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首页> 外文期刊>Journal of biomedical materials research, Part A >In vitro characterization of hepatocyte growth factor release from PHBV/PLGA microsphere scaffold.
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In vitro characterization of hepatocyte growth factor release from PHBV/PLGA microsphere scaffold.

机译:从PHBV / PLGA微球支架释放肝细胞生长因子的体外表征。

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摘要

Polymer scaffolds which can support cells to grow as well as deliver growth factors to the cells simultaneously have great potential for the successful regeneration of failed tissues. As popularly used vehicles to deliver anti-cancer drugs and growth factors, microspheres also show many advantages as substrates to guide the growth of cells. Therefore, we aimed to examine the feasibility of using microspheres as ideal scaffolds for liver tissue engineering. To determine the capabilities of previously used microsphere scaffold to deliver growth factors simultaneously, this work investigated a long-term (about three months) release of bovine serum albumin (BSA) from microsphere scaffolds fabricated by using two different polymers, poly(3-hydroxybutyrate-co-3-hydroxyvalerate) (PHBV, 8% PHV), poly(lactide-co-glycolide) acid (PLGA, 5050) and a blend of PLGA and PHBV. BSA served as a model for hepatocyte growth factor (HGF) since both proteins have similar molecular weights and hydrophilicity. Furthermore, HGF was encapsulated into the PLGA/PHBV composite microsphere with a core-shell structure, and sustained delivery of HGF with maintained bioactivity was achieved for at least 40 days. The moderate degradation rate (about 55% loss of the initial mass) and well-preserved structure after three months of incubation indicated that the PLGA/PHBV composite microspheres would therefore be more suitable than the pure PHBV or PLGA microspheres as a scaffold for engineering liver tissue.
机译:可以支撑细胞生长并同时向细胞传递生长因子的聚合物支架具有成功再生受损组织的巨大潜力。作为普遍使用的传递抗癌药物和生长因子的载体,微球作为引导细胞生长的底物也显示出许多优势。因此,我们旨在研究使用微球作为肝组织工程理想支架的可行性。为了确定以前使用的微球支架同时传递生长因子的能力,这项工作研究了使用两种不同的聚合物聚(3-羟基丁酸酯)从微球支架中长期释放牛血清白蛋白(BSA)的时间(约三个月)。 -羟基-3-羟基戊酸酯(PHBV,8%PHV),聚(丙交酯-乙交酯-乙交酯)酸(PLGA,5050)和PLGA和PHBV的混合物。 BSA充当肝细胞生长因子(HGF)的模型,因为这两种蛋白具有相似的分子量和亲水性。此外,将HGF封装到具有核-壳结构的PLGA / PHBV复合微球中,并保持生物活性的HGF持续递送至少40天。孵育三个月后,中等的降解速率(约占初始质量的55%损失)和保存完好的结构表明,PLGA / PHBV复合微球比纯PHBV或PLGA微球更适合作为工程肝的支架组织。

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