| Literature DB >> 29576449 |
Jennifer Zenker1, Melanie D White1, Maxime Gasnier1, Yanina D Alvarez2, Hui Yi Grace Lim1, Stephanie Bissiere1, Maté Biro3, Nicolas Plachta4.
Abstract
Transformation from morula to blastocyst is a defining event of preimplantation embryo development. During this transition, the embryo must establish a paracellular permeability barrier to enable expansion of the blastocyst cavity. Here, using live imaging of mouse embryos, we reveal an actin-zippering mechanism driving this embryo sealing. Preceding blastocyst stage, a cortical F-actin ring assembles at the apical pole of the embryo's outer cells. The ring structure forms when cortical actin flows encounter a network of polar microtubules that exclude F-actin. Unlike stereotypical actin rings, the actin rings of the mouse embryo are not contractile, but instead, they expand to the cell-cell junctions. Here, they couple to the junctions by recruiting and stabilizing adherens and tight junction components. Coupling of the actin rings triggers localized myosin II accumulation, and it initiates a tension-dependent zippering mechanism along the junctions that is required to seal the embryo for blastocyst formation.Entities:
Keywords: actin dynamics; blastocyst; cortical flow; epithelia; live imaging; mammalian development; microtubules; morphogenesis; preimplantation mouse embryo; tight junctions
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Year: 2018 PMID: 29576449 DOI: 10.1016/j.cell.2018.02.035
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582