Temporal variability and cell mechanics control robustness in mammalian embryogenesis

How living systems achieve precision in form and function despite their intrinsic stochasticity is a fundamental yet ongoing question in biology. We generated morphomaps of preimplantation embryogenesis in mouse, rabbit, and monkey embryos, and these morphomaps revealed that although blastomere divi...

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Veröffentlicht in:Science (American Association for the Advancement of Science) 2024-10, Vol.386 (6718), p.eadh1145
Hauptverfasser: Fabrèges, Dimitri, Corominas-Murtra, Bernat, Moghe, Prachiti, Kickuth, Alison, Ichikawa, Takafumi, Iwatani, Chizuru, Tsukiyama, Tomoyuki, Daniel, Nathalie, Gering, Julie, Stokkermans, Anniek, Wolny, Adrian, Kreshuk, Anna, Duranthon, Véronique, Uhlmann, Virginie, Hannezo, Edouard, Hiiragi, Takashi
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Sprache:eng
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Zusammenfassung:How living systems achieve precision in form and function despite their intrinsic stochasticity is a fundamental yet ongoing question in biology. We generated morphomaps of preimplantation embryogenesis in mouse, rabbit, and monkey embryos, and these morphomaps revealed that although blastomere divisions desynchronized passively, 8-cell embryos converged toward robust three-dimensional shapes. Using topological analysis and genetic perturbations, we found that embryos progressively changed their cellular connectivity to a preferred topology, which could be predicted by a physical model in which actomyosin contractility and noise facilitate topological transitions, lowering surface energy. This mechanism favored regular embryo packing and promoted a higher number of inner cells in the 16-cell embryo. Synchronized division reduced embryo packing and generated substantially more misallocated cells and fewer inner-cell-mass cells. These findings suggest that stochasticity in division timing contributes to robust patterning.
ISSN:0036-8075
1095-9203
1095-9203
DOI:10.1126/science.adh1145