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首页> 外文期刊>Frontiers in Cardiovascular Medicine >Intravascular Molecular Imaging: Near-Infrared Fluorescence as a New Frontier
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Intravascular Molecular Imaging: Near-Infrared Fluorescence as a New Frontier

机译:血管内分子成像:近红外荧光作为新的前沿

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Despite exciting advances in structural intravascular imaging (intravascular ultrasound (IVUS) and optical coherence tomography (OCT)) that have enabled partial assessment of atheroma burden and high-risk features associated with acute coronary syndromes, structural-based imaging modalities alone do not comprehensively phenotype the complex pathobiology of atherosclerosis. Near-infrared fluorescence (NIRF) is an emerging molecular intravascular imaging modality that allows for in vivo visualization of pathobiological and cellular processes at atheroma plaque level, including inflammation, oxidative stress, and abnormal endothelial permeability. Established intravascular NIRF imaging targets include macrophages, cathepsin protease activity, oxidized low-density lipoprotein and abnormal endothelial permeability. Structural and molecular intravascular imaging provide complementary information about plaque microstructure and biology. For this reason, integrated hybrid catheters that combine NIRF-IVUS or NIRF-OCT have been developed to allow co-registration of morphological and molecular processes with a single pullback, as performed for standalone IVUS or OCT. NIRF imaging is approaching application in clinical practice. This will be accelerated by the use of FDA-approved indocyanine green (ICG), which illuminates lipid- and macrophage-rich zones of permeable atheroma. The ability to comprehensively phenotype coronary pathobiology in patients will enable a deeper understanding of plaque pathobiology, improve local and patient-based risk prediction, and usher in a new era of personalized therapy.
机译:尽管结构血管内成像(血管内超声(IVUS)和光学相干断层扫描(OCT)),但能够进行部分评估动脉瘤负荷和与急性冠状动脉综合征相关的高危特征,仅仅是基于结构的成像模式,单独的全面表型动脉粥样硬化的复杂病态生物学。近红外荧光(NIRF)是一种新兴的分子血管内成像模态,其允许体内可视化病症和细胞过程在运动斑块水平,包括炎症,氧化应激和异常内皮渗透性。建立的血管内NIRF成像靶标包括巨噬细胞,组织蛋白酶蛋白酶活性,氧化低密度脂蛋白和异常内皮渗透性。结构和分子血管内成像提供有关斑块微观结构和生物学的互补信息。因此,已经开发出结合NIRF-IVUS或NIRF-OCT结合NIRF-IVUS或NIRF-OCT的集成混合导管,以允许与独立IVUS或OCT进行单一回调的形态和分子过程共同登记。 NIRF成像正在接近临床实践中的应用。通过使用FDA批准的吲哚菁绿(ICG)将加速,这将照亮渗透性动脉粥样硬化的脂质和巨噬细胞的区域。在患者中全面表型冠状动脉病病病变能力将能够更深入地了解斑块病理学,改善基于局部和患者的风险预测,并在个性化治疗的新时代。

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