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Cell–Matrix Entanglement and Mechanical Anchorage of Fibroblasts in Three-dimensional Collagen Matrices

机译:三维胶原基质中成纤维细胞的细胞基质缠结和机械锚固

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Fibroblast-3D collagen matrix culture provides a physiologically relevant model to study cell–matrix interactions. In tissues, fibroblasts are phagocytic cells, and in culture, they have been shown to ingest both fibronectin and collagen-coated latex particles. Compared with cells on collagen-coated coverslips, phagocytosis of fibronectin-coated beads by fibroblasts in collagen matrices was found to be reduced. This decrease could not be explained by integrin reorganization, tight binding of fibronectin beads to the collagen matrix, or differences in overall bead binding to the cells. Rather, entanglement of cellular dendritic extensions with collagen fibrils seemed to interfere with the ability of the extensions to interact with the beads. Moreover, once these extensions became entangled in the matrix, cells developed an integrin-independent component of adhesion. We suggest that cell–matrix entanglement represents a novel mechanism of cell anchorage that uniquely depends on the three-dimensional character of the matrix.
机译:成纤维细胞3D胶原基质培养提供了一种生理学相关的模型来研究细胞与基质的相互作用。在组织中,成纤维细胞是吞噬细胞,在培养中,它们被摄入纤维连接蛋白和胶原蛋白包被的乳胶颗粒。与胶原包被的盖玻片上的细胞相比,发现胶原基质中的成纤维细胞对纤连蛋白包被的珠的吞噬作用降低。这种减少不能通过整联蛋白重组,纤连蛋白珠与胶原蛋白基质的紧密结合或珠与细胞整体结合的差异来解释。而是,细胞树突状延伸物与胶原原纤维的缠结似乎干扰了延伸物与珠相互作用的能力。此外,一旦这些延伸物缠绕在基质中,细胞就会形成不依赖整合素的成分。我们建议细胞与基质的缠结代表细胞锚固的新机制,该机制独特地取决于基质的三维特征。

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