal, Sadaf S.; Riesenberg, Stefanie; Hölzel, Michael; Winterhager, Elke; Schorle, Hubert

doi:10.1242/dev.128553

Cited by 33 publications

(33 citation statements)

References 66 publications

(84 reference statements)

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“…We identified a substantial fraction of transcriptional repressors (IKZF5, IFI16, BHLME40 and CBFA2T2), genes associated with DNA mismatch repair (PMS1, MBD4) and several components of NFκβ (BCL3, RELA) and WNT (CDX1, HBP1, HMGN3) signalling pathways. Interestingly, the network also contained TFAP2C and GCM1, which in mouse are associated with trophoblast lineage specification (Kaiser et al, 2015;Sharma et al, 2016) and regulation of syncytium formation (Kashif et al, 2011;Lu et al, 2016), respectively. For quantitative visualisation of species specificity we plotted relative expression of transcription factors and epigenetic modifiers ( Fig.…”

Section: Conserved and Primate-specific Elements Of The Epi And Pre Tmentioning

confidence: 99%

Single-cell transcriptome analysis of human, marmoset and mouse embryos reveals common and divergent features of preimplantation development

Boroviak

Stirparo

Dietmann

et al. 2018

Preprint

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The mouse embryo is the canonical model for mammalian preimplantation development. Recent advances in single-cell profiling allow detailed analysis of embryogenesis in other eutherian species, including human, to distinguish conserved from divergent regulatory programs and signalling pathways in the rodent paradigm. Here, we identify and compare transcriptional features of human, marmoset and mouse embryos by single-cell RNA-seq. Zygotic genome activation correlates with the presence of Polycomb Repressive Complexes in all three species, while ribosome biogenesis emerges as a predominant attribute in primate embryos, supporting prolonged translation of maternally deposited RNAs. We find that transposable element expression signatures are species-, stage-and lineage-specific. The pluripotency network in the primate epiblast lacks certain regulators operative in mouse, but encompasses WNT components and genes associated with trophoblast specification. Sequential activation of GATA6, SOX17 and GATA4 markers of primitive endoderm identity is conserved in primates. Unexpectedly, OTX2 is also associated with primitive endoderm specification in human and nonhuman primate blastocysts. Our cross-species analysis demarcates both conserved and primate-specific features of preimplantation development and underscores the molecular adaptability of early mammalian embryogenesis.

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Section: Conserved and Primate-specific Elements Of The Epi And Pre Tmentioning

confidence: 99%

Single-cell transcriptome analysis of human, marmoset and mouse embryos reveals common and divergent features of preimplantation development

Boroviak

Stirparo

Dietmann

et al. 2018

Preprint

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show abstract

“…Recently, we developed a genetic mouse model of placental insufficiency via growth arrest of the junctional zone of the placenta (45). This was accomplished by conditional ablation of transcription factor Tfap2c (transcription factor AP-2y) in Tpbpa-positive (trophoblast specific protein a) cell lineage at gestational day 14.5.…”

Section: Introductionmentioning

confidence: 99%

Placental insufficiency contributes to fatty acid metabolism alterations in aged female mouse offspring

Stojanovska

Sharma

Dijkstra

et al. 2018

American Journal of Physiology-Regulatory, Integrative and Comp

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Intrauterine growth restriction (IUGR) is an accepted risk factor for metabolic disorders in later life, including obesity and type 2 diabetes. The level of metabolic dysregulation can vary between subjects and is dependent on the severity and the type of IUGR insult. Classical IUGR animal models involve nutritional deprivation of the mother or uterine artery ligation. The latter aims to mimic a placental insufficiency, which is the most frequent cause of IUGR. In this study, we investigated whether IUGR due to placental insufficiency impacts the glucose and lipid homeostasis at advanced age. Placental insufficiency was achieved by deletion of the transcription factor AP-2y (Tfap2c), which serves as one of the major trophoblast differentiation regulators. TdelT-IUGR mice were obtained by crossing mice with a floxed Tfap2c allele and mice with Cre recombinase under the control of the Tpbpa promoter. In advanced adulthood (9-12 months) female and male IUGR mice are respectively 20% and 12% leaner compared to controls. At this age, IUGR mice have unaffected glucose clearance and lipid parameters (cholesterol, triglycerides and phospholipids) in the liver. However, female IUGR mice have increased plasma free fatty acids (FFAs) (+87%) compared to controls. This is accompanied by increased mRNA levels of fatty acid synthase and endoplasmic reticulum stress markers in white adipose tissue. Taken together, our results suggest that IUGR by placental insufficiency may lead to higher lipogenesis in female mice in advanced adulthood, at least indicated by greater Fasn expression. This effect was sex-specific for the aged IUGR females.

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“…2E). For example, as shown in Figs 2F and 3A, d2 DARs are located proximal to a previously described regulator of trophoblast cell migration Ovol2 26 , Tfap2c known to govern trophoblast differentiation and proliferation 27–29 , and Prdm1 required for SpA-TGC specification 19 . These observations strongly suggest that increased accessibility promotes activation of proximal gene expression.…”

Section: Resultsmentioning

confidence: 79%

“…As for transfected P19 embryonal carcinoma cells 33 , here we observe occupancy by Blimp1 and Tfap2c at common target sites in trophoblasts, though it is not clear whether they bind independently or cooperatively in this case. Tfap2c functions as a transcriptional repressor governing trophoblast differentiation within the SpT layer 29 , but a cooperative Blimp1 and Tfap2c functional relationship has not previously been reported during placenta development. Interestingly, coexpression was recently confirmed in trophoblasts at the single-cell level 20 .…”

Section: Discussionmentioning

confidence: 91%

Mapping the chromatin landscape and Blimp1 transcriptional targets that regulate trophoblast differentiation

Nelson

Mould

Bikoff

et al. 2017

Sci Rep

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Trophoblast stem cells (TSCs) give rise to specialized cell types within the placenta. However, the regulatory mechanisms that guide trophoblast cell fate decisions during placenta development remain ill defined. Here we exploited ATAC-seq and transcriptional profiling strategies to describe dynamic changes in gene expression and chromatin accessibility during TSC differentiation. We detect significantly increased chromatin accessibility at key genes upregulated as TSCs exit from the stem cell state. However, downregulated gene expression is not simply due to the loss of chromatin accessibility in proximal regions. Additionally, transcriptional targets recognized by the zinc finger transcriptional repressor Prdm1/Blimp1, an essential regulator of placenta development, were identified in ChIP-seq experiments. Comparisons with previously reported ChIP-seq datasets for primordial germ cell-like cells and E18.5 small intestine, combined with functional annotation analysis revealed that Blimp1 has broadly shared as well as cell type-specific functional activities unique to the trophoblast lineage. Importantly, Blimp1 not only silences TSC gene expression but also prevents aberrant activation of divergent developmental programmes. Overall the present study provides new insights into the chromatin landscape and Blimp1-dependent regulatory networks governing trophoblast gene expression.

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Tpbpa mediated deletion of Tfap2c leads to deregulation of MAPK, P21, AKT and subsequent placental growth arrest

Cited by 33 publications

References 66 publications

Single-cell transcriptome analysis of human, marmoset and mouse embryos reveals common and divergent features of preimplantation development

Single-cell transcriptome analysis of human, marmoset and mouse embryos reveals common and divergent features of preimplantation development

Placental insufficiency contributes to fatty acid metabolism alterations in aged female mouse offspring

Mapping the chromatin landscape and Blimp1 transcriptional targets that regulate trophoblast differentiation

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