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首页> 外文期刊>Biomaterials >Electrospun sulfated silk fibroin nanofibrous scaffolds for vascular tissue engineering.
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Electrospun sulfated silk fibroin nanofibrous scaffolds for vascular tissue engineering.

机译:静电纺丝的硫酸丝素蛋白纳米纤维支架,用于血管组织工程。

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One of the major downfalls of tissue-engineered small-diameter vascular grafts is the inability to obtain a confluent endothelium on the lumenal surface. Loosely attached endothelial cells (ECs) are easily separated from the vessel wall when exposed to the in vivo vascular system. Thus any denuded areas on the lumenal surface of vascular grafts may lead to thrombus formation via platelet deposition and activation. If the denuded areas could express anticoagulant activity until the endothelial cell lining is fully achieved, it may greatly improve the chances of successful vascular reconstruction. In this study, we fabricate sulfated silk fibroin nanofibrous scaffolds (S-silk scaffolds) and assess the anticoagulant activity and cytocompatibility of S-silk scaffolds in vitro in order to improve the antithrombogenicity and get some insights into its potential use for vascular tissue engineering. Sulfated silk fibroin was prepared by reaction with chlorosulphonic acid in pyridine, and then was developed to form an S-silk scaffold by electrospinning technique. FTIR analyses identified the successful incorporation of sulfate groups in silk fibroin molecules. It was found that the anticoagulant activity of S-silk scaffolds was significantly enhanced compared with silk fibroin nanofibrous scaffolds (Silk scaffolds). Vascular cells, including ECs and smooth muscle cells (SMCs), demonstrated strong attachment to S-silk scaffolds and proliferated well with higher expression of some phenotype-related marker genes and proteins. Overall, the data in this study suggest the suitability of S-silk scaffolds used along with vascular cells for the development of tissue-engineered vascular grafts.
机译:组织工程化的小直径血管移植物的主要缺点之一是无法在管腔表面获得融合的内皮。当暴露于体内血管系统时,松散附着的内皮细胞(EC)容易从血管壁分离。因此,血管移植物腔表面上的任何裸露区域都可能通过血小板沉积和激活而导致血栓形成。如果裸露的区域可以表达抗凝活性,直到完全形成内皮细胞衬里,则可以大大提高成功进行血管重建的机会。在这项研究中,我们制造了硫酸化丝素蛋白纳米纤维支架(S-silk支架),并评估了S-silk支架的体外抗凝活性和细胞相容性,以提高抗血栓形成性,并对其在血管组织工程中的潜在用途获得了一些见识。通过与氯磺酸在吡啶中反应制备硫酸化丝素蛋白,然后通过静电纺丝技术将其显影以形成S-丝支架。 FTIR分析确定了丝素蛋白分子中硫酸盐基团的成功结合。已经发现,与丝素蛋白纳米纤维支架(丝绸支架)相比,S-丝绸支架的抗凝活性显着增强。包括EC和平滑肌细胞(SMC)在内的血管细胞表现出对S丝支架的牢固附着,并且随着某些表型相关标记基因和蛋白质的高表达而增殖良好。总体而言,这项研究中的数据表明,与血管细胞一起使用的S丝质支架适用于组织工程化的血管移植物的发展。

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