首页> 外文期刊>Annals of Biomedical Engineering: The Journal of the Biomedical Engineering Society >Novel approach for endothelializing vascular devices: understanding and exploiting elastin-endothelial interactions.
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Novel approach for endothelializing vascular devices: understanding and exploiting elastin-endothelial interactions.

机译:血管装置内皮化的新方法:了解和利用弹性蛋白-内皮相互作用。

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摘要

Elastin is an essential component of arteries which provides structural integrity and instructs smooth muscle cells to adopt a quiescent state. Despite interaction of endothelial cells with elastin in the internal elastic lamina, the potential for exploiting this interaction therapeutically has not been explored in detail. In this study, we show that tropoelastin (a precursor of elastin) stimulates endothelial cell migration and adhesion more than smooth muscle cells. The biological activity of tropoelastin on endothelial cells is contained in the VGVAPG domain and in the carboxy-terminal 17-amino acids. We show that the effects of the carboxy-terminal 17 amino acids, but not those of VGVAPG, are mediated by integrin alpha(V)beta(3). We demonstrate that tropoelastin covalently linked to stainless steel disks promotes adhesion of endothelial progenitor cells and endothelial cells to the metal surfaces. The adherent cells on the tropoelastin-coated metal surfaces form monolayers that can withstand and respond to arterial shear stress. Because of the unique effects of tropoelastin on endothelial and smooth muscle cells, coating intravascular devices with tropoelastin may stimulate their endothelialization, inhibit smooth muscle hyperplasia, and improve device performance.
机译:弹性蛋白是动脉的重要组成部分,可提供结构完整性并指示平滑肌细胞进入静止状态。尽管内皮细胞与内部弹性层中的弹性蛋白相互作用,但尚未详细探讨在治疗上利用这种相互作用的潜力。在这项研究中,我们表明原弹性蛋白(弹性蛋白的前体)比平滑肌细胞更能刺激内皮细胞迁移和粘附。原弹性蛋白对内皮细胞的生物学活性包含在VGVAPG结构域和羧基末端的17个氨基酸中。我们表明,羧基末端17个氨基酸的作用,而不是VGVAPG的作用,是由整联蛋白alpha(V)beta(3)介导的。我们证明原弹性蛋白共价连接到不锈钢盘促进内皮祖细胞和内皮细胞对金属表面的粘附。原弹性蛋白涂层金属表面上的粘附细胞形成可以承受并响应动脉切应力的单层。由于原弹性蛋白对内皮细胞和平滑肌细胞的独特作用,用原弹性蛋白包被血管内装置可刺激其内皮化,抑制平滑肌增生并改善装置性能。

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