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Fluid viscosity affects the fragmentation and inertial cavitation threshold of lipid encapsulated microbubbles

机译:流体粘度影响脂质包裹的微泡的破碎和惯性空化阈值

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摘要

Ultrasound and microbubble optimization studies for therapeutic applications are often conducted in water/saline, with a fluid viscosity of 1 cP. In an in vivo context, microbubbles are situated in blood, a more viscous fluid (~4 cP). In this study, ultra-high speed microscopy and passive cavitation approaches were employed to investigate the effect of fluid viscosity on microbubble behavior at 1 MHz subject to high pressures (0.25 – 2 MPa). The propensity for individual microbubble (n=220) fragmentation was shown to significantly decrease in 4 cP fluid as compared to 1 cP fluid, despite achieving similar maximum radial excursions. Microbubble populations diluted in 4 cP fluid exhibited decreased wideband emissions (up to 10.2 times), and increasingly distinct harmonic emission peaks (e.g. ultraharmonic) with increasing pressure as compared to 1 cP fluid. These results suggest that in vitro studies should consider an evaluation using physiologic viscosity perfusate before transitioning to in vivo evaluations.
机译:用于治疗应用的超声和微泡优化研究通常在水/盐水中进行,流体粘度为1 cP。在体内环境中,微泡位于血液中,是一种更粘的流体(〜4 cP)。在这项研究中,采用超高速显微镜和被动气蚀方法来研究流体粘度对在1 MHz下承受高压(0.25 – 2 MPa)的微气泡行为的影响。尽管实现了类似的最大径向偏移,但与1 cP流体相比,在4 cP流体中单个微气泡(n = 220)破碎的倾向显示出显着降低。与1 cP流体相比,在4 cP流体中稀释的微气泡种群显示出降低的宽带发射(高达10.2倍),并且随着压力的增加,谐波发射峰(例如超谐波)越来越明显。这些结果表明,体外研究应在过渡到体内评估之前考虑使用生理粘度灌注液进行评估。

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