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Ligand Distribution and Lipid Phase Behavior in Phospholipid-Coated Microbubbles and Monolayers

机译:磷脂涂覆的微泡和单层中的配体分布和脂质相行使

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摘要

Phospholipid-coated targeted microbubbles are ultrasound contrast agents that can be used for molecular imaging and enhanced drug delivery. However, a better understanding is needed of their targeting capabilities and how they relate to microstructures in the microbubble coating. Here, we investigated the ligand distribution, lipid phase behavior, and their correlation in targeted microbubbles of clinically relevant sizes, coated with a ternary mixture of 1,2-dipalmitoyl-sn-glycero-3-phosphocholine (DPPC) or 1,2-distearoyl-sn-glycero-3phosphocholine ( DSPC), with PEG40-stearate and DSPE-PEG2000. To investigate the effect of lipid handling prior to microbubble production in DSPC-based microbubbles, the components were either dispersed in aqueous medium (direct method) or first dissolved and mixed in an organic solvent (indirect method). To determine the lipid-phase behavior of all components, experiments were conducted on monolayers at the air/water interface. In comparison to pure DSPC and DPPC, the ternary mixtures had an additional transition plateau around 10-12 mN/m. As confirmed by infrared reflection absorption spectroscopy (IRRAS), this plateau was due to a transition in the conformation of the PEGylated components (mushroom to brush). While the condensed phase domains had a different morphology in the ternary DPPC and DSPC monolayers on the Langmuir trough, the domain morphology was similar in the coating of both ternary DPPC and DSPC microbubbles (1.5-8 mu m diameter). The ternary DPPC microbubbles had a homogenous ligand distribution and significantly less liquid condensed (LC) phase area in their coating than the DSPC-based microbubbles. For ternary DSPC microbubbles, the ligand distribution and LC phase area in the coating depended on the lipid handling. The direct method resulted in a heterogeneous ligand distribution, less LC phase area than the indirect method, and the ligand colocalizing with the liquid expanded (LE) phase area. The indirect method resulted in a homogenous ligand distribution with the largest LC phase area. In conclusion, lipid handling prior to microbubble production is of importance for a ternary mixture of DSPC, PEG40-stearate, and DSPE-PEG2000.
机译:磷脂涂覆的靶向微泡是超声造影剂,其可用于分子成像和增强的药物递送。然而,需要更好的理解它们的靶向能力以及它们如何与微泡涂层中的微观结构相关。在这里,我们研究了配体分布,脂质相行为及其在临床相关尺寸的靶向微泡中的相关性,涂有1,2-Dipalmitoyl-sn-甘油-3-普膦啉(DPPC)或1,2-的三元混合物Distearoyl-Sn-甘油-3phospholine(DSPC),具有PEG40-硬脂酸盐和DSPE-PEG2000。为了研究在基于DSPC的微泡的微泡制作之前脂质处理的影响,将组分分散在水性介质(直接方法)中,或者首先溶解并在有机溶剂中混合(间接方法)。为了确定所有组分的脂相行为,在空气/水界面的单层上进行实验。与纯DSPC和DPPC相比,三元混合物具有额外的过渡平台,约为10-12mN / m。如红外反射吸收光谱(ANRAS)所证实,该平台是由于聚乙二醇化成分的构象(蘑菇刷)的转变。虽然凝结的相位域在朗米尔槽上的三元DPPC和DSPC单层中具有不同的形态,但是域形态在三元DPPC和DSPC微泡(直径1.5-8μm)的涂层中相似。三元DPPC微泡具有均匀的配体分布,其涂层中的液体浓缩(LC)相面积较低而不是基于DSPC的微泡。对于三元DSPC微泡,涂层中的配体分布和LC相面积依赖于脂质处理。直接方法导致异质配体分布,比间接方法较少的LC相位面积,与液体膨胀(LE)相面积分解的配体。间接方法导致具有最大LC相位区域的均匀配体分布。总之,微泡生产前的脂质处理对于DSPC,PEG40-硬脂酸酯和DSPE-PEG2000的三元混合物具有重要性。

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