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Wnt5a Control of Cell Polarity and Directional Movement by Polarized Redistribution of Adhesion Receptors

机译:Wnt5a通过粘附受体的极化重新分布控制细胞极性和方向运动

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摘要

Mechanisms by which Wnt pathways integrate the organization of receptors, organelles, and cytoskeletal proteins to confer cell polarity and directional cell movement are incompletely understood. We show that acute responses to Wnt5a involve recruitment of actin, myosin IIB, Frizzled 3, and melanoma cell adhesion molecule into an intracellular structure in a melanoma cell line. In the presence of a chemokine gradient, this Wnt-mediated receptor–actin–myosin polarity (W-RAMP) structure accumulates asymmetrically at the cell periphery, where it triggers membrane contractility and nuclear movement in the direction of membrane retraction. The process requires endosome trafficking, is associated with multivesicular bodies, and is regulated by Wnt5a through the small guanosine triphosphatases Rab4 and RhoB. Thus, cell-autonomous mechanisms allow Wnt5a to control cell orientation, polarity, and directional movement in response to positional cues from chemokine gradients.
机译:Wnt途径整合受体,细胞器和细胞骨架蛋白的组织以赋予细胞极性和定向细胞运动的机制尚未完全了解。我们表明对Wnt5a的急性反应涉及肌动蛋白,肌球蛋白IIB,毛躁3和黑色素瘤细胞粘附分子募集到黑色素瘤细胞系的细胞内结构。在存在趋化因子梯度的情况下,这种Wnt介导的受体-肌动蛋白-肌球蛋白极性(W-RAMP)结构在细胞外围不对称累积,在细胞外围触发膜收缩和向膜收缩方向的核运动。该过程需要内体运输,与多囊泡体相关,并由Wnt5a通过小的鸟苷三磷酸酶Rab4和RhoB调控。因此,细胞自主机制允许Wnt5a响应来自趋化因子梯度的位置提示控制细胞的方向,极性和方向性运动。

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