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首页> 外文期刊>Journal of Ultrasound in Medicine: Official Journal of the American Institute of Ultrasound in Medicine >Experimental Study on Targeted Methotrexate Delivery to the Rabbit Brain via Magnetic Resonance Imaging–Guided Focused Ultrasound
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Experimental Study on Targeted Methotrexate Delivery to the Rabbit Brain via Magnetic Resonance Imaging–Guided Focused Ultrasound

机译:磁共振成像引导聚焦超声靶向甲氨蝶呤靶向兔脑的实验研究

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Objective. The purpose of this study was to investigate the effects of targeted and reversible disruption of the blood-brain barrier (BBB) by magnetic resonance imaging (MRI)-guided focused ultrasound (FUS) and delivery of methotrexate (MTX) to the rabbit brain. Methods. The brains of 20 rabbits were sonicated by MRI-guided FUS at different exposure times, and then Evans blue extravasation, contrast-enhanced MRI, and histologic examination were performed to determine the optimal exposure time for reversible BBB disruption with minimal damage. Five rabbits were sonicated at the optimal exposure time after MTX was injected intravenously (IV); the targeted locations were included in the sonicated group, and the nontargeted contralateral counterparts were included in the IV control group. Five other rabbits were not subjected to sonication and were administered internal carotid artery (ICA) injections of MTX; the specimens of the counterpart brain tissue were harvested as the ICA group. The MTX concentration in all of the specimens was determined by high-performance liquid chromatography. Results. The MTX concentration in the sonicated group (mean ± SD, 7.412 ± 1.471 μg/g of tissue) was notably higher than that in both the IV control group (0.544 ± 0.084 μg/g) and ICA group (1.984 ± 0.65 μg/g; P <.01). Conclusions. Magnetic resonance imaging–guided FUS can disrupt the BBB reversibly and deliver IV administered MTX to targeted brain locations; it brings about a greater than 10-fold increase in the drug level and is much more effective (≈3.7-fold) than drug delivery through the ICA without sonication. This may facilitate the development of improved treatment methods for central nervous system disorders.
机译:目的。这项研究的目的是研究磁共振成像(MRI)引导的聚焦超声(FUS)靶向性和可逆性破坏血脑屏障(BBB)并将甲氨蝶呤(MTX)递送至兔脑的影响。方法。在不同的暴露时间通过MRI引导的FUS对20只兔的大脑进行超声处理,然后进行伊文思蓝外渗,增强对比的MRI和组织学检查,以确定可逆性BBB破坏的最小暴露时间。静脉注射MTX后,在最佳暴露时间对五只兔子进行超声处理(IV);超声检查组包括目标位置,静脉注射对照组包括非目标对侧对应物。另外五只兔子未进行超声处理,并经颈内动脉(ICA)注射MTX。收集对应的脑组织标本作为ICA组。所有样品中的MTX浓度通过高效液相色谱法测定。结果。超声处理组的MTX浓度(平均±SD,7.412±1.471μg/ g组织)显着高于IV对照组(0.544±0.084μg/ g)和ICA组(1.984±0.65μg/ g) ; P <.01)。结论。磁共振成像引导的FUS可以可逆地破坏血脑屏障,并通过静脉注射MTX将MTX输送到目标大脑位置。它使药物水平增加了10倍以上,并且比不进行超声处理的通过ICA的药物有效得多(约3.7倍)。这可以促进开发用于中枢神经系统疾病的改进的治疗方法。

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