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首页> 外文期刊>Journal of the American Society of Echocardiography: official publication of the American Society of Echocardiography >Effect of acoustic power on in vivo molecular imaging with targeted microbubbles: implications for low-mechanical index real-time imaging.
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Effect of acoustic power on in vivo molecular imaging with targeted microbubbles: implications for low-mechanical index real-time imaging.

机译:声功率对靶向微气泡的体内分子成像的影响:对低机械指数实时成像的影响。

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摘要

BACKGROUND: The aim of this study was to evaluate the influence of acoustic power on ultrasound molecular imaging data with targeted microbubbles. METHODS: Imaging was performed with a contrast-specific multipulse method at mechanical indexes (MIs) of 0.18 and 0.97. In vitro imaging was used to measure concentration-intensity relationships and to assess whether damping from microbubble attachment to cultured endothelial cells affected signal enhancement. Power-related differences in signal enhancement were evaluated in vivo by P-selectin-targeted and control microbubble imaging in a murine model of hind-limb ischemia-reperfusion injury. RESULTS: During in vitro experiments, there was minimal acoustic damping from microbubble-cell attachment at either MI. Signal enhancement in the in vitro and in vivo experiments was 2-fold to 3-fold higher for high-MI imaging compared with low-MI imaging, which was due to greater pixel intensity, the detection of a greater number of retained microbubbles, and increased point-spread function. Yet there was a linear relationship between high-MI and low-MI data indicating that the relative degree of enhancement was similar. CONCLUSION: During molecular imaging, high-MI protocols produce more robust targeted signal enhancement than low-MI protocols, although differences in relative enhancement caused by condition or agent are similar.
机译:背景:这项研究的目的是评估声功率对有针对性的微气泡的超声分子成像数据的影响。方法:采用对比特异性多脉冲方法在机械指数(MIs)为0.18和0.97时进行成像。体外成像用于测量浓度-强度关系并评估从微泡附着到培养的内皮细胞的阻尼是否影响信号增强。在后肢缺血-再灌注损伤的小鼠模型中,通过P-选择素靶向和对照微泡成像在体内评估了信号增强中与功率相关的差异。结果:在体外实验中,任一MI处的微气泡细胞附着均产生最小的声阻尼。与低MI成像相比,高MI成像在体外和体内实验中的信号增强高2到3倍,这是由于像素强度更高,检测到更多数量的保留微气泡以及增加点扩散功能。高MI和低MI数据之间存在线性关系,表明相对增强程度相似。结论:在分子成像过程中,尽管由条件或药物引起的相对增强差异相似,但高MI方案比低MI方案产生更强的靶向信号增强。

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