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Dynamic 3D Cell Rearrangements Guided by a Fibronectin Matrix Underlie Somitogenesis

机译:由纤连蛋白基质指导的动态3D细胞重排是促生的基础

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摘要

Somites are transient segments formed in a rostro-caudal progression during vertebrate development. In chick embryos, segmentation of a new pair of somites occurs every 90 minutes and involves a mesenchyme-to-epithelium transition of cells from the presomitic mesoderm. Little is known about the cellular rearrangements involved, and, although it is known that the fibronectin extracellular matrix is required, its actual role remains elusive. Using 3D and 4D imaging of somite formation we discovered that somitogenesis consists of a complex choreography of individual cell movements. Epithelialization starts medially with the formation of a transient epithelium of cuboidal cells, followed by cell elongation and reorganization into a pseudostratified epithelium of spindle-shaped epitheloid cells. Mesenchymal cells are then recruited to this medial epithelium through accretion, a phenomenon that spreads to all sides, except the lateral side of the forming somite, which epithelializes by cell elongation and intercalation. Surprisingly, an important contribution to the somite epithelium also comes from the continuous egression of mesenchymal cells from the core into the epithelium via its apical side. Inhibition of fibronectin matrix assembly first slows down the rate, and then halts somite formation, without affecting pseudopodial activity or cell body movements. Rather, cell elongation, centripetal alignment, N-cadherin polarization and egression are impaired, showing that the fibronectin matrix plays a role in polarizing and guiding the exploratory behavior of somitic cells. To our knowledge, this is the first 4D in vivo recording of a full mesenchyme-to-epithelium transition. This approach brought new insights into this event and highlighted the importance of the extracellular matrix as a guiding cue during morphogenesis.
机译:体节是脊椎动物发育过程中以尾状尾状进展形成的瞬时节段。在鸡胚中,每隔90分钟就会发生一对新的节段的分割,涉及从早熟中胚层到细胞的间质向上皮转换。关于所涉及的细胞重排知之甚少,尽管已知需要纤连蛋白胞外基质,但其实际作用仍然难以捉摸。使用3D和4D成像的体节形成,我们发现体节发生由单个细胞运动的复杂编排组成。上皮化在中间开始于立方细胞的瞬时上皮的形成,然后细胞伸长并重组为纺锤形上皮细胞的假复层上皮。然后,间充质细胞通过吸积被募集到该内侧上皮中,这种现象扩散到除形成的m突石的外侧以外的所有侧面,该现象通过细胞伸长和嵌入而上皮化。出人意料的是,对间质上皮的重要贡献还来自间充质细胞通过其顶侧从核心向上皮的连续排出。抑制纤连蛋白基质装配首先会减慢速率,然后停止体节的形成,而不会影响假足活动或细胞体运动。而是,细胞伸长,向心排列,N-钙粘着蛋白极化和外出受到损害,表明纤连蛋白基质在极化和引导体细胞的探索行为中起作用。据我们所知,这是第一个4D体内完整的间质到上皮细胞过渡的记录。这种方法为这一事件带来了新的见解,并强调了细胞外基质作为形态发生过程中的指导线索的重要性。

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