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Boyden chamber-based method for characterizing the distribution of adhesions and cytoskeletal structure in HT1080 fibrosarcoma cells

机译:基于Boyden室的表征HT1080纤维肉瘤细胞黏附和细胞骨架结构分布的方法

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摘要

A 2D model was previously presented that describes the gliding motility of human fibrosarcoma cells. The model was based on the observation that adhesions are present only on the outer rim of the leading lamella of the semicircular cell. The present model describes the organization of adhesions and the cytoskeleton of migrating HT1080 fibrosarcoma and LX2 hepatic stellate cells in three dimensions. The migration assays were performed in a modified Boyden chamber using fibronectin, Matrigel, or collagen I as chemoattractants. The distribution of the adhesions was analyzed by confocal laser scanning microscope, and following decoration with heavy meromyosin, the organization of actin filaments was analyzed by electron microscopy. Double labeling was performed to study the relationship of the actin and vimentin filament network in the moving cells. Vinculin containing adhesions were observed only at the front of the cell in the form of a ring while passing through a filter pore of the Boyden chamber. Actin filaments were present only below the plasma membrane, except the very tip of the leading lamella. Vimentin intermediate filaments were localized around the cell nucleus behind the actin filament-rich lamella.This paper describes a model of the organization of adhesions and the cytoskeleton of migrating cells in the Boyden chamber. The model is based on the observation that adhesions are present only at the leading edge of the cell. The results extend the earlier 2D model of cell locomotion into 3D.
机译:先前已经提出了一种2D模型,该模型描述了人纤维肉瘤细胞的滑动运动。该模型基于以下观察结果:粘附仅存在于半圆形细胞前片的外缘。本模型从三个方面描述了HT1080纤维肉瘤和LX2肝星状细胞迁移的黏附组织和细胞骨架。使用纤连蛋白,基质胶或胶原蛋白I作为趋化剂,在改良的Boyden室中进行迁移测定。通过共聚焦激光扫描显微镜分析粘附的分布,并用重的肌球蛋白修饰后,通过电子显微镜分析肌动蛋白丝的组织。进行双重标记以研究运动细胞中肌动蛋白和波形蛋白丝网络的关系。通过波伊登室的过滤孔时,仅在细胞的前部以环形观察到含有长春花蛋白的粘附。肌动蛋白丝仅存在于质膜下方,除了前片的最尖端。波形蛋白中间丝位于富含肌动蛋白丝的薄层后面的细胞核周围。本文描述了博伊登室中粘附组织和迁移细胞的细胞骨架的模型。该模型基于观察结果,即粘附仅存在于细胞的前缘。结果将细胞运动的早期2D模型扩展为3D。

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