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Controlled heparin conjugation on electrospun poly(-caprolactone)/gelatin fibers for morphology-dependent protein delivery and enhanced cellular affinity

机译:静电纺丝聚己内酯/明胶纤维上的肝素结合控制,可用于形态依赖的蛋白传递并增强细胞亲和力

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Electrospun fibrous scaffolds have now been shown to possess great potential for tissue engineering applications, owing to their unique mimicry of natural extracellular matrix structure. In this study, poly(-caprolactone) and gelatin were electrospun to fabricate tissue-engineered scaffolds with three different fiber morphologies (1.0 μm, 3.0 μm and co-electrospun containing both 1.0 and 3.0 μm diameter fibers). Subsequently, these scaffolds were conjugated with heparin to immobilize a bioactive molecule by electrostatic interactions. This study determined the quantity of heparin conjugation on the scaffolds and that the crosslinking time and the fiber morphologies govern the extent of heparin conjugation on the fibers. In order to evaluate the release capacity of the heparin-conjugated scaffolds, lysozyme was used as a model protein for conjugation. The heparin-conjugated scaffolds provided high loading efficiency and cumulative release of lysozyme with a relatively linear relationship. In addition, the release kinetics was significantly dependent on heparin conjugation and fiber morphology. This fundamental investigation into how fiber morphology and crosslinking protocols can affect the heparin binding ability of electrospun fibers is crucial for predicting the delivery of many different types of bioactive molecules from an electrospun scaffold for tissue engineering applications.
机译:由于其对天然细胞外基质结构的独特模仿,现已证明电纺纤维支架具有巨大的组织工程应用潜力。在这项研究中,对聚己内酯和明胶进行静电纺丝,以制造具有三种不同纤维形态(1.0μm,3.0μm和包含1.0和3.0μm直径纤维的共电纺丝)的组织工程支架。随后,将这些支架与肝素偶联以通过静电相互作用固定生物活性分子。这项研究确定了肝素在支架上的结合量,并且交联时间和纤维形态决定了肝素在纤维上的结合程度。为了评估结合肝素的支架的释放能力,溶菌酶被用作结合的模型蛋白。肝素结合的支架提供了较高的装载效率和溶菌酶的累积释放,具有相对线性的关系。另外,释放动力学显着取决于肝素结合和纤维形态。对纤维形态和交联规程如何影响静电纺丝纤维的肝素结合能力的基础研究对于预测用于组织工程应用的静电纺丝支架中许多不同类型的生物活性分子的递送至关重要。

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