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本文引用的文献

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Influence of lipid shell physicochemical properties on ultrasound-induced microbubble destruction.脂质壳物理化学性质对超声诱导微泡破坏的影响。
IEEE Trans Ultrason Ferroelectr Freq Control. 2005 Nov;52(11):1992-2002. doi: 10.1109/tuffc.2005.1561668.
2
Targeting vascular endothelium with avidin microbubbles.用抗生物素蛋白微泡靶向血管内皮。
Ultrasound Med Biol. 2005 Sep;31(9):1279-83. doi: 10.1016/j.ultrasmedbio.2005.06.001.
3
Targeted ultrasound contrast agents: in vitro assessment of endothelial dysfunction and multi-targeting to ICAM-1 and sialyl Lewisx.靶向超声造影剂:内皮功能障碍及对细胞间黏附分子-1和唾液酸化路易斯X多靶点的体外评估
Biotechnol Bioeng. 2005 Dec 20;92(6):780-8. doi: 10.1002/bit.20625.
4
Accelerated blood clearance of PEGylated liposomes following preceding liposome injection: effects of lipid dose and PEG surface-density and chain length of the first-dose liposomes.先前注射脂质体后聚乙二醇化脂质体的血液清除加速:首剂脂质体的脂质剂量、聚乙二醇表面密度和链长的影响
J Control Release. 2005 Jul 20;105(3):305-17. doi: 10.1016/j.jconrel.2005.04.003.
5
Acoustic radiation force enhances targeted delivery of ultrasound contrast microbubbles: in vitro verification.声辐射力增强超声造影微泡的靶向递送:体外验证
IEEE Trans Ultrason Ferroelectr Freq Control. 2005 Mar;52(3):421-33. doi: 10.1109/tuffc.2005.1417264.
6
Ligand-carrying gas-filled microbubbles: ultrasound contrast agents for targeted molecular imaging.携带配体的充气微泡:用于靶向分子成像的超声造影剂。
Bioconjug Chem. 2005 Jan-Feb;16(1):9-17. doi: 10.1021/bc049898y.
7
Radiation-force assisted targeting facilitates ultrasonic molecular imaging.辐射力辅助靶向有助于超声分子成像。
Mol Imaging. 2004 Jul;3(3):135-48. doi: 10.1162/15353500200404115.
8
A method for radiation-force localized drug delivery using gas-filled lipospheres.一种使用充气脂质球进行辐射力局部药物递送的方法。
IEEE Trans Ultrason Ferroelectr Freq Control. 2004 Jul;51(7):822-31. doi: 10.1109/tuffc.2004.1320741.
9
Surface phase behavior and microstructure of lipid/PEG-emulsifier monolayer-coated microbubbles.脂质/聚乙二醇-乳化剂单层包覆微泡的表面相行为和微观结构
Colloids Surf B Biointerfaces. 2004 Jun 1;35(3-4):209-23. doi: 10.1016/j.colsurfb.2004.03.007.
10
Binding and detachment dynamics of microbubbles targeted to P-selectin under controlled shear flow.在可控剪切流条件下靶向P-选择素的微泡的结合与脱离动力学。
J Control Release. 2004 May 18;96(3):473-82. doi: 10.1016/j.jconrel.2004.03.002.

超声辐射力能够使负载于微泡上的模型药物载体实现靶向沉积。

Ultrasound radiation force enables targeted deposition of model drug carriers loaded on microbubbles.

作者信息

Lum Aaron F H, Borden Mark A, Dayton Paul A, Kruse Dustin E, Simon Scott I, Ferrara Katherine W

机构信息

University of California: Davis, Department of Biomedical Engineering, 451 East Health Sciences Drive, Davis, CA 95616, USA.

出版信息

J Control Release. 2006 Mar 10;111(1-2):128-34. doi: 10.1016/j.jconrel.2005.11.006. Epub 2005 Dec 27.

DOI:10.1016/j.jconrel.2005.11.006
PMID:16380187
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1526414/
Abstract

A novel drug delivery vehicle that specifically targets using ultrasound radiation force (USRF) and biotin-avidin interactions is presented. Model vehicles consist of avidinated fluorescent nanobeads bound directly to the biotinylated lipid shells of preformed microbubbles. USRF was used to deflect the vehicle from the center of flow to a tube surface in order to facilitate receptor-ligand mediated adhesion. At wall shear stress levels commensurate with venous and arterial flow, USRF was used to direct the vehicles to a biotinylated tube surface. Subsequent high-pressure pulses fragmented the carrier, and molecular interactions induced deposition of the nanobeads on the wall. Targeting of nanobeads to the tube was molecularly specific and dependent on, in order of importance, vehicle concentration, wall shear stress, nanobead size, and insonation time. The observation that portions of the microbubble lipid monolayer shell remain attached to adherent nanobeads is important for future consideration of drug transport mechanisms. This versatile method of delivery is shown to enable targeted deposition of nanoparticles in shear flow and could be modified to carry therapeutic agents for controlled release in targeted delivery applications.

摘要

本文介绍了一种新型药物递送载体,该载体利用超声辐射力(USRF)和生物素-抗生物素蛋白相互作用进行特异性靶向。模型载体由直接结合到预制微泡生物素化脂质壳上的抗生物素蛋白化荧光纳米珠组成。USRF用于将载体从流中心偏转到管壁表面,以促进受体-配体介导的粘附。在与静脉和动脉血流相当的壁面剪应力水平下,USRF用于将载体引导至生物素化的管壁表面。随后的高压脉冲使载体破碎,分子相互作用导致纳米珠沉积在管壁上。纳米珠靶向管壁具有分子特异性,并且按重要性顺序取决于载体浓度、壁面剪应力、纳米珠大小和声作用时间。微泡脂质单层壳的部分仍附着在粘附的纳米珠上这一观察结果,对于未来药物转运机制的研究具有重要意义。这种通用的递送方法能够在剪切流中实现纳米颗粒的靶向沉积,并且可以进行改进以携带治疗剂,用于靶向递送应用中的控释。