Efficient ultrasound-mediated drug delivery to orthotopic liver tumors – Direct comparison of doxorubicin-loaded nanobubbles and microbubbles

微气泡 阿霉素 体内 体内分布 药物输送 医学 细胞凋亡 肝癌 超声波 癌症研究 药代动力学 肝肿瘤 药理学 转移 药品 癌症 化疗 化学 内科学 放射科 生物 肝细胞癌 有机化学 生物技术 生物化学
作者
Pinunta Nittayacharn,Eric Abenojar,Michaela B. Cooley,Felipe M. Berg,Claire Counil,Amin Jafari Sojahrood,Muhammad Saad Khan,Celina Yang,Elizabeth S. L. Berndl,Marcin Golczak,Michael C. Kolios,Agata A. Exner
出处
期刊:Journal of Controlled Release [Elsevier BV]
卷期号:367: 135-147 被引量:17
标识
DOI:10.1016/j.jconrel.2024.01.028
摘要

Liver metastasis is a major obstacle in treating aggressive cancers, and current therapeutic options often prove insufficient. To overcome these challenges, there has been growing interest in ultrasound-mediated drug delivery using lipid-shelled microbubbles (MBs) and nanobubbles (NBs) as promising strategies for enhancing drug delivery to tumors. Our previous work demonstrated the potential of Doxorubicin-loaded C3F8 NBs (hDox-NB, 280 ± 123 nm) in improving cancer treatment in vitro using low-frequency unfocused therapeutic ultrasound (TUS). In this study, we investigated the pharmacokinetics and biodistribution of sonicated hDox-NBs in orthotopic rat liver tumors. We compared their delivery and therapeutic efficiency with size-isolated MBs (hDox-MB, 1104 ± 373 nm) made from identical shell material and core gas. Results showed a similar accumulation of hDox in tumors treated with hDox-MBs and unfocused therapeutic ultrasound (hDox-MB + TUS) and hDox-NB + TUS. However, significantly increased apoptotic cell death in the tumor and fewer off-target apoptotic cells in the normal liver were found upon the treatment with hDox-NB + TUS. The tumor-to-liver apoptotic ratio was elevated 9.4-fold following treatment with hDox-NB + TUS compared to hDox-MB + TUS, suggesting that the therapeutic efficacy and specificity are significantly increased when using hDox-NB + TUS. These findings highlight the potential of this approach as a viable treatment modality for liver tumors. By elucidating the behavior of drug-loaded bubbles in vivo, we aim to contribute to developing more effective liver cancer treatments that could ultimately improve patient outcomes and decrease off-target side effects.
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