Pivotal role of the transcriptional co-activator YAP in trophoblast stemness of the developing human placenta

Meinhardt, Gerold; Haider, Sandra; Kunihs, Victoria; Saleh, Leila; Pollheimer, Jürgen; Fiala, Christian; Hetey, Szabolcs; Fehér, Zsófia; Szilágyi, András; Than, Nándor Gábor; Knöfler, Martin

doi:10.1073/pnas.2002630117

Cited by 99 publications

(113 citation statements)

References 59 publications

(79 reference statements)

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“…The comprehensive analysis of the results suggests that YAP/TAZ and downstream self-renewal-associated genes are involved in the biological process of radial shockwave-mediated promotion of SCB-SPC self-renewal. The results are consistent with previous studies that demonstrated that YAP correlated closely with the self-renewal of ES cells because elevated YAP maintains the potency of ES cells [ 46 , 47 ]. Meanwhile, others reported that YAP/TAZ are dispensable for ES cell fate [ 48 ].…”

Section: Discussionsupporting

confidence: 93%

Radial extracorporeal shockwave promotes subchondral bone stem/progenitor cell self-renewal by activating YAP/TAZ and facilitates cartilage repair in vivo

Zhao

Wang

et al. 2021

Stem Cell Res Ther

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Background Radial extracorporeal shockwave (r-ESW), an innovative and noninvasive technique, is gaining increasing attention in regenerative medicine due to its mechanobiological effects. Subchondral bone stem/progenitor cells (SCB-SPCs), originating from the pivotal zone of the osteochondral unit, have been shown to have multipotency and self-renewal properties. However, thus far, little information is available regarding the influences of r-ESW on the biological properties of SCB-SPCs and their therapeutic effects in tissue regeneration. Methods SCB-SPCs were isolated from human knee plateau osteochondral specimens and treated with gradient doses of r-ESW in a suspension stimulation system. The optimized parameters for SCB-SPC self-renewal were screened out by colony-forming unit fibroblast assay (CFU-F). Then, the effects of r-ESW on the proliferation, apoptosis, and multipotency of SCB-SPCs were evaluated. Moreover, the repair efficiency of radial shockwave-preconditioned SCB-SPCs was evaluated in vivo via an osteochondral defect model. Potential mechanisms were explored by western blotting, confocal laser scanning, and high-throughput sequencing. Results The CFU-F data indicate that r-ESW could augment the self-renewal of SCB-SPCs in a dose-dependent manner. The CCK-8 and flow cytometry results showed that the optimized shockwave markedly promoted SCB-SPC proliferation but had no significant influence on cell apoptosis. Radial shockwave exerted no significant influence on osteogenic capacity but strongly suppressed adipogenic ability in the current study. For chondrogenic potentiality, the treated SCB-SPCs were mildly enhanced, while the change was not significant. Importantly, the macroscopic scores and further histological analysis strongly demonstrated that the in vivo therapeutic effects of SCB-SPCs were markedly improved post r-ESW treatment. Further analysis showed that the cartilage-related markers collagen II and proteoglycan were expressed at higher levels compared to their counterpart group. Mechanistic studies suggested that r-ESW treatment strongly increased the expression of YAP and promoted YAP nuclear translocation in SCB-SPCs. More importantly, self-renewal was partially blocked by the YAP-specific inhibitor verteporfin. Moreover, the high-throughput sequencing data indicated that other self-renewal-associated pathways may also be involved in this process. Conclusion We found that r-ESW is capable of promoting the self-renewal of SCB-SPCs in vitro by targeting YAP activity and strengthening its repair efficiency in vivo, indicating promising application prospects.

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Section: Discussionsupporting

confidence: 93%

Radial extracorporeal shockwave promotes subchondral bone stem/progenitor cell self-renewal by activating YAP/TAZ and facilitates cartilage repair in vivo

Zhao

Wang

et al. 2021

Stem Cell Res Ther

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“…Like in the mouse, YAP is essential for the development of the human TE and placenta, and its expression is negatively correlated with pregnancy disorders like preeclampsia [40,41]. The YAP-TEAD4 transcriptional program was recently shown to maintain human trophoblast stemness in primary cytotrophoblasts and repress cell fusion [40].…”

Section: Yap In the Human Vs The Mouse Embryo And Placentamentioning

confidence: 99%

Context-dependent roles of YAP/TAZ in stem cell fates and cancer

LeBlanc

Ramirez

Kim

2021

Cell. Mol. Life Sci.

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Hippo effectors YAP and TAZ control cell fate and survival through various mechanisms, including transcriptional regulation of key genes. However, much of this research has been marked by conflicting results, as well as controversy over whether YAP and TAZ are redundant. A substantial portion of the discordance stems from their contradictory roles in stem cell self-renewal vs. differentiation and cancer cell survival vs. apoptosis. In this review, we present an overview of the multiple context-dependent functions of YAP and TAZ in regulating cell fate decisions in stem cells and organoids, as well as their mechanisms of controlling programmed cell death pathways in cancer.

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“…Interestingly, YAP1 is expressed in the human placenta and its levels are downregulated in patients with preeclampsia ( Sun et al , 2018 ), indicating that Hippo signaling may be important for human trophoblast lineage development. In support of this notion, a recent study using human cell models revealed that YAP1 and TEAD4 promote self-renewal of cytotrophoblast progenitor cells, while inhibiting formation of differentiated syncytiotrophoblast cells ( Meinhardt et al , 2020 ). Based on the function of the Hippo signaling pathway in mouse preimplantation embryos and embryos from other large animal species such as cattle and pigs ( Negron-Perez and Hansen, 2018 ; Cao et al , 2019 ; Emura et al , 2020 ; Sharma and Madan, 2020 ), it is easy to postulate that Hippo signaling plays a fundamental role in human preimplantation embryo development and early lineage formation.…”

Section: Discussionmentioning

confidence: 87%

A tale of two cell-fates: role of the Hippo signaling pathway and transcription factors in early lineage formation in mouse preimplantation embryos

Karasek

Ashry

Driscoll

et al. 2020

Molecular Human Reproduction

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Abstract In mammals, the first cell-fate decision occurs during preimplantation embryo development when the inner cell mass (ICM) and trophectoderm (TE) lineages are established. The ICM develops into the embryo proper, while the TE lineage forms the placenta. The underlying molecular mechanisms that govern lineage formation involve cell-to-cell interactions, cell polarisation, cell signaling and transcriptional regulation. In this review, we will discuss the current understanding regarding the cellular and molecular events that regulate lineage formation in mouse preimplantation embryos with an emphasis on cell polarity and the Hippo signaling pathway. Moreover, we will provide an overview on some of the molecular tools that are used to manipulate the Hippo pathway and study cell-fate decisions in early embryos. Lastly, we will provide exciting future perspectives on transcriptional regulatory mechanisms that modulate the activity of the Hippo pathway in preimplantation embryos to ensure robust lineage segregation.

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Pivotal role of the transcriptional co-activator YAP in trophoblast stemness of the developing human placenta

Cited by 99 publications

References 59 publications

Radial extracorporeal shockwave promotes subchondral bone stem/progenitor cell self-renewal by activating YAP/TAZ and facilitates cartilage repair in vivo

Radial extracorporeal shockwave promotes subchondral bone stem/progenitor cell self-renewal by activating YAP/TAZ and facilitates cartilage repair in vivo

Context-dependent roles of YAP/TAZ in stem cell fates and cancer

A tale of two cell-fates: role of the Hippo signaling pathway and transcription factors in early lineage formation in mouse preimplantation embryos

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