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Enhanced oral delivery of paclitaxel using acetylcysteine functionalized chitosan-vitamin E succinate nanomicelles based on a mucus bioadhesion and penetration mechanism

机译:基于黏液生物粘附和渗透机制,使用乙酰半胱氨酸官能化的壳聚糖-维生素E琥珀酸酯纳米胶束增强紫杉醇的口服给药

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摘要

In addition to being a physiological protective barrier, the gastrointestinal mucosal membrane is also a primary obstacle that hinders the oral absorption of many therapeutic compounds, especially drugs with a poor permeability. In order to resolve this impasse, we have designed multifunctional nanomicelles based on the acetylcysteine functionalized chitosan-vitamin E succinate copolymer (CS-VES-NAC, CVN), which exhibit marked bioadhesion, possess the ability to penetrate mucus, and enhance the oral absorption of a hydrophobic drug with a poor penetrative profile, paclitaxel. The intestinal absorption (Ka = 0.38 ± 0.04 min-1, Papp = 0.059 cm·min-1) of CVN nanomicelles was greatly improved (4.5-fold) in comparison with paclitaxel solution, and CLSM (confocal laser scanning microscope) pictures also showed not only enhanced adhesion to the intestinal surface but improved accumulation within intestinal villi. The in vivo pharmacokinetics indicated that the AUC0-t (586.37 ng/mL·h) of CVN nanomicelles was markedly enhanced compared with PTX solution. In summary, the novel multifunctional CVN nanomicelles appear to be a promising nanocarrier for insoluble and poorly permeable drugs due to their high bioadhesion and permeation-enhancing capability.
机译:胃肠道粘膜除了是一种生理保护性屏障外,也是阻碍许多治疗性化合物,尤其是渗透性较差的药物的口服吸收的主要障碍。为了解决这一难题,我们基于乙酰半胱氨酸官能化的壳聚糖-维生素E琥珀酸酯共聚物(CS-VES-NAC,CVN)设计了多功能纳米胶束,该胶束具有显着的生物粘附性,具有穿透粘液的能力,并可以增强口腔吸收紫杉醇是一种渗透性较差的疏水性药物。与紫杉醇溶液相比,CVN纳米胶束的肠道吸收(Ka = 0.38±0.04 min-1,Papp = 0.059 cm·min-1)大大提高(4.5倍),CLSM(共聚焦激光扫描显微镜)照片也显示不仅增强了对肠道表面的附着力,而且改善了肠绒毛内的积累。体内药代动力学表明,与PTX溶液相比,CVN纳米胶束的AUC0-t(586.37 ng / mL·h)显着增强。综上所述,新型多功能CVN纳米胶束由于其高的生物粘附性和增强的渗透能力,似乎是用于不溶性和低渗透性药物的有前途的纳米载体。

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