The failure to reconstitute the second extracellular matrix-integrin-cytoskeleton system in human endothelial cells on type V collagen.

Artery Pub Date : 1994-01-01
K Yamamoto, M Yamamoto
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Abstract

We examined the formation of F-actin filaments and the expression of beta 1 integrin in human vascular endothelial cells cultured on type V collagen. The cells attached to the exogenous substrate, formed complete F-actin filaments, and expressed vinculin and beta 1 integrin 0.5-1 h after inoculation. These phenomena are referred to as the first ECM-integrin-cytoskeleton system. After 3-6 h, disassembly of the F-actin filaments was observed to occur from the leading edges, and the cells developed focal adhesions only in their central regions. After 12-24 h, the cells on the type V collagen failed to form the second ECM-integrin-cytoskeleton system, and gradually detached from the substrate. In contrast, the cells on type I collagen developed both the first and second system, and acclimatized themselves to the environment. Thrombospondin (TSP), an anti-adhesive protein, was capable of inhibiting the spreading of the cells both after 1 h and 24 h. However, type V collagen treated with TSP inhibited the cell spreading after 1 h, but not after 24 h. The attachment and spreading of the cells on type V collagen were little affected by an anti-TSP antibody and the synthetic peptide GRGDSP (Gly-Arg-Gly-Asp-Ser-Pro), which significantly inhibited the attachment and spreading of the cells on TSP. Taken together, these results suggest that the cell detachment from type V collagen is not attributed to endogenously produced TSP (or member of TSP family) with anti-adhesive properties, but resulted from the failure to reconstitute the second ECM-integrin-cytoskeleton system in focal adhesion.

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在V型胶原蛋白上重建人内皮细胞第二细胞外基质-整合素-细胞骨架系统的失败。
我们检测了V型胶原培养的人血管内皮细胞中f -肌动蛋白丝的形成和β 1整合素的表达。细胞附着在外源底物上,形成完整的f -肌动蛋白丝,并在接种0.5-1 h后表达血管素和β 1整合素。这些现象被称为第一个ecm -整合素-细胞骨架系统。3-6小时后,观察到f -肌动蛋白丝在前缘发生断裂,细胞仅在其中心区域发生局灶性粘连。12-24 h后,V型胶原上的细胞未能形成第二ecm -整合素-细胞骨架系统,并逐渐脱离底物。相比之下,I型胶原蛋白上的细胞同时发育了第一和第二系统,并使自己适应了环境。血小板反应蛋白(TSP) anti-adhesive蛋白质,既能抑制细胞的扩散后1 h和24 h。然而,V型胶原蛋白治疗、抑制细胞扩散后1 h,但不是在24 h。细胞的吸附和扩散对V型胶原蛋白小受一个anti-TSP抗体和合成肽GRGDSP (Gly-Arg-Gly-Asp-Ser-Pro),大大抑制了细胞的吸附和扩散在TSP。综上所述,这些结果表明,细胞脱离V型胶原不是由于内源性产生具有抗黏附特性的TSP(或TSP家族成员),而是由于在局灶黏附中未能重建第二ecm -整合素-细胞骨架系统。
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