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Long-circulating and target-specific nanoparticles: theory to practice.

机译:长循环和特定于目标的纳米颗粒:理论实践。

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The rapid recognition of intravenously injected colloidal carriers, such as liposomes and polymeric nanospheres from the blood by Kupffer cells, has initiated a surge of development for "Kupffer cell-evading" or long-circulating particles. Such carriers have applications in vascular drug delivery and release, site-specific targeting (passive as well as active targeting), as well as transfusion medicine. In this article we have critically reviewed and assessed the rational approaches in the design as well as the biological performance of such constructs. For engineering and design of long-circulating carriers, we have taken a lead from nature. Here, we have explored the surface mechanisms, which affords red blood cells long-circulatory lives and the ability of specific microorganisms to evade macrophage recognition. Our analysis is then centered where such strategies have been translated and fabricated to design a wide range of particulate carriers (e.g., nanospheres, liposomes, micelles, oil-in-water emulsions) with prolonged circulation and/or target specificity. With regard to the targeting issues, attention is particularly focused on the importance of physiological barriers and disease states.
机译:库普弗细胞对血液中静脉注射的胶体载体(例如脂质体和聚合物纳米球)的快速识别,引发了“逃避库普弗”或长循环颗粒的发展。这样的载体在血管药物递送和释放,位点特异性靶向(被动和主动靶向)以及输血药物中具有应用。在本文中,我们严格审查和评估了设计中的合理方法以及此类构建体的生物学性能。对于长循环运输船的工程和设计,我们从自然界中取得了领先。在这里,我们探索了表面机制,该机制赋予红细胞长循环寿命以及特定微生物规避巨噬细胞识别的能力。然后我们的分析集中在已翻译和制造此类策略的地方,以设计具有延长的循环和/或目标特异性的各种颗粒载体(例如纳米球,脂质体,胶束,水包油乳剂)。关于目标问题,注意力特别集中在生理障碍和疾病状态的重要性上。

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