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PLGA微球复合明胶组织工程支架缓释蛋白药物的研究 被引量:1

Encapsulation of Proteins in PLGA Microsphere-gelatin Composite Scaffold
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摘要 目的:研究PLGA微球复合明胶支架对蛋白药物的释放影响。方法:将模型蛋白BSA通过复乳法制备成缓释PLGA微球,然后将微球埋置于明胶支架中,形成担载蛋白的PLGA微球复合明胶组织工程支架。考察复合支架体外蛋白释放行为,并用Micro BCA法定量测定释放的BSA量,采用β-半乳糖苷酶催化ONPG的方法检测制备前后蛋白的活性,并与不含PLGA微球直接担载蛋白的支架做对照。结果:PLGA微球复合支架蛋白的包封率能达到73.2%,其中第一天释放20%,对蛋白活性的保持达到70%以上。结论:微球复合明胶支架可以改善一般组织工程支架蛋白药物的突释,提高蛋白药物在制剂,贮存,释放过程中的稳定性。 Objective: To investigate the effect of PLGAmicrospheres composite scaffold on the releasing behavior of protein drug. Methods: BSA was encapsulated into PLGA microspheres by W/O/W emulsion methods, then embedding the microspheres into gelatin to form 3-D composite scaffolds. The release behavior of the composite scaffold in vitro was detected by MicroBCA method and the bioactivity of β-galactosidase (β-gal) was determined by ONPG method. The results were compared with the composite scaffolds without microspheres. Results: Drug loading for the experiment group reached 73.2%, with first day release amount is 20%, the bioactivity of β-gal preserved more than 70 %. Conclusion: Microspheres composite scaffold can improve release behavior of protein drug in tissue engineering, increase drug loading and drug stability during preparation, storation and release process.
作者 刘一浓 秦明杰 卢映蓉 牟颖 张忠恒 吴飞
机构地区 上海交通大学药学院
出处 《现代生物医学进展》 CAS 2013年第33期6463-6465,6444,共4页 Progress in Modern Biomedicine
基金 国家自然科学基金项目(81102406)
关键词 复合明胶支架 PLGA微球 组织工程 Composite gelatin scaffold Poly (lactic-co-glycolic acid )microspheres Tissue Engineering
分类号 R318.08 [医药卫生—生物医学工程] R918 [医药卫生—药学]
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参考文献19

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同被引文献15

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现代生物医学进展
2013年 第33期

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