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使用临床超声系统进行超声介导的药物递送:评估

Ultrasound-Mediated Drug Delivery With a Clinical Ultrasound System: Evaluation.

作者信息

de Maar Josanne S, Rousou Charis, van Elburg Benjamin, Vos Hendrik J, Lajoinie Guillaume P R, Bos Clemens, Moonen Chrit T W, Deckers Roel

机构信息

Imaging and Oncology Division, University Medical Center Utrecht, Utrecht University, Utrecht, Netherlands.

Department of Pharmaceutical Sciences, Utrecht Institute for Pharmaceutical Sciences (UIPS), Utrecht University, Utrecht, Netherlands.

出版信息

Front Pharmacol. 2021 Oct 19;12:768436. doi: 10.3389/fphar.2021.768436. eCollection 2021.

Abstract

Chemotherapy efficacy is often reduced by insufficient drug uptake in tumor cells. The combination of ultrasound and microbubbles (USMB) has been shown to improve drug delivery and to enhance the efficacy of several drugs and , through effects collectively known as sonopermeation. However, clinical translation of USMB therapy is hampered by the large variety of (non-clinical) US set-ups and US parameters that are used in these studies, which are not easily translated to clinical practice. In order to facilitate clinical translation, the aim of this study was to prove that USMB therapy using a clinical ultrasound system (Philips iU22) in combination with clinically approved microbubbles (SonoVue) leads to efficient sonopermeation. To this end, we measured the efficacy of USMB therapy for different US probes (S5-1, C5-1 and C9-4) and US parameters in FaDu cells. The US probe with the lowest central frequency (i.e. 1.6 MHz for S5-1) showed the highest USMB-induced intracellular uptake of the fluorescent dye SYTOX™ Green (SG). These SG uptake levels were comparable to or even higher than those obtained with a custom-built US system with optimized US parameters. Moreover, USMB therapy with both the clinical and the custom-built US system increased the cytotoxicity of the hydrophilic drug bleomycin. Our results demonstrate that a clinical US system can be used to perform USMB therapy as efficiently as a single-element transducer set-up with optimized US parameters. Therefore, future trials could be based on these clinical US systems, including validated US parameters, in order to accelerate successful translation of USMB therapy.

摘要

化疗疗效常常因肿瘤细胞对药物摄取不足而降低。超声与微泡(USMB)联合使用已被证明可改善药物递送,并通过统称为声透法的效应提高多种药物的疗效。然而,USMB疗法的临床转化受到这些研究中使用的大量(非临床)超声设备和声参数的阻碍,这些设备和参数不易转化为临床实践。为了促进临床转化,本研究的目的是证明使用临床超声系统(飞利浦iU22)与临床批准的微泡(声诺维)联合进行USMB疗法可实现有效的声透法。为此,我们在FaDu细胞中测量了不同超声探头(S5-1、C5-1和C9-4)和声参数的USMB疗法的疗效。中心频率最低的超声探头(即S5-1为1.6MHz)显示出荧光染料SYTOX™ Green(SG)的最高USMB诱导的细胞内摄取。这些SG摄取水平与使用具有优化超声参数的定制超声系统所获得的水平相当,甚至更高。此外,临床和定制超声系统的USMB疗法均增加了亲水性药物博来霉素的细胞毒性。我们的结果表明,临床超声系统可用于像具有优化超声参数的单元素换能器设备一样高效地进行USMB疗法。因此,未来的试验可以基于这些临床超声系统,包括经过验证的超声参数,以加速USMB疗法的成功转化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ac19/8560689/a29f1a1753a7/fphar-12-768436-g001.jpg

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