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微孔YIGSR/PEG修饰聚脲聚氨酯的内皮化

Endothelialization of microporous YIGSR/PEG-modified polyurethaneurea.

作者信息

Jun Ho-Wook, West Jennifer L

机构信息

Department of Bioengineering, Rice University, Houston, TX 77005, USA.

出版信息

Tissue Eng. 2005 Jul-Aug;11(7-8):1133-40. doi: 10.1089/ten.2005.11.1133.

Abstract

Bioactive polyurethaneurea modified with polyethylene glycol (PEG) and the endothelial cell-adhesive peptide YIGSR was synthesized and fabricated into microporous scaffolds. This material has shown appropriate mechanical properties for vascular graft applications, resists platelet adhesion, and promotes endothelialization. In the current study, microporous scaffolds were formed by a gasfoaming and salt-leaching method. The scaffolds showed highly interconnected open pores throughout the matrices, with porosity of approximately 78% and pore sizes of 20-200 microm. The peptide modified scaffolds showed superior mechanical properties over peptide-free scaffolds (tensile strength, 1.4 +/- 0.03 versus 0.19 +/- 0.01 MPa; p < 0.01). Bovine aortic endothelial cells were seeded on the scaffolds, and cell attachment, proliferation, extracellular matrix production, and migration were investigated. Histological and scanning electron microscopy analysis showed that few cells adhered on peptide-free scaffolds, whereas confluent endothelial cell monolayers formed along the pores in peptide-modified scaffolds. DNA content, hydroxyproline production, and cell migration were also significantly greater in peptide-modified scaffolds.

摘要

用聚乙二醇(PEG)和内皮细胞黏附肽YIGSR改性的生物活性聚脲氨酯被合成并制成微孔支架。这种材料已显示出适用于血管移植应用的机械性能,能抵抗血小板黏附,并促进内皮化。在当前研究中,微孔支架通过气体发泡和盐沥滤法形成。支架在整个基质中显示出高度相互连通的开孔,孔隙率约为78%,孔径为20 - 200微米。肽修饰的支架比无肽支架显示出更好的机械性能(拉伸强度,1.4±0.03对0.19±0.01兆帕;p < 0.01)。将牛主动脉内皮细胞接种在支架上,研究细胞黏附、增殖、细胞外基质产生和迁移。组织学和扫描电子显微镜分析表明,无肽支架上几乎没有细胞黏附,而在肽修饰的支架中,沿孔隙形成了融合的内皮细胞单层。肽修饰的支架中的DNA含量、羟脯氨酸产生和细胞迁移也显著更高。

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