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Optical and acoustical observations of the effects of ultrasound on contrast agents

机译:超声对造影剂影响的光学和声学观察

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Optimal use of encapsulated microbubbles for ultrasound contrast agents and drug delivery requires an understanding of the complex set of phenomena that affect the contrast agent echo and persistence. With the use of a video microscopy system coupled to either an ultrasound flow phantom or a chamber for insonifying stationary bubbles, we show that ultrasound has significant effects on encapsulated microbubbles. In vitro studies show that a train of ultrasound pulses can alter the structure of an albumin-shelled bubble, initiate various mechanisms of bubble destruction or produce aggregation that changes the echo spectrum. In this analysis, changes observed optically are compared with those observed acoustically for both albumin and lipid-shelled agents. We show that, when insonified with a narrowband pulse at an acoustic pressure of several hundred kPa, a phospholipid-shelled bubble can undergo net radius fluctuations of at least 15%; and an albumin-shelled bubble initially demonstrates constrained expansion and contraction. If the albumin shell contains air, the shell may not initially experience surface tension; therefore, the echo changes more significantly with repeated pulsing. A set of observations of contrast agent destruction is presented, which includes the slow diffusion of gas through the shell and formation of a shell defect followed by rapid diffusion of gas into the surrounding liquid. These observations demonstrate that the low-solubility gas used in these agents can persist for several hundred milliseconds in solution. With the transmission of a high-pulse repetition rate and a low pressure, the echoes from, contrast agents can be affected by secondary radiation force. Secondary radiation force is an attractive force for these experimental conditions, creating aggregates with distinct echo characteristics and extended persistence. The scattered echo from an aggregate is several times stronger and more narrowband than echoes from individual bubbles.
机译:为超声造影剂和药物输送最佳地使用封装的微泡,需要了解影响造影剂回声和持久性的一系列复杂现象。通过将视频显微镜系统与超声流动体模或超声室耦合使用,我们可以证明超声对封装的微泡具有重大影响。体外研究表明,一系列超声波脉冲可以改变带白蛋白的气泡的结构,引发气泡破坏的各种机制或产生改变回波光谱的聚集。在此分析中,将光学观察到的变化与白蛋白和脂质脱壳剂的声学观察结果进行了比较。我们表明,当在几百kPa的声压下用窄带脉冲声化时,磷脂壳气泡会经历至少15%的净半径波动;带有白蛋白的气泡最初显示出受约束的膨胀和收缩。如果白蛋白壳中含有空气,则该壳最初可能不会受到表面张力的影响。因此,回声随着重复脉冲而变化更大。提出了一系列造影剂破坏的观察结果,包括气体通过壳的缓慢扩散和壳缺陷的形成,然后气体迅速扩散到周围的液体中。这些观察表明,这些试剂中使用的低溶解度气体可以在溶液中持续数百毫秒。通过高脉冲重复率和低压的传输,造影剂的回波会受到二次辐射力的影响。对于这些实验条件,次级辐射力是一种吸引力,它会产生具有明显回波特性和持久性的聚集体。来自聚集体的散射回波比单个气泡的回波强几倍,带宽更窄。

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