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用于 BSA 包封和软组织工程的基于共价多糖的海藻酸盐/壳聚糖水凝胶嵌入海藻酸盐微球。

Covalently polysaccharide-based alginate/chitosan hydrogel embedded alginate microspheres for BSA encapsulation and soft tissue engineering.

机构信息

School of Materials Science and Engineering, Nanjing University of Science and Technology, Nanjing 210094, China.

School of Materials Science and Engineering, Nanjing University of Science and Technology, Nanjing 210094, China.

出版信息

Int J Biol Macromol. 2019 Apr 15;127:340-348. doi: 10.1016/j.ijbiomac.2019.01.065. Epub 2019 Jan 15.

Abstract

Hydrogels based scaffolds are very promising materials for a wide range of medical applications including tissue engineering and drug delivery. This study reports a covalently cross-linked composite hydrogel embedded with microspheres basing natural polysaccharides as a protein delivery system for soft tissue engineering. This biodegradable composite hydrogel derived from water-soluble chitosan and alginate derivatives upon mixing, without addition of chemical cross-linking agents. The gelation is attributed to the Schiff-base reaction between amino and aldehyde groups of N-succinyl chitosan (N-Chi) and oxidized alginate (OAlg), respectively. Meanwhile, gel-like microspheres were prepared with a diameter of 2-10 μm by conjugating sodium alginate with Ca in an aqueous emulsion via the emulsion cross-linking technique. Bull Serum Albumin (BSA) was encapsulated into alginate gel microspheres and subsequently incorporated into OAlg/N-Chi hydrogels to produce a composite scaffold. In the current work, gelation rate, morphology, mechanical properties, swelling ratio, in vitro degradation and BSA release of the composite scaffolds were examined. The results show that mechanical and stable properties of gel scaffolds can be significantly improved by embedding alginate microspheres. The alginate microspheres can serve as a filler to toughen the soft OAlg/N-Chi hydrogels. Compressive modulus of composite gel scaffolds containing 0.5 mL volume of microspheres was 57.3 KPa, which was higher than the control hydrogel without microspheres. Moreover, the controlled release of BSA encapsulated within this composite hydrogels showed significantly lower rate when compared with control hydrogel or microspheres alone. These characteristics provide a potential opportunity to use this injectable composite gel scaffold in protein delivery and soft tissue engineering applications.

摘要

基于水凝胶的支架是非常有前途的材料,可用于广泛的医学应用,包括组织工程和药物输送。本研究报告了一种共价交联的复合水凝胶,其中嵌入了基于天然多糖的微球,作为用于软组织工程的蛋白质输送系统。这种可生物降解的复合水凝胶是由水溶性壳聚糖和藻酸盐衍生物混合而成的,无需添加化学交联剂。凝胶化归因于 N-琥珀酰壳聚糖(N-Chi)和氧化藻酸盐(OAlg)中的氨基和醛基之间的席夫碱反应。同时,通过在水乳液中使藻酸钠与 Ca 偶联,通过乳液交联技术制备直径为 2-10 μm 的凝胶状微球。牛血清白蛋白(BSA)被包封在藻酸盐凝胶微球中,并随后掺入 OAlg/N-Chi 水凝胶中以产生复合支架。在目前的工作中,研究了复合支架的凝胶速率、形态、机械性能、溶胀比、体外降解和 BSA 释放。结果表明,通过嵌入藻酸盐微球可以显著提高凝胶支架的机械和稳定性能。藻酸盐微球可以作为填充剂来增韧柔软的 OAlg/N-Chi 水凝胶。含有 0.5 mL 体积微球的复合凝胶支架的压缩模量为 57.3 KPa,高于没有微球的对照水凝胶。此外,与对照水凝胶或单独的微球相比,包封在这种复合水凝胶中的 BSA 的控释释放率明显较低。这些特性为在蛋白质输送和软组织工程应用中使用这种可注射复合凝胶支架提供了潜在的机会。

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