Litcius/Paper detail

The primitive endoderm supports lineage plasticity to enable regulative development

Madeleine Linneberg-Agerholm, Annika Charlotte Sell, Alba Redó Riveiro, Marta Perera, Martin Proks, Teresa E. Knudsen, Antonio Barral, Miguel Manzanares, Joshua M. Brickman

2024Cell34 citationsDOIOpen Access PDF

Abstract

Mammalian blastocyst formation involves the specification of the trophectoderm followed by the differentiation of the inner cell mass into embryonic epiblast and extra-embryonic primitive endoderm (PrE). During this time, the embryo maintains a window of plasticity and can redirect its cellular fate when challenged experimentally. In this context, we found that the PrE alone was sufficient to regenerate a complete blastocyst and continue post-implantation development. We identify an in vitro population similar to the early PrE in vivo that exhibits the same embryonic and extra-embryonic potency and can form complete stem cell-based embryo models, termed blastoids. Commitment in the PrE is suppressed by JAK/STAT signaling, collaborating with OCT4 and the sustained expression of a subset of pluripotency-related transcription factors that safeguard an enhancer landscape permissive for multi-lineage differentiation. Our observations support the notion that transcription factor persistence underlies plasticity in regulative development and highlight the importance of the PrE in perturbed development.

Topics & Concepts

EpiblastBiologyEndodermEmbryonic stem cellCell biologyBlastocystTranscription factorInner cell massEmbryogenesisCellular differentiationCell fate determinationEmbryoGeneticsGastrulationGenePluripotent Stem Cells ResearchCRISPR and Genetic EngineeringRenal and related cancers