首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >PNAS Plus: Spatially modulated ephrinA1:EphA2 signaling increases local contractility and global focal adhesion dynamics to promote cell motility
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PNAS Plus: Spatially modulated ephrinA1:EphA2 signaling increases local contractility and global focal adhesion dynamics to promote cell motility

机译:PNAS Plus:空间调节的ephrinA1:EphA2信号传导可增加局部收缩力和全局粘着动力学从而促进细胞运动

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摘要

Recent studies have revealed pronounced effects of the spatial distribution of EphA2 receptors on cellular response to receptor activation. However, little is known about molecular mechanisms underlying this spatial sensitivity, in part due to lack of experimental systems. Here, we introduce a hybrid live-cell patterned supported lipid bilayer experimental platform in which the sites of EphA2 activation and integrin adhesion are spatially controlled. Using a series of live-cell imaging and single-molecule tracking experiments, we map the transmission of signals from ephrinA1:EphA2 complexes. Results show that ligand-dependent EphA2 activation induces localized myosin-dependent contractions while simultaneously increasing focal adhesion dynamics throughout the cell. Mechanistically, Src kinase is activated at sites of ephrinA1:EphA2 clustering and subsequently diffuses on the membrane to focal adhesions, where it up-regulates FAK and paxillin tyrosine phosphorylation. EphrinA1:EphA2 signaling triggers multiple cellular responses with differing spatial dependencies to enable a directed migratory response to spatially resolved contact with ephrinA1 ligands.
机译:最近的研究表明,EphA2受体的空间分布对细胞对受体激活的反应具有明显的影响。但是,对于这种空间敏感性的分子机制知之甚少,部分原因是缺乏实验系统。在这里,我们介绍了一个混合的活细胞模式支持脂质双层实验平台,其中EphA2激活和整联蛋白粘附的位置在空间上受到控制。使用一系列活细胞成像和单分子跟踪实验,我们绘制了ephrinA1:EphA2复合物的信号传递图。结果表明,依赖配体的EphA2激活诱导局部的肌球蛋白依赖的收缩,同时增加整个细胞的粘着斑动态。从机理上讲,Src激酶在ephrinA1:EphA2聚集的位置被激活,然后在膜上扩散至粘着斑,从而上调FAK和paxillin酪氨酸磷酸化。 EphrinA1:EphA2信号触发具有不同空间依赖性的多种细胞反应,从而实现针对与ephrinA1配体的空间分辨接触的定向迁移反应。

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