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Fluorescence lifetime imaging microscopy for the characterization ofatherosclerotic plaques

机译:荧光寿命显微镜显微镜,用于表征TheroRotic Plaques

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Atherosclerotic plaque composition has been associated with plaque instability and rupture. This study investigates the use of fluorescence lifetime imaging microscopy (FLIM) for mapping plaque composition and assessing features of vulnerability. Measurements were conducted in atherosclerotic human aortic samples using an endoscopic FLIM system (spatial resolution of 35 μm; temporal resolution 200 ps) developed in our lab which allows mapping in one measurement the composition within a volume of 4 mm diameter x 250 gm depth. Each pixel in the image represents a corresponding fluorescence lifetime value; images are formed through a flexible 0.6 mm side-viewing imaging bundle which allows for further intravascular applications. Based on previously recorded spectra of human atherosclerotic plaque, fluorescence emission was collected through two filters: fl: 377/50 and f2: 460/60 (center wavelength/bandwidth), which together provides the greatest discrimination between intrinsic fluorophores related to plaque vulnerability. We have imaged nine aortas and lifetime images were retrieved using a Laguerre expansion deconvolution technique and correlated with histopathology. Early results demonstrate discrimination using fluorescence lifetime between early, lipid-rich, and collagen-rich lesions which are consistent with previously reported time-resolved atherosclerotic plaque measurements.
机译:动脉粥样硬化斑块组合物与斑块不稳定性和破裂有关。本研究研究了荧光寿命成像显微镜(FLIM)用于绘制斑块组成和评估脆弱性的特征。使用内窥镜FLIM系统(空间分辨率为35μm的空间分辨率)在动脉粥样硬化的人主动脉样品中进行测量;在我们的实验室中开发的时间分辨率200 ps),其允许在一个测量中映射到4mm直径×250克250的体积内的组合物。图像中的每个像素表示相应的荧光寿命值;通过柔性0.6mm侧视图成像束形成图像,其允许进一步的血管内应用。基于先前记录的人类动脉粥样硬化斑块的光谱,通过两个过滤器收集荧光发射:FL:377/50和F2:460/60(中心波长/带宽),其中共同提供与斑块脆弱性有关的内在荧光团之间的最大判断。我们已经进行了成像九个主动脉,使用LAGUERRE扩展解卷积技术检索寿命图像,并与组织病理学相关。早期结果表明使用早期,富含脂质和富含胶原富叶片之间的荧光寿命的歧视,其与先前报道的时间分辨动脉粥样硬化斑块测量一致。

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