Stanford University, Byers Eye Institute, Palo Alto, California, United States.
University of Rochester, Center for Visual Science, Rochester, New York, United States.
J Biomed Opt. 2024 Jun;29(Suppl 2):S22707. doi: 10.1117/1.JBO.29.S2.S22707. Epub 2024 Jul 3.
Adaptive optics fluorescence lifetime ophthalmoscopy (AOFLIO) provides a label-free approach to observe functional and molecular changes at cellular scale . Adding multispectral capabilities improves interpretation of lifetime fluctuations due to individual fluorophores in the retinal pigment epithelium (RPE).
To quantify the cellular-scale changes in autofluorescence with age and eccentricity due to variations in lipofuscin, melanin, and melanolipofuscin in RPE using multispectral AOFLIO.
AOFLIO was performed on six subjects at seven eccentricities. Four imaging channels ( ) were used: 473/SSC, 473/LSC, 532/LSC, and 765/NIR. Cells were segmented and the timing signals of each pixel in a cell were combined into a single histogram, which were then used to compute the lifetime and phasor parameters. An ANOVA was performed to investigate eccentricity and spectral effects on each parameter.
A repeatability analysis revealed change in lifetime parameters in repeat visits for 532/LSC. The 765/NIR and 532/LSC had eccentricity and age effects similar to previous reports. The 473/LSC had a change in eccentricity with mean lifetime and a phasor component. Both the 473/LSC and 473/SSC had changes in eccentricity in the short lifetime component and its relative contribution. The 473/SSC had no trend in eccentricity in phasor. The comparison across the four channels showed differences in lifetime and phasor parameters.
Multispectral AOFLIO can provide a more comprehensive picture of changes with age and eccentricity. These results indicate that cell segmentation has the potential to allow investigations in low-photon scenarios such as in older or diseased subjects with the co-capture of an NIR channel (such as 765/NIR) with the desired spectral channel. This work represents the first multispectral, cellular-scale fluorescence lifetime comparison in the human RPE and may be a useful method for tracking diseases.
自适应光学荧光寿命眼底镜(AOFLIO)提供了一种无标记的方法来观察细胞尺度的功能和分子变化。增加多光谱功能可以提高对视网膜色素上皮(RPE)中单个荧光团寿命波动的解释。
使用多光谱 AOFLIO 量化由于 RPE 中脂褐素、黑色素和黑素脂褐素的变化,年龄和离轴度引起的自发荧光的细胞尺度变化。
在七个离轴度对六名受试者进行 AOFLIO。使用四个成像通道( ):473/SSC、473/LSC、532/LSC 和 765/NIR。对细胞进行分割,并将细胞中每个像素的定时信号组合成单个直方图,然后用于计算寿命和相量参数。进行方差分析以研究各参数的离轴度和光谱效应。
重复访问的重复性分析显示,532/LSC 的寿命参数变化了 。765/NIR 和 532/LSC 的离轴度和年龄效应与之前的报告相似。473/LSC 的离轴度随平均寿命和相量分量而变化。473/LSC 和 473/SSC 的短寿命分量及其相对贡献都有离轴度变化。473/SSC 的相量中没有离轴度趋势。四个通道之间的比较显示了寿命和相量参数的差异。
多光谱 AOFLIO 可以更全面地描述年龄和离轴度的变化。这些结果表明,细胞分割有可能允许在低光子情况下进行研究,例如在年龄较大或患有疾病的受试者中,同时捕获所需光谱通道的近红外通道(如 765/NIR)。这项工作代表了人类 RPE 中首次多光谱、细胞尺度荧光寿命比较,可能是跟踪疾病的有用方法。
Zotero 插件
