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Colloidal Stability of Silk Fibroin Nanoparticles Coated with Cationic Polymer for Effective Drug Delivery

机译:阳离子聚合物包覆丝素蛋白纳米粒的胶体稳定性,可有效递送药物。

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Generally, silk fibroin nanoparticles (SFNPs) are great candidates to deliver drugs or other bioactive substances in vivo. However, their further applications are largely limited by the low colloidal stability of SENPs, as they tend to aggregate in biological media. To address this issue, SFNP composite materials with a core shell structure (CS-SFNPs) were fabricated by coating SFNPs with four different selected cationic polymers, glycol chitosan, N,N,N-trimethyl chitosan, polyethylenimine, and PEGylated polyethylenimine, through electrostatic interaction. According to the DLS and NTA results, compared with the bare SFNPs, the CS-SFNPs showed much higher colloidal stability in biological media. When treated with human cervical carcinoma (HeLa) cells, the CS-SFNPs were efficiently internalized and accumulated in lysosome; and when loaded with an anticancer drug, DOX, the CS-SFNPs also showed higher cytotoxicity against HeLa cells. Our results suggest that the fabricated CS-SFNPs with desirable colloidal stability in biological media have the potential to be employed as drug carriers for the anticancer drug delivery system.
机译:通常,丝素蛋白纳米粒子(SFNP)是在体内递送药物或其他生物活性物质的理想选择。但是,它们的进一步应用在很大程度上受到SENPs胶体稳定性的限制,因为它们倾向于在生物介质中聚集。为了解决这个问题,通过用静电将四种不同的阳离子聚合物(乙二醇壳聚糖,N,N,N-三甲基壳聚糖,聚乙烯亚胺和聚乙二醇化聚乙烯亚胺)涂覆在SFNP上,从而制造出具有核壳结构(CS-SFNPs)的SFNP复合材料。相互作用。根据DLS和NTA结果,与裸SFNP相比,CS-SFNP在生物介质中显示出更高的胶体稳定性。当用人宫颈癌(HeLa)细胞治疗时,CS-SFNPs被有效地内化并积累在溶酶体中。当加入抗癌药物DOX时,CS-SFNPs也显示出对HeLa细胞更高的细胞毒性。我们的结果表明,在生物介质中具有理想的胶体稳定性的人造CS-SFNP具有潜力用作抗癌药物递送系统的药物载体。

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