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Self-cross-linking biopolymers as injectable in situ forming biodegradable scaffolds

硼砂 自愈水凝胶 明胶 肿胀 的 高碘酸钠 葡萄糖醛酸 组织工程 药物输送 材料科学 高碘酸盐 多糖 高分子化学 可生物降解聚合物 化学工程 聚合物 化学 生物降解 生物医学工程 生物高聚物 有机化学 复合材料 纳米技术 原材料 工程类 医学
作者
Biji Balakrishnan,A. Jayakrishnan
出处
期刊:Biomaterials [Elsevier BV]
卷期号:26 (18): 3941-3951 被引量:674
标识
DOI:10.1016/j.biomaterials.2004.10.005
摘要

The injectable polymer scaffolds which are biocompatible and biodegradable are important biomaterials for tissue engineering and drug delivery. Hydrogels derived from natural proteins and polysaccharides are ideal scaffolds for tissue engineering since they resemble the extracellular matrices of the tissue comprised of various amino acids and sugar-based macromolecules. Here, we report a new class of hydrogels derived from oxidized alginate and gelatin. We show that periodate-oxidized sodium alginate having appropriate molecular weight and degree of oxidation rapidly cross-links proteins such as gelatin in the presence of small concentrations of sodium tetraborate (borax) to give injectable systems for tissue engineering, drug delivery and other medical applications. The rapid gelation in the presence of borax is attributed to the slightly alkaline pH of the medium as well as the ability of borax to complex with hydroxyl groups of polysaccharides. The effect of degree of oxidation and concentration of alginate dialdehyde, gelatin and borax on the speed of gelation was examined. As a general rule, the gelling time decreased with increase in concentration of oxidized alginate, gelatin and borax and increase in the degree of oxidation of alginate. Cross-linking parameters of the gel matrix were studied by swelling measurements and trinitrobenzene sulphonic acid (TNBS) assay. In general, the degree of cross-linking was found to increase with increase in the degree of oxidation of alginate, whereas the swelling ratio and the degree of swelling decreased. The gel was found to be biocompatible and biodegradable. The potential of the system as an injectable drug delivery vehicle and as a tissue-engineering scaffold is demonstrated by using primaquine as a model drug and by encapsulation of hepatocytes inside the gel matrix, respectively.
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