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首页> 外文期刊>Investigative ophthalmology & visual science >Quantitative analysis of fluorescence lifetime measurements of the macula using the fluorescence lifetime imaging ophthalmoscope in healthy subjects
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Quantitative analysis of fluorescence lifetime measurements of the macula using the fluorescence lifetime imaging ophthalmoscope in healthy subjects

机译:使用荧光寿命成像检眼镜在健康受试者中对黄斑的荧光寿命进行定量分析

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Purpose. Fundus autofluorescence (FAF) cannot only be characterized by the intensity or the emission spectrum, but also by its lifetime. As the lifetime of a fluorescent molecule is sensitive to its local microenvironment, this technique may provide more information than fundus autofluorescence imaging. We report here the characteristics and repeatability of FAF lifetime measurements of the human macula using a new fluorescence lifetime imaging ophthalmoscope (FLIO). Methods. A total of 31 healthy phakic subjects were included in this study with an age range from 22 to 61 years. For image acquisition, a fluorescence lifetime ophthalmoscope based on a Heidelberg Engineering Spectralis system was used. Fluorescence lifetime maps of the retina were recorded in a short- (498-560 nm) and a long- (560-720 nm) spectral channel. For quantification of fluorescence lifetimes a standard ETDRS grid was used. Results. Mean fluorescence lifetimes were shortest in the fovea, with 208 picoseconds for the short-spectral channel and 239 picoseconds for the long-spectral channel, respectively. Fluorescence lifetimes increased from the central area to the outer ring of the ETDRS grid. The test-retest reliability of FLIO was very high for all ETDRS areas (Spearman's ρ = 0.80 for the short- and 0.97 for the long-spectral channel, P < 0.0001). Fluorescence lifetimes increased with age. ConclusionS. The FLIO allows reproducible measurements of fluorescence lifetimes of the macula in healthy subjects. By using a custom-built software, we were able to quantify fluorescence lifetimes within the ETDRS grid. Establishing a clinically accessible standard against which to measure FAF lifetimes within the retina is a prerequisite for future studies in retinal disease.
机译:目的。眼底自发荧光(FAF)不仅可以通过强度或发射光谱来表征,还可以通过其寿命来表征。由于荧光分子的寿命对其局部微环境敏感,因此该技术可能比眼底自发荧光成像提供更多的信息。我们在这里报告使用新型荧光寿命成像检眼镜(FLIO)的人类黄斑FAF寿命测量的特征和可重复性。方法。本研究共纳入31位健康晶状体受试者,年龄范围为22至61岁。为了获取图像,使用了基于海德堡工程光谱系统的荧光寿命检眼镜。在短(498-560 nm)和长(560-720 nm)光谱通道中记录视网膜的荧光寿命图。为了定量荧光寿命,使用标准的ETDRS网格。结果。中央凹的平均荧光寿命最短,短光谱通道分别为208皮秒和长光谱通道为239皮秒。从ETDRS栅格的中心区域到外环,荧光寿命增加。在所有ETDRS区域,FLIO的重测可靠性非常高(对于短光谱通道,Spearmanρ= 0.80;对于长光谱通道,Spearmanρ= 0.97,P <0.0001)。荧光寿命随年龄增长。结论FLIO允许对健康受试者中黄斑的荧光寿命进行可重复的测量。通过使用定制软件,我们能够量化ETDRS网格内的荧光寿命。建立可衡量视网膜内FAF寿命的临床可及标准是未来视网膜疾病研究的前提。

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