Four simple rules that are sufficient to generate the mammalian blastocyst.
Silas Boye NissenMarta PereraJavier Martin GonzalezSophie M MorganiMogens H JensenKim SneppenJoshua M BrickmanAla TrusinaPublished in: PLoS biology (2017)
Early mammalian development is both highly regulative and self-organizing. It involves the interplay of cell position, predetermined gene regulatory networks, and environmental interactions to generate the physical arrangement of the blastocyst with precise timing. However, this process occurs in the absence of maternal information and in the presence of transcriptional stochasticity. How does the preimplantation embryo ensure robust, reproducible development in this context? It utilizes a versatile toolbox that includes complex intracellular networks coupled to cell-cell communication, segregation by differential adhesion, and apoptosis. Here, we ask whether a minimal set of developmental rules based on this toolbox is sufficient for successful blastocyst development, and to what extent these rules can explain mutant and experimental phenotypes. We implemented experimentally reported mechanisms for polarity, cell-cell signaling, adhesion, and apoptosis as a set of developmental rules in an agent-based in silico model of physically interacting cells. We find that this model quantitatively reproduces specific mutant phenotypes and provides an explanation for the emergence of heterogeneity without requiring any initial transcriptional variation. It also suggests that a fixed time point for the cells' competence of fibroblast growth factor (FGF)/extracellular signal-regulated kinase (ERK) sets an embryonic clock that enables certain scaling phenomena, a concept that we evaluate quantitatively by manipulating embryos in vitro. Based on these observations, we conclude that the minimal set of rules enables the embryo to experiment with stochastic gene expression and could provide the robustness necessary for the evolutionary diversification of the preimplantation gene regulatory network.
Keyphrases
- single cell
- gene expression
- cell cycle arrest
- cell therapy
- induced apoptosis
- oxidative stress
- transcription factor
- signaling pathway
- healthcare
- body mass index
- escherichia coli
- mental health
- cell proliferation
- stem cells
- mesenchymal stem cells
- weight loss
- bone marrow
- climate change
- heat shock
- biofilm formation
- protein kinase
- tyrosine kinase
- heat shock protein
- birth weight
- human health
- cell adhesion