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不同类型的 IV 型胶原在亲水和疏水基底上的组装改变了内皮细胞的相互作用。

Different assembly of type IV collagen on hydrophilic and hydrophobic substrata alters endothelial cells interaction.

机构信息

Institut de Bioenginyeria de Catalunya, Barcelona, Spain.

出版信息

Eur Cell Mater. 2010 Jun 9;19:262-72. doi: 10.22203/ecm.v019a25.

DOI:10.22203/ecm.v019a25
PMID:20533192
Abstract

Considering the structural role of type IV collagen (Col IV) in the assembly of the basement membrane (BM) and the perspective of mimicking its organization for vascular tissue engineering purposes, we studied the adsorption pattern of this protein on model hydrophilic (clean glass) and hydrophobic trichloro(octadecyl)silane (ODS) surfaces known to strongly affect the behavior of other matrix proteins. The amount of fluorescently labeled Col IV was quantified showing saturation of the surface for concentration of the adsorbing solution of about 50microg/ml, but with approximately twice more adsorbed protein on ODS. AFM studies revealed a fine - nearly single molecular size - network arrangement of Col IV on hydrophilic glass, which turns into a prominent and growing polygonal network consisting of molecular aggregates on hydrophobic ODS. The protein layer forms within minutes in a concentration-dependent manner. We further found that human umbilical vein endothelial cells (HUVEC) attach less efficiently to the aggregated Col IV (on ODS), as judged by the significantly altered cell spreading, focal adhesions formation and the development of actin cytoskeleton. Conversely, the immunofluorescence studies for integrins revealed that the fine Col IV network formed on hydrophilic substrata is better recognized by the cells via both alpha1 and alpha2 heterodimers which support cellular interaction, apart from these on hydrophobic ODS where almost no clustering of integrins was observed.

摘要

考虑到 IV 型胶原蛋白 (Col IV) 在基底膜 (BM) 组装中的结构作用,以及模拟其组织以用于血管组织工程的观点,我们研究了该蛋白质在亲水(清洁玻璃)和疏水三氯 (十八烷基) 硅烷 (ODS) 模型表面上的吸附模式,这些表面已知会强烈影响其他基质蛋白的行为。用荧光标记 Col IV 的量进行定量,结果表明表面吸附溶液的浓度约为 50μg/ml 时达到饱和,但在 ODS 上吸附的蛋白质约多两倍。原子力显微镜研究显示 Col IV 在亲水玻璃上呈现出精细的 - 几乎是单分子大小的 - 网络排列,而在疏水 ODS 上则变成明显且不断增长的由分子聚集体组成的多边形网络。该蛋白质层以浓度依赖的方式在数分钟内形成。我们还发现,人脐静脉内皮细胞 (HUVEC) 在疏水性 ODS 上的附着效率较低,这可以通过细胞明显改变的铺展、焦点黏附形成和肌动蛋白细胞骨架的发育来判断。相反,通过免疫荧光研究整合素发现,在亲水基质上形成的精细 Col IV 网络通过支持细胞相互作用的 alpha1 和 alpha2 异二聚体被细胞更好地识别,而在几乎观察不到整合素聚集的疏水 ODS 上则没有。

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