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Microbubble-liposome conjugate: payload evaluation of potential theranostic vehicle.

机译:微泡-脂质体结合物:潜在治疗治疗载体的有效载荷评估。

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摘要

Liposome-microbubble conjugates are considered as better targeted drug delivery vehicles compared to microbubbles alone. The microbubble in the integrated drug delivery system delivers the drug intracellularly on the target, whereas the liposome component allows loading of high drug dose and extravasation through leaky vasculature. In this work, a new high yielding microbubble production method was used to prepare microbubbles for formulation of the liposomeconjugated drug delivery system. In formulation process, the prepared liposome of 200 nm diameter was attached to the microbubble surface using the avidin-biotin interaction. The analysis of the confocal scanning laser microscope images showed that approximately 8 x 108 microbubbles per millilitre (range: 2-7 mm, mean size 5 + 0.5 mm) can be efficiently conjugated to the liposomes. The method of conjugation was found to be effective in attaching liposome to microbubbles.
机译:与单独的微泡相比,脂质体-微泡缀合物被认为是更好的靶向药物递送载体。集成药物输送系统中的微泡可将药物通过细胞内输送到靶标上,而脂质体组分则允许装载高剂量的药物并通过渗漏的脉管系统进行渗出。在这项工作中,一种新的高产微泡生产方法被用来制备微泡,以配制脂质体偶联的药物递送系统。在配制过程中,使用抗生物素蛋白-生物素相互作用将制得的直径200 nm的脂质体附着到微泡表面。共聚焦扫描激光显微镜图像的分析表明,每毫升约8 x 108个微气泡(范围:2-7毫米,平均大小5 + 0.5毫米)可以有效地与脂质体结合。发现缀合方法可有效地将脂质体附着到微泡上。

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