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Pharmacodynamic Analysis of Magnetic Resonance Imaging-Monitored Focused Ultrasound-Induced Blood-Brain Barrier Opening for Drug Delivery to Brain Tumors

机译:磁共振成像监测的聚焦超声诱导的血脑屏障开放的药物动力学分析,用于向脑肿瘤的药物递送。

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摘要

Microbubble-enhanced focused ultrasound (FUS) can enhance the delivery of therapeutic agents into the brain for brain tumor treatment. The purpose of this study was to investigate the influence of brain tumor conditions on the distribution and dynamics of small molecule leakage into targeted regions of the brain after FUS-BBB opening. A total of 34 animals were used, and the process was monitored by 7T-MRI. Evans blue (EB) dye as well as Gd-DTPA served as small molecule substitutes for evaluation of drug behavior. EB was quantified spectrophotometrically. Spin-spin (R1) relaxometry and area under curve (AUC) were measured by MRI to quantify Gd-DTPA. We found that FUS-BBB opening provided a more significant increase in permeability with small tumors. In contrast, accumulation was much higher in large tumors, independent of FUS. The AUC values of Gd-DTPA were well correlated with EB delivery, suggesting that Gd-DTPA was a good indicator of total small-molecule accumulation in the target region. The peripheral regions of large tumors exhibited similar dynamics of small-molecule leakage after FUS-BBB opening as small tumors, suggesting that FUS-BBB opening may have the most significant permeability-enhancing effect on tumor peripheral. This study provides useful information toward designing an optimized FUS-BBB opening strategy to deliver small-molecule therapeutic agents into brain tumors.
机译:微泡增强聚焦超声(FUS)可以增强治疗剂向大脑的输送,以治疗脑肿瘤。这项研究的目的是调查FUS-BBB开放后,脑部肿瘤状况对小分子泄漏到脑部目标区域的分布和动力学的影响。总共使用了34只动物,并通过7T-MRI监测该过程。伊文思蓝(EB)染料以及Gd-DTPA可用作评估药物行为的小分子替代品。 EB用分光光度法定量。通过MRI测量自旋(R1)弛豫法和曲线下面积(AUC)以量化Gd-DTPA。我们发现,FUS-BBB开孔可在小肿瘤的通透性方面提供更大的提高。相反,大肿瘤中的蓄积要高得多,与FUS无关。 Gd-DTPA的AUC值与EB传递密切相关,表明Gd-DTPA是目标区域总小分子积累的良好指标。 FUS-BBB开放后,大肿瘤的周边区域表现出与小肿瘤相似的小分子渗漏动态,这表明FUS-BBB开放可能对肿瘤的周边具有最显着的通透性增强作用。这项研究为设计优化的FUS-BBB开放策略提供了有用的信息,以将小分子治疗剂输送到脑瘤中。

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