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Nanoparticles as potential oral delivery systems of proteins and vaccines: A mechanistic approach

机译:纳米粒子作为蛋白质和疫苗的潜在口服递送系统:一种机械方法

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Peptides and proteins remain poorly bioavailable upon oral administration. One of the most promising strategies to improve their oral delivery relies on their association with colloidal carriers, e.g. polymeric nanoparticles, stable in gastrointestinal tract, protective for encapsulated substances and able to modulate physicochemical characteristics, drug release and biological behavior. The mechanisms of transport of these nanoparticles across intestinal mucosa are reviewed. In particular, the influence of size and surface properties on their non-specific uptake or their targeted uptake by enterocytes and/or M cells is discussed. Enhancement of their uptake by appropriate cells, i.e. M cells by (i) modeling surface properties to optimize access to and transport by M cells (ii) identifying surface markers specific to human M cell allowing targeting to M cells and nanoparticles transcytosis is illustrated. Encouraging results upon in vivo testing are reported but low bioavailability and lack of control on absorbed dose slow down products development. Vaccines are certainly the most promising applications for orally delivered nanoparticles. (c) 2006 Elsevier B.V. All rights reserved.
机译:口服时肽和蛋白质的生物利用度仍然很差。改善其口服递送的最有希望的策略之一是依赖于它们与胶体载体的结合,例如胶体载体。高分子纳米颗粒,在胃肠道中稳定,对封装的物质具有保护作用,并能够调节理化特性,药物释放和生物学行为。综述了这些纳米颗粒跨肠粘膜的转运机制。特别地,讨论了大小和表面性质对其非特异性摄取或肠细胞和/或M细胞的靶向摄取的影响。通过(i)模拟表面性质以优化对M细胞的访问和转运(ii)鉴定对人M细胞特异的表面标记,从而靶向于M细胞和纳米颗粒转胞吞作用,增强了它们对适当细胞即M细胞的摄取的增强。据报导了体内测试的令人鼓舞的结果,但是生物利用度低和对吸收剂量的控制不足会减慢产品的发展。毫无疑问,疫苗是口服纳米颗粒的最有前途的应用。 (c)2006 Elsevier B.V.保留所有权利。

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