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空化增强型药物外渗

Cavitation-enhanced extravasation for drug delivery.

机构信息

Institute of Biomedical Engineering, Department of Engineering Science, University of Oxford, Headington, Oxford, UK.

出版信息

Ultrasound Med Biol. 2011 Nov;37(11):1838-52. doi: 10.1016/j.ultrasmedbio.2011.08.004. Epub 2011 Oct 2.

Abstract

A flow-through tissue-mimicking phantom composed of a biocompatible hydro-gel with embedded tumour cells was used to assess and optimize the role of ultrasound-induced cavitation on the extravasation of a macromolecular compound from a channel mimicking vessel in the gel, namely a non-replicating luciferase-expressing adenovirus (Ad-Luc). Using a 500 KHz therapeutic ultrasound transducer confocally aligned with a focussed passive cavitation detector, different exposure conditions and burst mode timings were selected by performing time and frequency domain analysis of passively recorded acoustic emissions, in the absence and in the presence of ultrasound contrast agents acting as cavitation nuclei. In the presence of Sonovue, maximum ultraharmonic emissions were detected for peak rarefactional pressures of 360 kPa, and maximum broadband emissions occurred at 1250 kPa. The energy of the recorded acoustic emissions was used to optimise the pulse repetition frequency and duty cycle in order to maximize either ultraharmonic or broadband emissions while keeping the acoustic energy delivered to the focus constant. Cell viability measurements indicated that none of the insonation conditions investigated induces cell death in the absence of a therapeutic agent (i.e. virus). Phase contrast images of the tissue-mimicking phantom showed that short range vessel disruption can occur when ultra-harmonic emissions (nf0/2) are maximised whereas formation of a micro-channel perpendicular to the flow can be obtained in the presence of broadband acoustic emissions. Following Ad-Luc delivery, luciferase expression measurements showed that a 60-fold increase in its bioavailability can be achieved when broadband noise emissions are present during insonation, even for modest contrast agent concentrations. The findings of the present study suggest that drug delivery systems based on acoustic cavitation may help enhance the extravasation of anticancer agents, thus increasing their penetration distance to hypoxic regions and poorly vascularised tumour regions.

摘要

一种由可生物相容的水凝胶组成的流动式组织模拟体,其中嵌入了肿瘤细胞,用于评估和优化超声诱导空化在大分子化合物从凝胶中模拟血管的通道中渗出的作用,即非复制的表达荧光素的腺病毒(Ad-Luc)。使用 500 kHz 治疗超声换能器与聚焦被动空化探测器共焦排列,通过对被动记录的声发射进行时频域分析,选择不同的暴露条件和脉冲模式定时,在不存在和存在作为空化核的超声造影剂的情况下。在 SonoVue 的存在下,在 360 kPa 的峰值稀疏压力下检测到最大超谐波发射,而在 1250 kPa 时发生最大宽带发射。记录的声发射能量用于优化脉冲重复频率和占空比,以在保持焦点处传递的声能恒定的情况下最大化超谐波或宽带发射。细胞活力测量表明,在没有治疗剂(即病毒)的情况下,研究中调查的任何照射条件都不会导致细胞死亡。组织模拟体的相衬图像表明,当最大化超谐波发射(nf0/2)时,可以发生短程血管破坏,而在存在宽带声发射的情况下,可以形成垂直于流动的微通道。在 Ad-Luc 给药后,荧光素酶表达测量表明,当存在宽带噪声发射时,即使对比剂浓度适中,其生物利用度也可以增加 60 倍。本研究的结果表明,基于声空化的药物输送系统可能有助于增强抗癌剂的渗出,从而增加其穿透缺氧区域和血管化不良肿瘤区域的距离。

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