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Neural crest cells bulldoze through the microenvironment using Aquaporin 1 to stabilize filopodia

机译:通过使用水素1来稳定箔片的神经嵴细胞膨胀微量环境

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摘要

Neural crest migration requires cells to move through an environment filled with dense extracellular matrix and mesoderm to reach targets throughout the vertebrate embryo. Here, we use high-resolution microscopy, computational modeling, and in vitro and in vivo cell invasion assays to investigate the function of Aquaporin 1 (AQP-1) signaling. We find that migrating lead cranial neural crest cells express AQP-1 mRNA and protein, implicating a biological role for water channel protein function during invasion. Differential AQP-1 levels affect neural crest cell speed and direction, as well as the length and stability of cell filopodia. Furthermore, AQP-1 enhances matrix metalloprotease activity and colocalizes with phosphorylated focal adhesion kinases. Colocalization of AQP-1 with EphB guidance receptors in the same migrating neural crest cells has novel implications for the concept of guided bulldozing by lead cells during migration.
机译:神经嵴迁移需要细胞穿过含有致密细胞外基质的环境和中胚层,以在整个脊椎动物胚胎中到达靶标。 在这里,我们使用高分辨率显微镜,计算建模和体外和体内细胞侵袭测定来研究水上素1(AQP-1)信号传导的功能。 我们发现迁移铅颅神经嵴细胞表达AQP-1 mRNA和蛋白质,对侵袭过程中的水通道蛋白质功能表示生物学作用。 差分AQP-1水平影响神经嵴细胞速度和方向,以及细胞氟化绦虫的长度和稳定性。 此外,AQP-1增强了基质金属蛋白酶活性,并用磷酸化的焦粘激酶结合。 在同一迁移神经嵴细胞中具有Ephb引导受体的AQP-1的分致化对迁移期间铅细胞引导推土的概念具有新颖的影响。

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