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活成纤维细胞中3'磷酸肌醇信号的空间分析,III:细胞形态和形态极性的影响。

Spatial analysis of 3' phosphoinositide signaling in living fibroblasts, III: influence of cell morphology and morphological Polarity.

作者信息

Schneider Ian C, Parrish Elizabeth M, Haugh Jason M

机构信息

Department of Chemical & Biomolecular Engineering, North Carolina State University, Raleigh, 27695, USA.

出版信息

Biophys J. 2005 Aug;89(2):1420-30. doi: 10.1529/biophysj.105.061218. Epub 2005 May 27.

Abstract

Activation of phosphoinositide (PI) 3-kinase is a required signaling pathway in fibroblast migration directed by platelet-derived growth factor. The pattern of 3' PI lipids in the plasma membrane, integrating local PI 3-kinase activity as well as 3' PI diffusion and turnover, influences the spatiotemporal regulation of the cytoskeleton. In fibroblasts stimulated uniformly with platelet-derived growth factor, visualized using total internal reflection fluorescence microscopy, we consistently observed localized regions with significantly higher or lower 3' PI levels than adjacent regions (hot and cold spots, respectively). A typical cell contained multiple hot spots, coinciding with apparent leading edge structures, and at most one cold spot at the rear. Using a framework for finite-element modeling with actual cell contact area geometries, we find that although the 3' PI pattern is affected by irregular contact area shape, cell morphology alone cannot explain the presence of hot or cold spots. Our results and analysis instead suggest that these regions reflect different local 3' PI dynamics, specifically through a combination of mechanisms: enhanced PI 3-kinase activity, reduced 3' PI turnover, and possibly slow/constrained 3' PI diffusion. The morphological polarity of the cell may thus bias 3' PI signaling to promote persistent migration in fibroblasts.

摘要

磷脂酰肌醇(PI)3-激酶的激活是血小板衍生生长因子介导的成纤维细胞迁移所需的信号通路。质膜中3' PI脂质的模式,整合了局部PI 3-激酶活性以及3' PI的扩散和周转,影响细胞骨架的时空调节。在用全内反射荧光显微镜观察的、由血小板衍生生长因子均匀刺激的成纤维细胞中,我们始终观察到3' PI水平明显高于或低于相邻区域的局部区域(分别为热点和冷点)。一个典型的细胞包含多个热点,与明显的前沿结构重合,并且在细胞后部最多有一个冷点。使用具有实际细胞接触面积几何形状的有限元建模框架,我们发现尽管3' PI模式受不规则接触面积形状的影响,但仅细胞形态不能解释热点或冷点的存在。相反,我们的结果和分析表明,这些区域反映了不同的局部3' PI动态,具体是通过多种机制的组合:增强的PI 3-激酶活性、降低的3' PI周转,以及可能缓慢/受限的3' PI扩散。因此,细胞的形态极性可能会使3' PI信号偏向,以促进成纤维细胞的持续迁移。

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