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Non-canonical Wnt signaling regulates cell polarity in female reproductive tract development via van gogh-like 2

机译:非经典Wnt信号调节女性的细胞极性 通过梵高样2的生殖道发育

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摘要

Wnt signaling effectors direct the development and adult remodeling of the female reproductive tract (FRT); however, the role of non-canonical Wnt signaling has not been explored in this tissue. The non-canonical Wnt signaling protein van gogh-like 2 is mutated in loop-tail (Lp) mutant mice (Vangl2Lp), which display defects in multiple tissues. We find that Vangl2Lp mutant uterine epithelium displays altered cell polarity, concommitant with changes in cytoskeletal actin and scribble (scribbled, Scrb1) localization. The postnatal mutant phenotype is an exacerbation of that seen at birth, exhibiting more smooth muscle and reduced stromal mesenchyme. These data suggest that early changes in cell polarity have lasting consequences for FRT development. Furthermore, Vangl2 is required to restrict Scrb1 protein to the basolateral epithelial membrane in the neonatal uterus, and an accumulation of fibrillar-like structures observed by electron microscopy in Vangl2Lp mutant epithelium suggests that mislocalization of Scrb1 in mutants alters the composition of the apical face of the epithelium. Heterozygous and homozygous Vangl2Lp mutant postnatal tissues exhibit similar phenotypes and polarity defects and display a 50% reduction in Wnt7a levels, suggesting that the Vangl2Lp mutation acts dominantly in the FRT. These studies demonstrate that the establishment and maintenance of cell polarity through non-canonical Wnt signaling are required for FRT development.
机译:Wnt信号转导因子指导女性生殖道(FRT)的发育和成年重塑;然而,尚未在该组织中探索非经典Wnt信号传导的作用。非经典的Wnt信号蛋白梵高样2在环尾(Lp)突变小鼠(Vangl2Lp)中突变,该小鼠在多个组织中显示缺陷。我们发现,Vangl2Lp突变子宫上皮显示出改变的细胞极性,并伴随着细胞骨架肌动蛋白和涂抹(涂抹,Scrb1)本地化的变化。出生后的突变表型加剧了出生时的表现,表现出更平滑的肌肉和减少的间质。这些数据表明,细胞极性的早期改变对FRT的发展具有持久的影响。此外,需要Vangl2将Scrb1蛋白限制在新生儿子宫的基底外侧上皮膜上,并且通过电子显微镜观察到的Vangl2Lp突变体上皮中纤维状结构的积累表明,Srbb1在突变体中的定位不正确会改变其顶表面的组成。上皮。杂合子和纯合子的Vangl2Lp突变产后组织表现出相似的表型和极性缺陷,并且Wnt7a水平降低了50%,这表明Vangl2Lp突变在FRT中起主要作用。这些研究表明,通过FRT开发需要通过非规范的Wnt信号来建立和维持细胞极性。

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