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首页> 外文期刊>Arteriosclerosis, thrombosis, and vascular biology >Discrimination of human coronary artery atherosclerotic lipid-rich lesions by time-resolved laser-induced fluorescence spectroscopy.
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Discrimination of human coronary artery atherosclerotic lipid-rich lesions by time-resolved laser-induced fluorescence spectroscopy.

机译:通过时间分辨激光诱导荧光光谱法区分人冠状动脉粥样硬化脂质丰富的病变。

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Lesion composition plays a significant role in atherosclerotic lesion instability and rupture. Current clinical techniques cannot fully characterize lesion composition or accurately identify unstable lesions. This study investigates the use of time-resolved fluorescence spectroscopy for unstable atherosclerotic lesion diagnosis. The fluorescence of human coronary artery samples was induced with nitrogen laser and detected in the 360- to 510-nm wavelength range. The samples were sorted into 7 groups according to the AHA classification: normal wall and types I, II(a) (fatty streaks), III (preatheroma), IV (atheroma), V(a) (fibrous), and V(b) (calcified) lesions. Spectral intensities and time-dependent parameters [average lifetime tau(f); decay constants: tau(1) (fast-term), tau(2) (slow-term), A(1) (fast-term amplitude contribution)] derived from the time-resolved spectra of coronary samples were used for tissue characterization. We determined that a few intensity values at longer wavelengths (>430 nm) and time-dependent parameters at peak emission region (390 nm) discriminate between all types of arterial samples except between normal wall and type I lesions. The lipid-rich lesions (more unstable) can be discriminated from fibrous lesions (more stable) on the basis of time-dependent parameters (lifetime and fast-term decay). We inferred that features of lipid fluorescence are reflected on lipid-rich lesion emission. Our results demonstrate that analysis of the time-resolved spectra may be used to enhance the discrimination between different grades of atherosclerotic lesions and provide a means of discrimination between lipid-rich and fibrous lesions.
机译:病变成分在动脉粥样硬化病变的不稳定性和破裂中起重要作用。当前的临床技术不能完全表征病变组成或不能准确识别不稳定病变。这项研究调查了时间分辨荧光光谱在不稳定动脉粥样硬化病变诊断中的应用。用氮气激光诱导人冠状动脉样品的荧光,并在360至510 nm波长范围内检测到。根据AHA分类将样品分为7组:正常壁和类型I,II(a)(脂肪条纹),III(动脉粥样硬化),IV(动脉瘤),V(a)(纤维)和V(b) )(钙化)病变。光谱强度和与时间有关的参数[平均寿命tau(f);衰变常数:从冠状动脉样品的时间分辨光谱得出的tau(1)(快速),tau(2)(慢速),A(1)(快速幅度贡献)]用于组织表征。我们确定,在较长波长(> 430 nm)处的一些强度值和在峰值发射区(390 nm)处的时间相关参数可区分所有类型的动脉样本,除了正常壁和I型病变之间。可以根据时间相关的参数(寿命和快速衰变)将富含脂质的病变(更不稳定)与纤维病变(更稳定)区分开。我们推断,脂质荧光特征反映在富含脂质的病变发射上。我们的结果表明,时间分辨谱的分析可用于增强对不同等级的动脉粥样硬化病变的区分,并提供区分富含脂质和纤维性病变的手段。

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