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首页> 外文期刊>Placenta >Early placental ontogeny in the mouse.
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Early placental ontogeny in the mouse.

机译:小鼠的早期胎盘发育。

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摘要

Fundamental to placental morphogenesis is union between the allantois and the chorion, two tissues initially separated in the conceptus. Results of previous studies in the mouse have suggested that chorio-allantoic union is driven by the developmental maturity of the allantois and involves molecular interactions between Vascular Cell Adhesion Molecule (VCAM-1) in the allantois and alpha4-integrin in the chorion. Little more is known about the cellular and/or molecular control of this important morphogenetic event in any species.Gross, histological, microsurgical and immunohistochemical analyses in the mouse conceptus revealed that placental ontogeny took place in three major steps. The first, chorio-allantoic contact, was not enduring and was mediated by the allantois' mesothelial surface and the mesodermal component of the chorion. Modest amounts of VCAM-1 were found in distal allantoic mesothelium, whilst levels of alpha4-integrin were high throughout chorionic mesoderm. The second step, chorio-allantoic fusion, was more enduring. During this time, the distal allantoic region contained maximal levels of VCAM-1, and all allantoises had expanded far enough to reach the posterior chorion from where they spread toward a central chorionic depression. The last step, breakdown of chorio-allantoic fusing surfaces, was dependent upon chorio-allantoic fusion and resulted in the intimate juxtaposition of allantoic endothelium and chorionic ectoderm, possibly as a result of VCAM-1-mediated interactions. The umbilical connection was thereafter fixed at its perimeter to the chorionic surface by large amounts of VCAM-1 in disto-lateral allantoic mesothelium and alpha4-integrin in the remaining peripheral mesodermal component of the chorion.Thus, chorio-allantoic union is highly regulated, taking place in multiple steps. It is dependent upon the developmental maturity of distal allantoic mesothelium and involves the mesodermal component of the chorion. Breakdown of fusing surfaces enables penetration of the allantoic vasculature into the chorion. These findings provide a secure developmental foundation in which to elucidate the genetic control of early placentation.
机译:胎盘形态发生的基础是尿囊和绒毛膜之间的结合,这两个组织最初在概念中是分开的。小鼠先前的研究结果表明,绒毛膜尿囊的联合是由尿囊的发育成熟所驱动的,并且涉及尿囊中的血管细胞粘附分子(VCAM-1)与绒毛膜中的α4-整联蛋白之间的分子相互作用。对任何物种中重要的形态发生事件的细胞和/或分子控制知之甚少。小鼠概念中的总的,组织学的,显微外科的和免疫组织化学分析表明,胎盘的发生是通过三个主要步骤进行的。第一次绒毛膜-尿囊接触并不持久,并且由尿囊的间皮表面和绒毛膜的中胚层成分介导。在远端尿囊上皮中发现适量的VCAM-1,而整个绒毛膜中胚层中的α4-整联蛋白水平较高。第二步,绒毛膜-尿囊融合术,更持久。在这段时间中,远端尿囊区含有最高水平的VCAM-1,所有尿囊均已扩张到足以到达后绒毛膜的程度,从那里扩散到中央绒毛膜凹陷。最后一步,绒毛膜-尿囊融合表面的破裂,取决于绒毛膜-尿囊融合并导致尿囊内皮和绒毛膜外胚层紧密并置,可能是由于VCAM-1介导的相互作用。此后,脐带连接被绒毛的单侧尿囊间质中的大量VCAM-1和绒毛膜其余外围中胚层成分中的α4-整联蛋白固定在绒毛膜表面。因此,绒毛膜-尿囊的结合受到高度调节,分多个步骤进行。它取决于远端尿囊上皮的发育成熟程度,并涉及绒毛膜的中胚层成分。融合表面的破坏使尿囊血管渗入绒毛膜。这些发现为阐明早期胎盘的遗传控制提供了可靠的发展基础。

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