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首页> 外文期刊>Carbohydrate Polymers: Scientific and Technological Aspects of Industrially Important Polysaccharides >Brij-grafted-chitosan copolymers with function of P-glycoprotein modulation: Synthesis, characterization and in vitro investigations
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Brij-grafted-chitosan copolymers with function of P-glycoprotein modulation: Synthesis, characterization and in vitro investigations

机译:具有p-糖蛋白调节功能的Brij-接枝 - 壳聚糖共聚物:合成,表征和体外研究

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摘要

Chitosan (CS), a nature-derived polysaccharide, is a promising nano-carrier material with good biocompatibility and biodegradability. However, the biomedical applications of CS are hindered because of its poor aqueous solubility. To circumvent this drawback, a series of Brij-grafted-chitosan copolymers (BCs) with various grafting degree of Brij-S20 were first developed and reported. The results indicated that the water solubility of BCs (from 9.13 to 9.54 mg/mL) were much higher than that of CS (0.32 mg/mL), due to the broken intra-and/or intermolecular hydrogen bonds and the decreased initial crystallinity in BCs. The amphiphilic structure of BCs presented lower critical micelle concentration (0.116-0.376 mg/mL) thus facilitating its self-aggregation into micelles for drug encapsulation. Moreover, BCs markedly enhanced the intracellular uptake of rhodamine-123 in MDCK-MDR1 cells. This inhibition on Pgp-mediated efflux was also confirmed by confocal microscopy. In conclusion, BCs could be further developed as polymeric nano-carriers for those drugs with Pgp-mediated efflux.
机译:壳聚糖(CS)是一种自然衍生的多糖,是具有良好的生物相容性和生物降解性的有前途的纳米载体材料。然而,由于其贫化性差,Cs的生物医学应用被阻碍。为了规避这一缺点,首先发育并报告了一系列具有各种嫁接程度的Brij-覆盆子共聚物(BCS)。结果表明,由于破裂的内外 - 和/或分子间氢键和初始结晶度降低,BCs(从9.13至9.54mg / ml)的水溶性远高于Cs(0.32mg / ml)的水溶性,并且初始结晶度降低BCS。 BCS的两亲结构呈现较低的临界胶束浓度(0.116-0.376mg / ml),从而促进其自聚集成用于药物包封的胶束。此外,BCS显着增强了MDCK-MDR1细胞中罗丹明-123的细胞内摄取。通过共聚焦显微镜也证实了对PGP介导的Efflux的这种抑制。总之,BCS可以进一步开发为具有PGP介导的流出的那些药物的聚合物纳米载体。

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