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Exploitation of acoustic cavitation-induced microstreaming to enhance molecular transport

机译:声析气诱导微晶的开发以增强分子运输

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摘要

Ultrasound (US) exposure of soft tissues, such as the skin, has been shown to increase permeability, enhancing the passage of drug molecules via passive processes such as diffusion. However, US regimes have not been exploited to enhance active convective transport of drug molecules from a donor layer, such as a gel, into another medium. A layered tissue-mimicking material (TMM) was used as a model for a drug donor layer and underlying soft tissue to test penetration of agents in response to a range of US parameters. Influence of agent molecular mass (3-2000 kDa), US frequency (0.256/1.1 MHz) and US pressure (0-10 MPa) on transport was characterised. Agents of four different molecular sizes were embedded within the TMM with or without cavitation nuclei (CN) and US applied to achieve inertial cavitation. Post-insonation, samples were analysed to determine the concentration and penetration distance of agent transported. US exposure substantially enhanced transport. At both US frequencies, enhancement of transport was significantly higher (p < 0.05) above the cavitation threshold, and CN reduced the pressure at which cavitation, and therefore transport, was achieved. Acoustic cavitation activity and related phenomena was the predominant transport mechanism, and addition of CN significantly enhanced transport within a range of clinically applicable acoustic pressures.
机译:已经显示超声(美国)诸如皮肤的软组织的暴露,以增加渗透性,通过诸如扩散的被动过程增强药物分子的通过。然而,美国制度尚未被利用以增强从供体层(例如凝胶)的药物分子的活性对流转运到另一个培养基中。层状组织模拟材料(TMM)用作药物供体层和底层软组织的模型,以响应于一系列美国参数测试药剂的渗透。特征表征试剂分子量(3-2000kDa),美国频率(0.256 / 1.1MHz)和美国压力(0-10MPa)的影响。在具有或没有空化核(CN)的TMM内嵌入四种不同分子尺寸的试剂,并且我们施加以达到惯性空化。分析样品以确定转运剂的浓度和渗透距离。美国曝光大幅增强了运输。在我们的两个频率下,高于空化阈值的运输增强显着升高(P <0.05),并且CN降低了逐渐降低了空化,因此运输的压力。声学空化活性和相关现象是主要的传输机制,并且CN的加入显着增强了一系列临床适用的声学压力。

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