4.8 Article

Multiscale analysis of single and double maternal-zygotic Myh9 and Myh10 mutants during mouse preimplantation development

ELIFE (2021)

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Journal

ELIFE
Volume 10, Issue -, Pages -

Publisher

eLIFE SCIENCES PUBL LTD
DOI: 10.7554/eLife.68536

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Categories

Biology

Funding

  1. Genetics and Developmental Biology unit at the Institut Curie (PICT-IBiSA@BDD), French National Research Infrastructure France-BioImaging [ANR-10-INBS-04]
  2. Institut Curie
  3. Centre National de la Recherche Scientifique (CNRS)
  4. Institut National de la Sante Et de la Recherche Me dicale (INSERM)
  5. ATIP-Avenir program
  6. Fondation Schlumberger pour l'Education et la Recherche via the Fondation pour la Recherche Medicale
  7. European Research Council Starting Grant [ERC-2017-StG 757557]
  8. European Molecular Biology Organization Young Investigator program (EMBO YIP)
  9. INSERM transversal program Human Development Cell Atlas (HuDeCA)
  10. Paris Sciences Lettres (PSL) 'nouvelle equipe' grant
  11. Paris Sciences Lettres (PSL) QLife grant [17-CONV-0005]
  12. Labex DEEP, IDEX PSL [ANR11-LABX-0044, ANR-10-IDEX-0001-02]
  13. Agence Nationale de la Recherche [2019/0253]
  14. European Union's Horizon 2020 research and innovation program under the Marie Sklodowska-Curie grant [666003]
  15. EMBO YIP bridging fund
  16. Carl Zeiss SAS [2019/0253]

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Studies have shown that actomyosin contractility plays a crucial role in driving mammalian embryo development, and even in cases of failed cell division, morphogenesis and fate specification can still take place in the embryo.
During the first days of mammalian development, the embryo forms the blastocyst, the structure responsible for implanting the mammalian embryo. Consisting of an epithelium enveloping the pluripotent inner cell mass and a fluid-filled lumen, the blastocyst results from a series of cleavage divisions, morphogenetic movements, and lineage specification. Recent studies have identified the essential role of actomyosin contractility in driving cytokinesis, morphogenesis, and fate specification, leading to the formation of the blastocyst. However, the preimplantation development of contractility mutants has not been characterized. Here, we generated single and double maternal-zygotic mutants of non-muscle myosin II heavy chains (NMHCs) to characterize them with multiscale imaging. We found that Myh9 (NMHC II-A) is the major NMHC during preimplantation development as its maternal-zygotic loss causes failed cytokinesis, increased duration of the cell cycle, weaker embryo compaction, and reduced differentiation, whereas Myh10 (NMHC II-B) maternal-zygotic loss is much less severe. Double maternal-zygotic mutants for Myh9 and Myh10 show a much stronger phenotype, failing most of the attempts of cytokinesis. We found that morphogenesis and fate specification are affected but nevertheless carry on in a timely fashion, regardless of the impact of the mutations on cell number. Strikingly, even when all cell divisions fail, the resulting single-celled embryo can initiate trophectoderm differentiation and lumen formation by accumulating fluid in increasingly large vacuoles. Therefore, contractility mutants reveal that fluid accumulation is a cell-autonomous process and that the preimplantation program carries on independently of successful cell division.

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