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Hyperthermia-induced doxorubicin delivery from thermosensitive liposomes via MR-HIFU in a pig model

药代动力学 阿霉素 热疗 脂质体 体内分布 药物输送 药理学 化学 医学 化疗 生物医学工程 外科 内科学 生物化学 体外 有机化学
作者
Lukas Christian Sebeke,Juan Daniel Castillo Gómez,Edwin Heijman,Pia Rademann,Alexandra Claudia Simon,Sandra N. Ekdawi,Susan Vlachakis,Dennis Toker,Ben Lasse Mink,Claudia Schubert-Quecke,Sin Yuin Yeo,Patrick Schmidt,Christina Lucas,Susanne Brodesser,Martin Hossann,Lars H. Lindner,Holger Grüll
出处
期刊:Journal of Controlled Release [Elsevier BV]
卷期号:343: 798-812 被引量:33
标识
DOI:10.1016/j.jconrel.2022.02.003
摘要

Encapsulation of cytotoxic drugs for a localized release is an effective way to increase the therapeutic window of such agents. In this article we present the localized release of doxorubicin (DOX) from phosphatidyldiglycerol (DPPG2) based thermosensitive liposomes using MR-HIFU mediated hyperthermia in a swine model.German landrace pigs of weights between 37.5 and 53.5 kg received a 30-min infusion of DOX containing thermosensitive liposomes (50 mg DOX/m2). The pigs' biceps femoris was treated locally in two separate target areas with mild hyperthermia using magnetic resonance guided high intensity focused ultrasound, starting 10 min and 60 min after initiation of the infusion, respectively. The pharmacokinetics and biodistribution of DOX were determined and an analysis of the treatment parameters' influence was performed.Compared to untreated tissue, we found a 15-fold and a 7-fold increase in DOX concentration in the muscle volumes that had undergone hyperthermia starting 10 min and 60 min after the beginning of the infusion, respectively. The pharmacokinetic analysis showed a prolonged circulation time of DOX and a correlation between the AUC of extra-liposomal DOX in the bloodstream and the amount of DOX accumulated in the target tissue.We have demonstrated a workflow for MR-HIFU hyperthermia drug delivery that can be adapted to a clinical setting, showing that HIFU-hyperthermia is a suitable method for local drug release of DOX using DPPG2 based thermosensitive liposomes in stationary targets. Using the developed pharmacokinetic model, an optimization of the drug quantity deposited in the target via the timing of infusion and hyperthermia should be possible.
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