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首页> 外文期刊>Investigative radiology >Electroporation-mediated transcatheter arterial chemoembolization in the rabbit VX2 liver tumor model.
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Electroporation-mediated transcatheter arterial chemoembolization in the rabbit VX2 liver tumor model.

机译:在兔VX2肝肿瘤模型中电穿孔介导的经导管动脉化疗栓塞。

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RATIONALE AND OBJECTIVES: Electropermeabilization involves the application of electrical pulses to increase cell membrane permeability. The purpose of our study was to demonstrate the potential to use electroporation-mediated transcatheter arterial chemoembolization (E-TACE) approaches to increase liver tumor drug uptake while using magnetic resonance imaging (MRI) for intraprocedural optimization of these procedures. METHODS: Fourteen VX2 tumors were grown in the left hepatic lobes of 8 rabbits. Two tumors were grown in each of 6 rabbits (1 tumor serving as E-TACE-treated tumor and the other as nonelectroporated control), and solitary larger tumors were grown in 2 rabbits (half of the tumor treated with E-TACE, remaining half serving as control). Each rabbit was selectively catheterized under digital subtraction angiography guidance. Baseline MRI was performed to generate tumor contrast enhancement curves following catheter-directed infusion of gadopentetate dimeglumine to estimate the proper time delay between subsequent bolus infusion of cisplatin and application of electrical pulses (electrodes were used to deliver 8, 100-mus, 1300-V pulses at the selected delay interval postinfusion). Three hours after E-TACE, rabbits were euthanized, and tumors were sectioned for inductively coupled plasma mass spectroscopy measurements of platinum concentration (serving as reference standard of cisplatin uptake levels). RESULTS: Inductively coupled plasma mass spectroscopy results demonstrated significantly increased cisplatin uptake in E-TACE-treated tumor tissues, increases of 6.0 +/- 3.3-fold compared with transcatheter infusion alone (P = 0.017). CONCLUSIONS: Our findings suggest that our E-TACE approach may significantly increase liver tumor drug uptake after targeted transcatheter infusion. MRI measurements permitted intraprocedural guidance during these catheter-directed E-TACE procedures.
机译:理由和目的:电通透性涉及施加电脉冲以增加细胞膜通透性。我们研究的目的是证明使用电穿孔介导的经导管动脉化学栓塞(E-TACE)方法增加肝脏肿瘤药物摄取的潜力,同时使用磁共振成像(MRI)进行这些程序的过程内优化。方法:14只VX2肿瘤在8只兔子的左肝叶中生长。每6只兔子中有2个肿瘤生长(1个肿瘤用作E-TACE治疗的肿瘤,另一只作为非电穿孔对照),并且在2只兔子中生长了单独的较大肿瘤(用E-TACE治疗的肿瘤占一半,其余一半作为控件)。在数字减影血管造影术指导下选择性地对每只兔子进行导管插入。导管定向输注g戊二酸二聚葡胺后,进行基线MRI成像以产生肿瘤对比增强曲线,以估计随后的顺铂大剂量输注与电脉冲施加之间的适当时间延迟(电极用于输送8、100 mus,1300 V输液后以选定的延迟间隔输出脉冲)。 E-TACE后三小时,对兔子实施安乐死,将肿瘤切成薄片,用于电感耦合血浆质谱法测量铂浓度(用作顺铂吸收水平的参考标准)。结果:电感耦合等离子体质谱法的结果表明,与单独经导管输注相比,E-TACE处理的肿瘤组织中顺铂的摄取显着增加,增加了6.0 +/- 3.3倍(P = 0.017)。结论:我们的研究结果表明我们的E-TACE方法可能会在靶向经导管输注后显着增加肝肿瘤药物的吸收。在这些导管导向的E-TACE程序中,MRI测量允许进行过程内指导。

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