Distinct Molecular Trajectories Converge to Induce Naive Pluripotency.
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Understanding how cell identity transitions occur and whether there are multiple paths between the same beginning and end states are questions of wide interest. Here we show that acquisition of naive pluripotency can follow transcriptionally and mechanistically distinct routes. Starting from post-implantation epiblast stem cells (EpiSCs), one route advances through a mesodermal state prior to naive pluripotency induction, whereas another transiently resembles the early inner cell mass and correspondingly gains greater developmental potency. These routes utilize distinct signaling networks and transcription factors but subsequently converge on the same naive endpoint, showing surprising flexibility in mechanisms underlying identity transitions and suggesting that naive pluripotency is a multidimensional attractor state. These route differences are reconciled by precise expression of Oct4 as a unifying, essential, and sufficient feature. We propose that fine-tuned regulation of this "transition factor" underpins multidimensional access to naive pluripotency, offering a conceptual framework for understanding cell identity transitions.
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1875-9777
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Wellcome Trust (097922/Z/11/Z)
Wellcome Trust (105031/D/14/Z)
Medical Research Council (MR/R017735/1)
Medical Research Council (MC_PC_12009)
Biotechnology and Biological Sciences Research Council (BB/M004023/1)
Biotechnology and Biological Sciences Research Council (BB/P009867/1)
Biotechnology and Biological Sciences Research Council (BB/R018588/1)