Ultrasound-triggered drug release and cytotoxicity of microbubbles with diverse drug attributes.

IF 8.7 1区 化学 Q1 ACOUSTICS Ultrasonics Sonochemistry Pub Date : 2025-01-01 Epub Date: 2024-12-01 DOI:10.1016/j.ultsonch.2024.107182
Chi-Fen Chuang, Chia-Wei Lin, Chih-Kuang Yeh
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Abstract

Ultrasound (US)-triggered cavitation of drug-loaded microbubbles (MBs) represents a promising approach for targeted drug delivery, with substantial benefits attainable through precise control over drug release dosage and form. This study investigates Camptothecin-loaded MBs (CPT-MBs) and Doxorubicin-loaded MBs (DOX-MBs), focusing on how properties such as hydrophilicity, hydrophobicity, and charged functional groups affect their interaction with the lipid surfaces of MBs, thereby influencing the fundamental characteristics and acoustic properties of the drug-loaded MBs. In comparison to DOX-MBs, CPT-MBs showed larger MB size (2.2 ± 0.3 and 1.4 ± 0.1 μm, respectively), a 2-fold increase in drug loading, and an 18 % reduction in leakage after 2 h at 37℃. Under 1 MHz US with a 100 ms pulse repetition interval (PRI), 1000 cycles, 5-minute duration, and 550 kPa acoustic pressure, CPT-MBs undergo inertial cavitation, while DOX-MBs undergo stable cavitation. Drug particles released from these MBs under US-induced cavitation were analyzed using dynamic light scattering, NanoSight, cryo-electron microscopy, and density gradient ultracentrifugation. Results showed that CPT-MBs mainly release free CPT, while DOX-MBs release multilayered DOX-lipid aggregates. The cytotoxicity to C6 cells induced by US-triggered cavitation of these two types of MBs also differed. DOX-lipid aggregates delayed initial uptake, leading to less pronounced short-term (2 h) effects compared to the rapid release of free CPT from CPT-MBs. These findings underscore the need to optimize drug delivery strategies by fine-tuning MB composition and US parameters to control drug release kinetics and achieve the best tumoricidal outcomes.

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超声触发不同药物属性微泡的药物释放和细胞毒性。
超声(US)触发的载药微泡(mb)空化是一种很有前途的靶向药物递送方法,通过精确控制药物释放剂量和形式可以获得实质性的好处。本研究研究了喜树碱负载的MBs (CPT-MBs)和阿霉素负载的MBs (DOX-MBs),重点研究了亲水性、疏水性和带电官能团等性质如何影响它们与MBs脂质表面的相互作用,从而影响载药MBs的基本特性和声学特性。与dox -MB相比,cpt -MB的MB尺寸更大(分别为2.2±0.3 μm和1.4±0.1 μm),载药量增加2倍,37℃作用2 h后漏药量减少18%。在1 MHz US、100 ms脉冲重复间隔(PRI)、1000个周期、5分钟持续时间和550 kPa声压下,cpt - mb发生惯性空化,而dox - mb发生稳定空化。利用动态光散射、NanoSight、低温电镜和密度梯度超离心等技术对us诱导空化作用下MBs释放的药物颗粒进行分析。结果表明,CPT- mbs主要释放游离CPT,而DOX-MBs释放多层dox -脂质聚集体。两种MBs在us诱导空化作用下对C6细胞的细胞毒性也不同。dox -脂质聚集体延迟了初始摄取,与从CPT- mb中快速释放游离CPT相比,导致短期(2小时)效应不那么明显。这些发现强调需要通过微调MB组成和US参数来优化药物递送策略,以控制药物释放动力学并达到最佳的杀肿瘤效果。
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来源期刊
Ultrasonics Sonochemistry
Ultrasonics Sonochemistry 化学-化学综合
CiteScore
15.80
自引率
11.90%
发文量
361
审稿时长
59 days
期刊介绍: Ultrasonics Sonochemistry stands as a premier international journal dedicated to the publication of high-quality research articles primarily focusing on chemical reactions and reactors induced by ultrasonic waves, known as sonochemistry. Beyond chemical reactions, the journal also welcomes contributions related to cavitation-induced events and processing, including sonoluminescence, and the transformation of materials on chemical, physical, and biological levels. Since its inception in 1994, Ultrasonics Sonochemistry has consistently maintained a top ranking in the "Acoustics" category, reflecting its esteemed reputation in the field. The journal publishes exceptional papers covering various areas of ultrasonics and sonochemistry. Its contributions are highly regarded by both academia and industry stakeholders, demonstrating its relevance and impact in advancing research and innovation.
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