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Cell and molecular regulation of the mouse blastocyst.

机译:小鼠胚泡的细胞和分子调控。

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摘要

Animals use diverse strategies to specify tissue lineages during development. A common strategy is to partition maternally supplied and localized lineage determinants into progenitor cells. The mouse embryo appears to use a different, more regulative strategy to specify the first three lineages: the epiblast (EPI: future embryo), the trophectoderm (TE: future placenta), and the primitive endoderm (PE: future yolk sac). These lineages are specified during two successive differentiation steps leading to formation of the blastocyst. Here, we review classic and contemporary models of early lineage specification in the mouse, and describe recent efforts to understand the molecular regulation of these events. We describe evidence that trophectoderm differentiation bears resemblance to the process of epithelialization and describe the importance of apical/basal protein complexes in regulating this process. Next, we present a revised model of PE specification, and describe evidence that PE cells in the inner cell mass sort out to occupy their ultimate position on the surface of the EPI. Finally, we describe factors that reinforce these lineages and three distinct stem cell types that can be isolated from them. Together, these mechanisms guide the differentiation of the first lineages of the mouse and thereby set up tissues that will be important for the first steps of embryonic body patterning.
机译:动物在发育过程中使用多种策略来指定组织谱系。一种常见的策略是将母体提供的和定位的谱系决定簇分成祖细胞。小鼠胚胎似乎使用不同的,更具调节性的策略来指定前三个谱系:外胚层(EPI:未来胚胎),滋养外胚层(TE:未来胎盘)和原始内胚层(PE:未来卵黄囊)。这些谱系是在导致胚泡形成的两个连续分化步骤中确定的。在这里,我们审查小鼠早期谱系规范的经典和现代模型,并描述最近的努力,以了解这些事件的分子调控。我们描述了滋养外胚层分化与上皮形成过程相似的证据,并描述了顶端/基底蛋白复合物在调节该过程中的重要性。接下来,我们提出PE规范的修订模型,并描述证据表明内部细胞团中的PE细胞经过分选以占据其在EPI表面上的最终位置。最后,我们描述了强化这些谱系的因素以及可以从中分离出的三种不同的干细胞类型。这些机制共同引导了小鼠第一系的分化,从而建立了对于胚胎人体构图的第一步非常重要的组织。

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