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Nanocomplex Based on Biocompatible Phospholipids and Albumin for Long-Circulation Applications

机译:基于生物相容性磷脂和白蛋白的纳米复合物用于长循环应用

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Achieving long circulating delivery of nano- particles (NPs) is important for efficient drug therapy, but it is difficult due largely to proteins adsorption (opsonization) or/ and nonsufficient stability of NPs. In this present work, we aimed to address the above issues by constructing a phospholipid and BSA-based nanocomplex system, namely BSA-phospholipid NPs (BSA-PL-NPs). Combining sodium dodecyl sulfate-polyacrylamide gel electrophoresis, X-ray photoelectron spectroscopy and proteins adsorption property, we confirmed that some BSA molecules were fixed on the inner surface of BSA-PL-NPs via hydrophobic interactions and the others were located in the core area. This special configuration allowed BSA-PL-NPs to not only maintain the antiadsorption and low phagocytosis properties but also have the slow zero-order drug release and the enhanced nanostructure stability. Interestingly, we found that BSA-PL-NPs had no cytotoxicity to mouse L929 fibroblasts but could stimulate the cells' growth instead. In conclusion, BSA-PL-NPs have a great potential to be developed as a long-circulation drug delivery system, and the ready availability, biocompatibility and nontoxicity of phospholipids and albumin give this system great promise for practical use.
机译:实现纳米颗粒(NPs)的长循环传递对于有效的药物治疗很重要,但是由于蛋白质的吸附(调理作用)或/和NPs的稳定性不足,很难做到这一点。在本工作中,我们旨在通过构建磷脂和基于BSA的纳米复合物系统(即BSA-磷脂NP(BSA-PL-NP))来解决上述问题。结合十二烷基硫酸钠-聚丙烯酰胺凝胶电泳,X射线光电子能谱和蛋白质吸附性能,我们确认了一些BSA分子通过疏水相互作用固定在BSA-PL-NPs的内表面上,而另一些位于核心区域。这种特殊的配置使BSA-PL-NPs不仅保持抗吸附和低吞噬性能,而且具有缓慢的零级药物释放和增强的纳米结构稳定性。有趣的是,我们发现BSA-PL-NP对小鼠L929成纤维细胞没有细胞毒性,但可以刺激细胞生长。总之,BSA-PL-NP具有开发作为长循环药物输送系统的巨大潜力,磷脂和白蛋白的现成可用性,生物相容性和无毒性为该系统提供了广阔的应用前景。

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