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首页> 外文期刊>Journal of vascular and interventional radiology: JVIR >Near-Infrared Fluorescence Imaging of Matrix Metalloproteinase 2 Activity as a Biomarker of Vascular Remodeling in Hemodialysis Access
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Near-Infrared Fluorescence Imaging of Matrix Metalloproteinase 2 Activity as a Biomarker of Vascular Remodeling in Hemodialysis Access

机译:基质金属蛋白酶2的近红外荧光成像2活性作为血液透析通道血管重塑的生物标志物

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摘要

PurposeTo establish the capability of near-infrared fluorescence (NIRF) imaging for the detection of matrix metalloproteinase 2 (MMP-2) activity as a biomarker of vascular remodeling (VR) in arteriovenous fistulae (AVFs) in?vivo. Materials and MethodsAVFs were created in the right groins of Wistar rats (n?= 10), and sham procedures were performed in the contralateral groins. Fistulography via a left common carotid artery approach confirmed stenosis (> 50%) in a subset of animals (n?= 5) 4 weeks after AVF creation. After administration of MMP-2–activated NIRF probe, near-infrared imaging was performed in?vivo and ex?vivo of both the AVF and the sham-treated vessels to measure radiant efficiency of MMP-2–activated NIRF signal over background. Histologic analyses of AVF and sham-treated vessels were performed to measure VR defined as inward growth of the vessel caused by intimal thickening. ResultsAVFs demonstrated a significantly higher percentage increase in radiant efficiency over background compared with sham vessels (45.5 ± 56% vs 16.1 ± 17.8%;P?= .008). VR in AVFs was associated with increased thickness of neointima staining positively for MMP-2 (161.8 ± 45.5 μm vs 73.2 ± 36.7 μm;P?= .01). A significant correlation was observed between MMP-2 activity as measured by relative increase in radiant efficiency for AVFs and thickness of neointima staining positively for MMP-2 (P?= .039). ConclusionsNIRF imaging can detect increased MMP activity in remodeled AVFs compared with contralateral sham vessels. MMP-2–activated NIRF signal correlates with the severity of intimal thickening. These findings suggest NIRF imaging of MMP-2 may be used as a biomarker of the vascular remodeling underlying stenosis.
机译:purposeto建立近红外荧光(NIRF)成像的能力,用于检测基质金属蛋白酶2(MMP-2)活性作为血管瘘(AVFS)中的血管重塑(VR)的生物标志物。在Wistar大鼠的右腹部(n≤10)产生材料和方法,并且在对侧腹股沟中进行假手术。通过左常见的颈动脉方法的瘘管术在AVF创建后4周内确认了动物子集中的狭窄(> 50%)(n?= 5)。在施用MMP-2激活的NIRF探针后,在AVF和假处理血管的体内和EXα体内进行近红外成像,以测量背景下的MMP-2激活NIRF信号的辐射效率。进行AVF和假处理血管的组织学分析以测量VR定义为由内膜增稠引起的容器的内向生长。结果AVFS与假血管相比,辐射效率的辐射效率提高显着提高了(45.5±56%Vs 16.1±17.8%; p?= .008)。 AVF中的VR与MMP-2正面染色的厚度增加相关(161.8±45.5μm,73.2±36.7μm; p?= .01)。在MMP-2活性之间观察到显着的相关性,以通过对MMP-2阳性的AVFS和Neointima厚度的辐射效率相对增加来测量(P?= .039)。结论与对侧假血管相比,该结论尼尔成像可以检测重塑AVF中的MMP活性。 MMP-2激活的NIRF信号与内膜增稠的严重程度相关。这些发现表明MMP-2的NIRF成像可以用作血管重塑的缺乏狭窄的生物标志物。

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