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用于超声-微泡介导药物输送研究的工程化 3D 微血管网络。

Engineered 3D Microvascular Networks for the Study of Ultrasound-Microbubble-Mediated Drug Delivery.

机构信息

Department of Bioengineering , University of Washington , Seattle , Washington 98195 , United States.

出版信息

Langmuir. 2019 Aug 6;35(31):10128-10138. doi: 10.1021/acs.langmuir.8b03288. Epub 2018 Dec 20.

DOI:10.1021/acs.langmuir.8b03288
PMID:30540481
Abstract

Localized and targeted drug delivery can be achieved by the combined action of ultrasound and microbubbles on the tumor microenvironment, likely through sonoporation and other therapeutic mechanisms that are not well understood. Here, we present a perfusable in vitro model with a realistic 3D geometry to study the interactions between microbubbles and the vascular endothelium in the presence of ultrasound. Specifically, a three-dimensional, endothelial-cell-seeded in vitro microvascular model was perfused with cell culture medium and microbubbles while being sonicated by a single-element 1 MHz focused transducer. This setup mimics the in vivo scenario in which ultrasound induces a therapeutic effect in the tumor vasculature in the presence of flow. Fluorescence and bright-field microscopy were employed to assess the microbubble-vessel interactions and the extent of drug delivery and cell death both in real time during treatment as well as after treatment. Propidium iodide was used as the model drug while calcein AM was used to evaluate cell viability. There were two acoustic parameter sets chosen for this work: (1) acoustic pressure: 1.4 MPa, pulse length: 500 cycles, duty cycle: 5% and (2) acoustic pressure: 0.4 MPa, pulse length: 1000 cycles, duty cycle: 20%. Enhanced drug delivery and cell death were observed in both cases while the higher pressure setting had a more pronounced effect. By introducing physiological flow to the in vitro microvascular model and examining the PECAM-1 expression of the endothelial cells within it, we demonstrated that our model is a good mimic of the in vivo vasculature and is therefore a viable platform to provide mechanistic insights into ultrasound-mediated drug delivery.

摘要

局部和靶向药物输送可以通过超声和微泡对肿瘤微环境的联合作用来实现,可能通过声孔作用和其他尚未完全理解的治疗机制来实现。在这里,我们提出了一种具有真实 3D 几何形状的可灌注体外模型,用于研究超声存在下微泡与血管内皮之间的相互作用。具体来说,使用单细胞 1 MHz 聚焦换能器对灌注有细胞培养基和微泡的三维、内皮细胞接种的体外微血管模型进行超声处理。该设置模拟了体内情景,即在存在流动的情况下,超声在肿瘤血管中诱导治疗效果。荧光和明场显微镜用于评估微泡-血管相互作用以及药物输送和细胞死亡的程度,包括在治疗过程中和治疗后实时进行评估。碘化丙啶被用作模型药物,而钙黄绿素 AM 被用于评估细胞活力。我们选择了两种声学参数集用于这项工作:(1)声压:1.4 MPa,脉冲长度:500 个周期,占空比:5%;(2)声压:0.4 MPa,脉冲长度:1000 个周期,占空比:20%。在这两种情况下,都观察到了增强的药物输送和细胞死亡,而较高的压力设置具有更明显的效果。通过将生理流动引入体外微血管模型并检查其中内皮细胞的 PECAM-1 表达,我们证明我们的模型很好地模拟了体内血管,因此是提供对超声介导药物输送的机制见解的可行平台。

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