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用于药物递送的超声驱动纳米杯

Ultrasound-Propelled Nanocups for Drug Delivery.

作者信息

Kwan James J, Myers Rachel, Coviello Christian M, Graham Susan M, Shah Apurva R, Stride Eleanor, Carlisle Robert C, Coussios Constantin C

机构信息

Institute of Biomedical Engineering, University of Oxford, Oxford, OX3 7DQ, UK.

Department of Oncology, University of Oxford, Oxford, OX3 7DQ, UK.

出版信息

Small. 2015 Oct 21;11(39):5305-14. doi: 10.1002/smll.201501322. Epub 2015 Aug 21.

Abstract

Ultrasound-induced bubble activity (cavitation) has been recently shown to actively transport and improve the distribution of therapeutic agents in tumors. However, existing cavitation-promoting agents are micron-sized and cannot sustain cavitation activity over prolonged time periods because they are rapidly destroyed upon ultrasound exposure. A novel ultrasound-responsive single-cavity polymeric nanoparticle (nanocup) capable of trapping and stabilizing gas against dissolution in the bloodstream is reported. Upon ultrasound exposure at frequencies and intensities achievable with existing diagnostic and therapeutic systems, nanocups initiate and sustain readily detectable cavitation activity for at least four times longer than existing microbubble constructs in an in vivo tumor model. As a proof-of-concept of their ability to enhance the delivery of unmodified therapeutics, intravenously injected nanocups are also found to improve the distribution of a freely circulating IgG mouse antibody when the tumor is exposed to ultrasound. Quantification of the delivery distance and concentration of both the nanocups and coadministered model therapeutic in an in vitro flow phantom shows that the ultrasound-propelled nanocups travel further than the model therapeutic, which is itself delivered to hundreds of microns from the vessel wall. Thus nanocups offer considerable potential for enhanced drug delivery and treatment monitoring in oncological and other biomedical applications.

摘要

最近研究表明,超声诱导的气泡活动(空化作用)能有效运输并改善治疗药物在肿瘤中的分布。然而,现有的空化促进剂为微米级,且由于在超声照射下会迅速被破坏,无法在较长时间内维持空化活性。本文报道了一种新型的超声响应性单腔聚合物纳米颗粒(纳米杯),它能够捕获并稳定气体,防止其在血液中溶解。在现有诊断和治疗系统所能达到的频率和强度下进行超声照射时,在体内肿瘤模型中,纳米杯引发并维持易于检测到的空化活性的时间至少是现有微泡结构的四倍。作为其增强未修饰治疗药物递送能力的概念验证,当肿瘤接受超声照射时,静脉注射的纳米杯还能改善自由循环的IgG小鼠抗体的分布。在体外流动模型中对纳米杯和共同给药的模型治疗药物的递送距离和浓度进行定量分析表明,超声驱动的纳米杯比模型治疗药物传播得更远,而模型治疗药物本身能从血管壁传递到数百微米处。因此,纳米杯在肿瘤学和其他生物医学应用中的药物递送增强和治疗监测方面具有巨大潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4bf5/4660885/d8671813f010/smll0011-5305-f1.jpg

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