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首页> 外文期刊>Nanoscale >Self-assembly of core-polyethylene glycol-lipid shell (CPLS) nanoparticles and their potential as drug delivery vehicles
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Self-assembly of core-polyethylene glycol-lipid shell (CPLS) nanoparticles and their potential as drug delivery vehicles

机译:自组装的core-polyethylene glycol-lipidshell (cpl)纳米粒子及其潜力药物运载工具

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Herein a new multifunctional formulation, referred to as a core-polyethylene glycol-lipid shell (CPLS) nanoparticle, has been proposed and studied in silico via large scale coarse-grained molecular dynamics simulations. A PEGylated core with surface tethered polyethylene glycol (PEG) chains is used as the starting configuration, where the free ends of the PEG chains are covalently bonded with lipid molecules (lipid heads). A complete lipid bilayer is formed at the surface of the PEGylated particle core upon addition of free lipids, driven by the hydrophobic properties of the lipid tails, leading to the formation of a CPLS nanoparticle. The self-assembly process is found to be sensitive to the grafting density and molecular weight of the tethered PEG chains, as well as the amount of free lipids added. At low grafting densities the assembly of CPLS nanoparticles cannot be accomplished. As demonstrated by simulations, a lipid bud/vesicle can be formed on the surface when an excess amount of free lipids is added at high grafting density. Therefore, the CPLS nanoparticles can only be formed under appropriate conditions of both PEG and free lipids. The CPLS nanoparticle has been recognized to be able to store a large quantity of water molecules, particularly with high molecular weight of PEG chains, indicating its capacity for carrying hydrophilic molecules such as therapeutic biomolecules or imaging agents. Under identical size and surface chemistry conditions of a liposome, it has been observed that the CPLS particle can be more efficiently wrapped by the lipid membrane, indicating its potential for a greater efficiency in delivering its hydrophilic cargo. As a proof-of-concept, the experimental realization of CPLS nanoparticles is explicitly demonstrated in this study. To test the capacity of the CPLS to store small molecule cargo a hydrophilic dye was successfully encapsulated in the particles' water soluble layer. The results of this study show the power and potential of simulation-driven approaches for guiding the design of more efficient nanomaterial delivery platforms.
机译:这一个新的多功能配方,被称为作为core-polyethylene glycol-lipid壳(cpl)纳米颗粒,已经提出了通过大规模的粗粒度的在网上学习分子动力学模拟。与表面拴在聚乙二醇(PEG)链作为初始配置,挂钩的自由端链在哪里吗与脂类分子共价键(脂质头)。聚乙二醇粒子表面的核心免费的脂质,由驱动疏水性能的脂质反面,导致产线的形成纳米颗粒。自组装过程是发现敏感的接枝密度和分子系链挂钩的重量,以及大量的免费的脂质补充道。密度cpl纳米粒子的组装不能完成。模拟,就可以形成脂质芽/泡当多余的自由表面脂质添加高接枝密度。cpl纳米粒子只能下形成的适当的条件挂钩和免费的脂质。能够储存大量的水分子,特别是高分子挂钩的连锁店,表明其能力带亲水分子等治疗性生物分子或显像剂。相同的尺寸和表面化学条件脂质体,观察到产线粒子可以更有效地包装脂质膜,说明其潜力更高的效率在交付其亲水性货物。实现产线的纳米颗粒是明确的在这项研究中。cpl的商店货物小分子亲水性染料被成功地封装在粒子的水溶性层。本研究显示的力量和潜力simulation-driven方法指导设计更高效的纳米材料交付平台。

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