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声介导血脑屏障开放过程中脂质壳微泡的时间稳定性

Temporal stability of lipid-shelled microbubbles during acoustically-mediated blood-brain barrier opening.

作者信息

Pouliopoulos Antonios N, Jimenez Daniella A, Frank Alexander, Robertson Alexander, Zhang Lin, Kline-Schoder Alina R, Bhaskar Vividha, Harpale Mitra, Caso Elizabeth, Papapanou Nicholas, Anderson Rachel, Li Rachel, Konofagou Elisa E

机构信息

Department of Biomedical Engineering, Columbia University, New York City, New York 10032, USA.

Department of Radiology, Columbia University, New York City, New York 10032, USA.

出版信息

Front Phys. 2020 May;8. doi: 10.3389/fphy.2020.00137. Epub 2020 May 6.

Abstract

Non-invasive blood-brain barrier (BBB) opening using focused ultrasound (FUS) is being tested as a means to locally deliver drugs into the brain. Such FUS therapies require injection of preformed microbubbles, currently used as contrast agents in ultrasound imaging. Although their behavior during exposure to imaging sequences has been well described, our understanding of microbubble stability within a therapeutic field is still not complete. Here, we study the temporal stability of lipid-shelled microbubbles during therapeutic FUS exposure in two timescales: the short time scale (i.e., μs of low-frequency ultrasound exposure) and the long time scale (i.e., days post-activation). We first simulated the microbubble response to low-frequency sonication, and found a strong correlation between viscosity and fragmentation pressure. Activated microbubbles had a concentration decay constant of 0.02 d but maintained a quasi-stable size distribution for up to 3 weeks (< 10% variation). Microbubbles flowing through a 4-mm vessel within a tissue-mimicking phantom (5% gelatin) were exposed to therapeutic pulses (f: 0.5 MHz, peak-negative pressure: 300 kPa, pulse length: 1 ms, pulse repetition frequency: 1 Hz, n=10). We recorded and analyzed their acoustic emissions, focusing on emitted energy and its temporal evolution, alongside the frequency content. Measurements were repeated with concentration-matched samples (10 microbubbles/ml) on day 0, 7, 14, and 21 after activation. Temporal stability decreased while inertial cavitation response increased with storage time both and , possibly due to changes in the shell lipid content. Using the same parameters and timepoints, we performed BBB opening in a mouse model (n=3). BBB opening volume measured through T1-weighted contrast-enhanced MRI was equal to 19.1 ± 7.1 mm, 21.8 ± 14 mm, 29.3 ± 2.5 mm, and 38 ± 20.1 mm on day 0, 7, 14, and 21, respectively, showing no significant difference over time (p-value: 0.49). Contrast enhancement was 24.9 ± 1.7 %, 23.7 ± 11.7 %, 28.9 ± 5.3 %, and 35 ± 13.4 %, respectively (p-value: 0.63). In conclusion, the in-house made microbubbles studied here maintain their capacity to produce similar therapeutic effects over a period of 3 weeks after activation, as long as the natural concentration decay is accounted for. Future work should focus on stability of commercially available microbubbles and tailoring microbubble shell properties towards therapeutic applications.

摘要

使用聚焦超声(FUS)无创打开血脑屏障(BBB)正在作为一种将药物局部递送至大脑的方法进行测试。此类FUS疗法需要注射预制微泡,目前其在超声成像中用作造影剂。尽管它们在成像序列曝光期间的行为已得到充分描述,但我们对治疗场中微泡稳定性的理解仍不完整。在此,我们在两个时间尺度上研究了脂质壳微泡在治疗性FUS曝光期间的时间稳定性:短时间尺度(即低频超声曝光的微秒级)和长时间尺度(即激活后数天)。我们首先模拟了微泡对低频超声处理的响应,发现粘度与破碎压力之间存在很强的相关性。激活的微泡浓度衰减常数为0.02 d,但在长达3周内保持准稳定的尺寸分布(变化<10%)。使流经组织模拟体模(5%明胶)内4毫米血管的微泡暴露于治疗脉冲(频率:0.5 MHz,负峰值压力:300 kPa,脉冲长度:1 ms,脉冲重复频率:1 Hz,n = 10)。我们记录并分析了它们的声发射,重点关注发射能量及其时间演变以及频率成分。在激活后第0、7、14和21天,用浓度匹配的样品(10个微泡/毫升)重复测量。随着储存时间的延长,时间稳定性降低,而惯性空化响应增加,这可能是由于壳脂质含量的变化所致。使用相同的参数和时间点,我们在小鼠模型(n = 3)中进行了BBB打开实验。通过T1加权对比增强MRI测量的BBB打开体积在第0、7、14和21天分别等于19.1±7.1立方毫米、21.8±14立方毫米、29.3±2.5立方毫米和38±20.1立方毫米,随时间无显著差异(p值:0.49)。对比增强分别为24.9±1.7%、23.7±11.7%、28.9±5.3%和35±13.4%(p值:0.63)。总之,只要考虑到自然浓度衰减,此处研究的自制微泡在激活后3周内保持产生相似治疗效果的能力。未来的工作应侧重于市售微泡的稳定性以及针对治疗应用定制微泡壳特性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/afa1/7250395/47fec85ae38a/nihms-1585710-f0001.jpg

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