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首页> 外文期刊>Chinese Journal of Chemical Engineering >In vitro Evaluation of Lysozyme-loaded Microspheres in Thermosen-sitive Methylcellulose-based Hydrogel
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In vitro Evaluation of Lysozyme-loaded Microspheres in Thermosen-sitive Methylcellulose-based Hydrogel

机译:热敏性甲基纤维素基水凝胶中溶菌酶微球的体外评价

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摘要

Long-term injectable microspheres have some inherent disadvantages such as migration of micro-spheres from the original site and the burst effect. In order to avoid these problems, microsphere-loaded thermosen-sitive hydrogel system was designed and expected to achieve a zero-order release of biomolecular drugs in relative high initial drug loadings. Lysozyme, an antibacterial protein usually used to reduce prosthetic valve endocarditis, was selected as the model drug. Poly (DL-lactide-co-glycolide) (PLGA) microspheres, prepared by solvent evaporation method, were employed to encapsulate lysozyme and dispersed into thermosensitive pre-gel solution containing methylcellulose (MC), polyethylene glycol (PEG), sodium citrate (SC), and sodium alginate (SA). The mixture could act as a drug reservoir by performing sol-gel transition rapidly if the temperature was raised from room temperature to 37℃. The in vitro release results showed that the burst effect was avoided due to strengthening of diffusion resistance in the gel. The formulation was able to deliver lysozyme for over 30 days in a nearly zero-order release profile with a rate of 32.8μg·d~(-1) which exhibits its remarkable potential for effective application in long-term drug delivery.
机译:长期可注射的微球具有一些固有的缺点,例如微球从原始部位迁移和爆发效应。为了避免这些问题,设计了微球载热敏水凝胶系统,并有望在相对较高的初始载药量下实现生物分子药物的零级释放。溶菌酶是一种通常用于减轻人工瓣膜心内膜炎的抗菌蛋白,被选作模型药物。采用溶剂蒸发法制备的聚DL-丙交酯-乙交酯共聚物(PLGA)微球包封溶菌酶,并分散在含有甲基纤维素(MC),聚乙二醇(PEG),柠檬酸钠(SC)的热敏预凝胶溶液中)和海藻酸钠(SA)。如果将温度从室温升高到37℃,该混合物可通过快速进行溶胶-凝胶转变而充当药物储存库。体外释放结果表明,由于增强了凝胶中的扩散阻力,避免了爆发效应。该制剂能够以接近零级的释放曲线递送溶菌酶超过30天,释放率为32.8μg·d〜(-1),显示了其在长期药物递送中的有效应用的巨大潜力。

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