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首页> 外文期刊>International journal of hyperthermia: The official journal of European Society for Hyperthermic Oncology, North American Hyperthermia Group >The effect of injected dose on localized tumor accumulation and cardiac uptake of doxorubicin in a Vx2 rabbit tumor model using MR-HIFU mild hyperthermia and thermosensitive liposomes
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The effect of injected dose on localized tumor accumulation and cardiac uptake of doxorubicin in a Vx2 rabbit tumor model using MR-HIFU mild hyperthermia and thermosensitive liposomes

机译:利用MR-HIFU温和高温和热敏脂质体,注射剂量对VX2兔肿瘤模型中局部肿瘤积累和心肌吸收的影响

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Purpose When doxorubicin (DOX) is administered via lyso-thermosensitive liposomes (LTLD), mild hyperthermia enhances localized delivery to heated vs. unheated tumors. The optimal LTLD dose and the impact of different doses on systemic drug distribution are unknown. Materials and methods: In this study, we evaluated local and systemic DOX delivery with three LTLD doses (0.1, 0.5, and 2.5 mg/kg) in a Vx2 rabbit tumor model. Temporally and spatially accurate controlled hyperthermia was achieved using a clinical MR-HIFU system for the intended heating duration (40 min). Results: DOX concentration in tissues delivered from LTLD combined with MR-HIFU mild hyperthermia are dose-dependent, including heated/unheated tumor, heart, and other healthy organs. Higher DOX accumulation and tumor-to-heart drug concentration ratio, defined as the ratio of DOX delivered into the tumor vs the heart, were observed in heated tumors compared to unheated tumors in all three tested doses. The DOX uptake efficiency for each mg/kg of LTLD injected IV of heated tumor was significantly higher than that of unheated tumor and heart within the tested dose range (0.1-2.5 mg/kg). The DOX uptake for the heart linearly scaled up as a function of dose while that for the heated tumor showed some evidence of saturation at the high dose of 2.5 mg/kg. Conclusions: These results provide guidance on clinical protocol design of hyperthermia-triggered drug delivery.
机译:目的,当莫制菌素(DOX)通过LySO-热敏脂质体(LTLD)给药时,轻度热热增强局部递送至加热的与加热的肿瘤。最佳LTLD剂量和不同剂量对系统性药物分布的影响是未知的。材料和方法:在本研究中,我们在Vx2兔肿瘤模型中评估了三种LTLD剂量(0.1,0.1,0.5和2.5mg / kg)的局部和全身性DOX递送。使用临床MR-HIFU系统实现时间和空间准确的控制热疗,用于预期的加热持续时间(40分钟)。结果:从LTLD提供的组织中的DOX浓度与HIFU MR-HIFU温和的热疗是剂量依赖性的,包括加热/未加热的肿瘤,心脏和其他健康器官。在加热的肿瘤中,在所有三种测试剂量中,在加热的肿瘤中观察到较高的DOX积聚和肿瘤到心脏药物浓度比。每个Mg / kg的加热肿瘤IV的每个mg / kg的DOX吸收效率显着高于测试剂量范围内(0.1-2.5mg / kg)的未加热肿瘤和心脏。心脏的DOX摄取是作为剂量的函数线性缩放,而用于加热的肿瘤的函数显示出在2.5mg / kg的高剂量下饱和的一些证据。结论:这些结果为临床协议设计提供了高温触发药物递送的指导。

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