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PRAMEL7 and CUL2 decrease NuRD stability to establish ground-state pluripotency.


ABSTRACT: Pluripotency is established in E4.5 preimplantation epiblast. Embryonic stem cells (ESCs) represent the immortalization of pluripotency, however, their gene expression signature only partially resembles that of developmental ground-state. Induced PRAMEL7 expression, a protein highly expressed in the ICM but lowly expressed in ESCs, reprograms developmentally advanced ESC+serum into ground-state pluripotency by inducing a gene expression signature close to developmental ground-state. However, how PRAMEL7 reprograms gene expression remains elusive. Here we show that PRAMEL7 associates with Cullin2 (CUL2) and this interaction is required to establish ground-state gene expression. PRAMEL7 recruits CUL2 to chromatin and targets regulators of repressive chromatin, including the NuRD complex, for proteasomal degradation. PRAMEL7 antagonizes NuRD-mediated repression of genes implicated in pluripotency by decreasing NuRD stability and promoter association in a CUL2-dependent manner. Our data link proteasome degradation pathways to ground-state gene expression, offering insights to generate in vitro models to reproduce the in vivo ground-state pluripotency.

SUBMITTER: Rupasinghe M 

PROVIDER: S-EPMC10933316 | biostudies-literature | 2024 Mar

REPOSITORIES: biostudies-literature

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PRAMEL7 and CUL2 decrease NuRD stability to establish ground-state pluripotency.

Rupasinghe Meneka M   Bersaglieri Cristiana C   Leslie Pedrioli Deena M DM   Pedrioli Patrick Ga PG   Panatta Martina M   Hottiger Michael O MO   Cinelli Paolo P   Santoro Raffaella R  

EMBO reports 20240208 3


Pluripotency is established in E4.5 preimplantation epiblast. Embryonic stem cells (ESCs) represent the immortalization of pluripotency, however, their gene expression signature only partially resembles that of developmental ground-state. Induced PRAMEL7 expression, a protein highly expressed in the ICM but lowly expressed in ESCs, reprograms developmentally advanced ESC+serum into ground-state pluripotency by inducing a gene expression signature close to developmental ground-state. However, how  ...[more]

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