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对人类软腭形态发生的分析支持腭融合的区域调控。

Analysis of human soft palate morphogenesis supports regional regulation of palatal fusion.

作者信息

Danescu Adrian, Mattson Melanie, Dool Carly, Diewert Virginia M, Richman Joy M

机构信息

Faculty of Dentistry, Life Sciences Institute, University of British Columbia, Vancouver, BC, Canada.

出版信息

J Anat. 2015 Oct;227(4):474-86. doi: 10.1111/joa.12365. Epub 2015 Aug 24.

Abstract

It is essential to complete palate closure at the correct time during fetal development, otherwise a serious malformation, cleft palate, will ensue. The steps in palate formation in humans take place between the 7th and 12th week and consist of outgrowth of palatal shelves from the paired maxillary prominences, reorientation of the shelves from vertical to horizontal, apposition of the medial surfaces, formation of a bilayered seam, degradation of the seam and bridging of mesenchyme. However, in the soft palate, the mechanism of closure is unclear. In previous studies it is possible to find support for both fusion and the alternative mechanism of merging. Here we densely sample the late embryonic-early fetal period between 54 and 74 days post-conception to determine the timing and mechanism of soft palate closure. We found the epithelial seam extends throughout the soft palates of 57-day specimens. Cytokeratin antibody staining detected the medial edge epithelium and distinguished clearly that cells in the midline retained their epithelial character. Compared with the hard palate, the epithelium is more rapidly degraded in the soft palate and only persists in the most posterior regions at 64 days. Our results are consistent with the soft palate following a developmentally more rapid program of fusion than the hard palate. Importantly, the two regions of the palate appear to be independently regulated and have their own internal clocks regulating the timing of seam removal. Considering data from human genetic and mouse studies, distinct anterior-posterior signaling mechanisms are likely to be at play in the human fetal palate.

摘要

在胎儿发育的正确时间完成腭部闭合至关重要,否则将导致严重的畸形——腭裂。人类腭部形成的步骤发生在第7至12周之间,包括腭突从成对的上颌突长出、腭突从垂直方向重新定向为水平方向、内侧表面贴合、形成双层缝、缝的降解以及间充质的桥接。然而,软腭的闭合机制尚不清楚。在以往的研究中,融合和另一种合并机制都能找到支持证据。在这里,我们对受孕后54至74天的胚胎晚期至胎儿早期进行密集采样,以确定软腭闭合的时间和机制。我们发现上皮缝在57天标本的整个软腭中延伸。细胞角蛋白抗体染色检测到内侧边缘上皮,并清楚地辨别出中线处的细胞保留了它们的上皮特征。与硬腭相比,软腭中的上皮降解更快,在64天时仅在最后部区域持续存在。我们的结果与软腭遵循比硬腭更快的发育融合程序一致。重要的是,腭部的这两个区域似乎是独立调节的,并且有各自内部的时钟来调节缝去除的时间。考虑到来自人类遗传学和小鼠研究的数据,不同的前后信号机制可能在人类胎儿腭部起作用。

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