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切应力和基质-底物锚定对内皮细胞黏附和迁移的控制。

The control of endothelial cell adhesion and migration by shear stress and matrix-substrate anchorage.

机构信息

Leibniz Institute of Polymer Research Dresden, Max Bergmann Center of Biomaterials Dresden, Hohe Strasse 6, 01069 Dresden, Germany.

出版信息

Biomaterials. 2012 Mar;33(7):1959-69. doi: 10.1016/j.biomaterials.2011.11.017. Epub 2011 Dec 10.

DOI:10.1016/j.biomaterials.2011.11.017
PMID:22154622
Abstract

Endothelial cells constitute the natural inner lining of blood vessels and possess anti-thrombogenic properties. This characteristic is frequently used by seeding endothelial cells on vascular prostheses. As the type of anchorage of adhesion ligands to materials surfaces is known to determine the mechanical balance of adherent cells, we investigated herein the behaviour of endothelial cells under physiological shear stress conditions. The adhesion ligand fibronectin was anchored to polymer surfaces of four physicochemical characteristics exhibiting covalent and non-covalent attachment as well as high and low hydrophobicity. The in situ analysis combined with cell tracking of shear stress-induced effects on cultured isolated cells and monolayers under venous (0.5 dyn/cm(2)) and arterial (12 dyn/cm(2)) shear stress over a time period of 24 h revealed distinct differences in their morphological and migratory features. Most pronounced, unidirectional and bimodal migration patterns of endothelial cells in or against flow direction were found in dependence on the type of substrate-matrix anchorage. Combined by an immunofluorescent analysis of the actin cytoskeleton, cell-cell junctions, cell-matrix adhesions, and matrix reorganization these results revealed a distinct balance of laminar shear stress, cell-cell contacts and substrate-matrix anchorage in affecting endothelial cell fate under flow conditions. This analysis underlines the importance of materials surface parameters as well as primary and secondary adhesion ligand anchorage in the context of artificial blood vessels for future therapeutic devices.

摘要

内皮细胞构成血管的天然内层,具有抗血栓形成的特性。这种特性常被用于在血管假体上种植内皮细胞。由于已知粘附配体在材料表面上的附着方式决定了粘附细胞的机械平衡,我们在此研究了内皮细胞在生理剪切应力条件下的行为。将粘附配体纤维连接蛋白固定在具有四种物理化学特性的聚合物表面上,这些特性表现出共价和非共价附着以及高和低疏水性。原位分析结合细胞跟踪技术,对在静脉(0.5 dyn/cm(2))和动脉(12 dyn/cm(2))剪切应力下培养的分离细胞和单层细胞在 24 小时内的剪切应力诱导效应进行了研究,结果显示出它们在形态和迁移特征上存在明显的差异。最显著的是,在基质附着的类型的依赖下,内皮细胞在流动方向或逆流动方向上表现出单向和双峰迁移模式。通过对肌动蛋白细胞骨架、细胞-细胞连接、细胞-基质粘附和基质重排的免疫荧光分析,这些结果揭示了在流动条件下,层流剪切应力、细胞-细胞接触和基质附着在影响内皮细胞命运方面的明显平衡。这种分析强调了材料表面参数以及初级和次级粘附配体附着在未来治疗性设备人工血管中的重要性。

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