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首页> 外文期刊>Biomacromolecules >Analysis of Immediate Stress Mechanisms upon Injection of Polymeric Micelles and Related Colloidal Drug Carriers: Implications on Drug Targeting
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Analysis of Immediate Stress Mechanisms upon Injection of Polymeric Micelles and Related Colloidal Drug Carriers: Implications on Drug Targeting

机译:注射聚合物胶束和相关胶体药物载体的即时应激机制分析:对靶向药物的影响

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摘要

Polymeric micelles are ideal carriers for solubilization and targeting applications using hydrophobic drugs. Stability of colloidal aggregates upon injection into the bloodstream is mandatory to maintain the drugs' targeting potential and to influence pharmacokinetics. In this review we analyzed and discussed the most relevant stress mechanisms that polymeric midelles and related colloidal carriers encounter upon injection, including (l) dilution, (2) interactions with blood components, and (3) immunological responses of the body. In detail we analyzed the opsonin-dysopsonin hypothesis that points at a connection between a particles' protein-corona and its tissue accumulation by the enhanced permeability and retention (EPR) effect. In the established theory, size is seen as a necessary condition to reach nanoparticle accumulation in disease modified tissue. There is, however, mounting evidence of other sufficient conditions (e.g., particle charge, receptor recognition of proteins adsorbed onto particle surfaces) triggering nanoparticle extravasation by active mechanisms. In conclusion, the analyzed stressmechanisms are directly responsible for in vivo success or failure of the site-specific delivery with colloidal carrier systems.
机译:高分子胶束是使用疏水性药物进行增溶和靶向应用的理想载体。胶体聚集体在注入血液后的稳定性对于维持药物的靶向潜力和影响药代动力学是必不可少的。在这篇综述中,我们分析并讨论了聚合物中层和相关胶体载体在注射时遇到的最相关的应激机制,包括(1)稀释,(2)与血液成分的相互作用以及(3)机体的免疫反应。详细地,我们分析了调理素-反调理素的假说,该假说通过增强的渗透性和保留(EPR)效应指出了颗粒的蛋白质电晕与其组织积累之间的联系。在已建立的理论中,大小被视为在疾病改良组织中达到纳米颗粒积累的必要条件。但是,越来越多的证据表明,其他充分条件(例如,粒子电荷,吸附在粒子表面的蛋白质的受体识别)也通过主动机制触发了纳米粒子的外溢。总之,所分析的应力机制直接导致体内通过胶体载体系统进行定点递送的成功或失败。

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