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Real-Time Technique for Improving Molecular Imaging and Guiding Drug Delivery in Large Blood Vessels: In Vitro and Ex Vivo Results

机译:实时技术,用于改善大血管中的分子成像和指导药物输送:体内和体外结果

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摘要

Ultrasound-based molecular imaging employs targeted microbubbles to image vascular pathology. This approach also has the potential to monitor molecularly targeted microbubble-based drug delivery. We present an image-guided drug delivery technique that uses multiple pulses to translate, image, and cavitate microbubbles in real time. This technique can be applied to both imaging of pathology in large arteries (sizes and flow comparable to those in humans) and guiding localized drug delivery in blood vessels. The microbubble translation (or pushing) efficacy of this technique was compared in a variety of flow media: saline, viscous saline (4 cp), and bovine blood. It was observed that the performance of this approach was marginally better (by 6, 4, and 2 dB) in viscous saline than in bovine blood with varying levels of hematocrit (40%, 30%, and 10%). The drug delivery efficacy of this technique was evaluated by in vitro and ex vivo experiments. High-intensity pulses mediated fluorophore (Dil) deposition on endothelial cells (in vitro) without causing cell destruction. Ex vivo fluorophore delivery experiments conducted on swine carotids of 2 and 5 mm cross-section diameter demonstrated a high degree of correspondence in spatial localization of the fluorophore delivery between the ultrasound and composite fluorescence microscopy images of the arterial cross sections.
机译:基于超声的分子成像采用靶向微泡来成像血管病理。这种方法还具有监测分子靶向的基于微泡的药物递送的潜力。我们提出了一种图像引导的药物输送技术,该技术使用多个脉冲实时翻译,成像和空化微泡。这项技术既可以应用于大动脉的病理成像(大小和血流与人类相当),也可以指导血管中的局部药物输送。在多种流动介质中比较了该技术的微气泡翻译(或推动)功效:盐水,粘性盐水(4厘泊)和牛血。可以观察到,这种方法的性能在粘性盐水中要比在不同血细胞比容水平(40%,30%和10%)的牛血中好一些(分别为6、4和2 dB)。通过体外和离体实验评估了该技术的药物递送功效。高强度脉冲介导的荧光团(Dil)沉积在内皮细胞上(体外)而不会引起细胞破坏。在横截面直径为2和5 mm的猪颈动脉上进行的离体荧光团递送实验表明,在超声和动脉截面的复合荧光显微镜图像之间,荧光团递送的空间定位高度一致。

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  • 来源
    《Molecular imaging》 |2011年第4期|p.238-247|共10页
  • 作者单位

    Department of Biomedical Engineering and Division of Cardiovascular Medicine, University of Virginia, Charlottesville, VA,and Targeson lnc, San Diego, CA;

    Department of Biomedical Engineering and Division of Cardiovascular Medicine, University of Virginia, Charlottesville, VA,and Targeson lnc, San Diego, CA;

    Department of Biomedical Engineering and Division of Cardiovascular Medicine, University of Virginia, Charlottesville, VA,and Targeson lnc, San Diego, CA;

    Department of Biomedical Engineering and Division of Cardiovascular Medicine, University of Virginia, Charlottesville, VA,and Targeson lnc, San Diego, CA;

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  • 入库时间 2022-08-18 00:39:16

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