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首页> 外文期刊>Journal of the American College of Cardiology >Two-dimensional intravascular near-infrared fluorescence molecular imaging of inflammation in atherosclerosis and stent-induced vascular injury.
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Two-dimensional intravascular near-infrared fluorescence molecular imaging of inflammation in atherosclerosis and stent-induced vascular injury.

机译:动脉粥样硬化炎症和支架引起的血管损伤的二维血管内近红外荧光分子成像。

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摘要

OBJECTIVES: This study sought to develop a 2-dimensional (2D) intravascular near-infrared fluorescence (NIRF) imaging strategy for investigation of arterial inflammation in coronary-sized vessels. BACKGROUND: Molecular imaging of arterial inflammation could provide new insights into the pathogenesis of acute myocardial infarction stemming from coronary atheromata and implanted stents. Presently, few high-resolution approaches can image inflammation in coronary-sized arteries in vivo. METHODS: A new 2.9-F rotational, automated pullback 2D imaging catheter was engineered and optimized for 360 degrees viewing intravascular NIRF imaging. In conjunction with the cysteine protease-activatable imaging reporter Prosense VM110 (VisEn Medical, Woburn, Massachusetts), intra-arterial 2D NIRF imaging was performed in rabbit aortas with atherosclerosis (n =10) or implanted coronary bare-metal stents (n = 10, 3.5-mm diameter, day 7 post-implantation). Intravascular ultrasound provided coregistered anatomical images of arteries. After sacrifice, specimens underwent ex vivo NIRF imaging, fluorescence microscopy, and histological and immunohistochemical analyses. RESULTS: Imaging of coronary artery-scaled phantoms demonstrated 8-sector angular resolution and submillimeter axial resolution, nanomolar sensitivity to NIR fluorochromes, and modest NIRF light attenuation through blood. High-resolution NIRF images of vessel wall inflammation with signal-to-noise ratios >10 were obtained in real-time through blood, without flushing or occlusion. In atherosclerosis, 2D NIRF, intravascular ultrasound-NIRF fusion, microscopy, and immunoblotting studies provided insight into the spatial distribution of plaque protease activity. In stent-implanted vessels, real-time imaging illuminated an edge-based pattern of stent-induced arterial inflammation. CONCLUSIONS: A new 2D intravascular NIRF imaging strategy provides high-resolution in vivo spatial mapping of arterial inflammation in coronary-sized arteries and reveals increased inflammation-regulated cysteine protease activity in atheromata and stent-induced arterial injury.
机译:目的:本研究旨在开发二维(2D)血管内近红外荧光(NIRF)成像策略,以研究冠状血管中的动脉炎症。背景:动脉炎症的分子影像学可以为由冠状动脉粥样斑块和植入支架引起的急性心肌梗死的发病机理提供新的见解。目前,很少有高分辨率的方法可以对体内冠状动脉的炎症成像。方法:设计并优化了一种新的2.9-F旋转自动回拉2D成像导管,可360度查看血管内NIRF成像。结合可激活半胱氨酸蛋白酶的成像报告仪Prosense VM110(马萨诸塞州沃本市的VisEn Medical,VisEn Medical),在动脉粥样硬化的兔子主动脉(n = 10)或植入的冠状裸金属支架(n = 10)中进行动脉内2D NIRF成像。 ,直径3.5毫米,植入后第7天)。血管内超声提供了动脉的配准解剖图像。处死后,对标本进行离体NIRF成像,荧光显微镜以及组织学和免疫组化分析。结果:冠状动脉标模的成像显示8扇区角分辨率和亚毫米轴向分辨率,对NIR荧光染料的纳摩尔灵敏度以及通过血液的适度NIRF光衰减。通过血液实时获取高信噪比> 10的血管壁炎症的高分辨率NIRF图像,而不会出现潮红或阻塞现象。在动脉粥样硬化中,二维NIRF,血管内超声-NIRF融合,显微镜检查和免疫印迹研究提供了对斑块蛋白酶活性空间分布的深入了解。在植入支架的血管中,实时成像可照亮支架诱导的动脉炎症的边缘模式。结论:一种新的二维血管内NIRF成像策略提供了冠状动脉中动脉炎症的高分辨率体内空间定位,并揭示了在动脉粥样硬化和支架诱发的动脉损伤中炎症调节的半胱氨酸蛋白酶活性增加。

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