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Prostaglandin E2 alters Wnt-dependent migration and proliferation in neuroectodermal stem cells: implications for autism spectrum disorders

机译:前列腺素E2改变神经外胚层干细胞中Wnt依赖性迁移和增殖:对自闭症谱系障碍的影响

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摘要

Prostaglandin E2 (PGE2) is a natural lipid-derived molecule that is involved in important physiological functions. Abnormal PGE2 signalling has been associated with pathologies of the nervous system. Previous studies provide evidence for the interaction of PGE2 and canonical Wnt signalling pathways in non-neuronal cells. Since the Wnt pathway is crucial in the development and organization of the brain, the main goal of this study is to determine whether collaboration between these pathways exists in neuronal cell types. We report that PGE2 interacts with canonical Wnt signalling through PKA and PI-3K in neuroectodermal (NE-4C) stem cells. We used time-lapse microscopy to determine that PGE2 increases the final distance from origin, path length travelled, and the average speed of migration in Wnt-activated cells. Furthermore, PGE2 alters distinct cellular phenotypes that are characteristic of Wnt-induced NE-4C cells, which corresponds to the modified splitting behaviour of the cells. We also found that in Wnt-induced cells the level of β-catenin protein was increased and the expression levels of Wnt-target genes (Ctnnb1, Ptgs2, Ccnd1, Mmp9) was significantly upregulated in response to PGE2 treatment. This confirms that PGE2 activated the canonical Wnt signalling pathway. Furthermore, the upregulated genes have been previously associated with ASD. Our findings show, for the first time, evidence for cross-talk between PGE2 and Wnt signalling in neuronal cells, where PKA and PI-3K might act as mediators between the two pathways. Given the importance of PGE2 and Wnt signalling in prenatal development of the nervous system, our study provides insight into how interaction between these two pathways may influence neurodevelopment.
机译:前列腺素E2(PGE2)是一种天然的脂质衍生分子,参与重要的生理功能。 PGE2信号异常与神经系统病变有关。先前的研究为非神经元细胞中PGE2和经典Wnt信号通路的相互作用提供了证据。由于Wnt途径对于大脑的发育和组织至关重要,因此本研究的主要目标是确定神经细胞类型中是否存在这些途径之间的协作。我们报告说,PGE2与神经外皮(NE-4C)干细胞中通过PKA和PI-3K的经典Wnt信号相互作用。我们使用延时显微镜确定PGE2增加了距原点的最终距离,行进的路径长度以及Wnt激活的细胞的平均迁移速度。此外,PGE 2改变了Wnt诱导的NE-4C细胞特征性的独特细胞表型,这与细胞的改良分裂行为相对应。我们还发现,在Wnt诱导的细胞中,β-catenin蛋白的水平增加,并且响应PGE2处理,Wnt靶基因(Ctnnb1,Ptgs2,Ccnd1,Mmp9)的表达水平显着上调。这证实了PGE2激活了经典的Wnt信号通路。此外,上调的基因先前已与ASD相关。我们的发现首次显示了神经元细胞中PGE2和Wnt信号之间串扰的证据,其中PKA和PI-3K可能是这两种途径之间的介体。鉴于PGE2和Wnt信号传导在神经系统产前发育中的重要性,我们的研究提供了关于这两种途径之间相互作用如何影响神经发育的见解。

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