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较长的加热时间可提高 MR-HIFU 温和热疗联合热敏脂质体阿霉素治疗 Vx2 肿瘤的局部阿霉素沉积和治疗指数。

Longer heating duration increases localized doxorubicin deposition and therapeutic index in Vx2 tumors using MR-HIFU mild hyperthermia and thermosensitive liposomal doxorubicin.

机构信息

a Department of Radiology , UT Southwestern Medical Center , Dallas , TX , USA.

b Children's Health , Dallas , TX , USA.

出版信息

Int J Hyperthermia. 2019;36(1):196-203. doi: 10.1080/02656736.2018.1550815. Epub 2018 Dec 12.

Abstract

Thermosensitive liposomal doxorubicin (LTSL-Dox) combined with mild hyperthermia enhances the localized delivery of doxorubicin (Dox) within a heated region. The optimal heating duration and the impact of extended heating on systemic drug distribution are unknown. Here we evaluated local and systemic Dox delivery with two different mild hyperthermia durations (42 °C for 10 or 40 minutes) in a Vx2 rabbit tumor model. We hypothesized that longer duration of hyperthermia would increase Dox concentration in heated tumors without increasing systemic exposure. Temporally and spatially accurate controlled hyperthermia was achieved using a clinical MR-HIFU system for the prescribed heating durations. Forty-minutes of heating resulted in a nearly 6-fold increase in doxorubicin concentration in heated vs unheated tumors in the same animals. Therapeutic ratio, defined as the ratio of Dox delivered into the heated tumor vs the heart, increased from 1.9-fold with 10 minutes heating to 4.4-fold with 40 minutes heating. MR-HIFU can be used to guide, deliver and monitor mild hyperthermia of a Vx2 tumor model in a rabbit model, and an increased duration of heating leads to higher Dox deposition from LTSL-Dox in a target tumor without a concomitant increase in systemic exposure. Results from this preclinical study can be used to help establish clinical treatment protocols for hyperthermia mediated drug delivery.

摘要

热敏脂质体阿霉素(LTSL-Dox)联合温和热疗可增强加热区域内阿霉素(Dox)的局部递送。最佳加热持续时间以及延长加热对全身药物分布的影响尚不清楚。在这里,我们在 Vx2 兔肿瘤模型中评估了两种不同温和热疗持续时间(42°C 持续 10 或 40 分钟)的局部和全身 Dox 递送。我们假设较长时间的热疗会增加加热肿瘤中的 Dox 浓度,而不会增加全身暴露。使用临床 MR-HIFU 系统在规定的加热持续时间内实现了时间和空间上准确的受控热疗。与在同一动物中未加热的肿瘤相比,40 分钟的加热导致加热肿瘤中的阿霉素浓度增加近 6 倍。治疗比,定义为递送到加热肿瘤中的 Dox 与心脏中的 Dox 之比,从 10 分钟加热的 1.9 倍增加到 40 分钟加热的 4.4 倍。MR-HIFU 可用于引导、输送和监测兔模型中 Vx2 肿瘤模型的温和热疗,并且加热持续时间的延长会导致来自 LTSL-Dox 的更高的 Dox 沉积在靶肿瘤中,而不会同时增加全身暴露。这项临床前研究的结果可用于帮助建立用于热疗介导药物递送的临床治疗方案。

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