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体内荧光成像:光栅扫描点源成像比宽光束几何结构提供更准确的定量分析。

Fluorescence imaging in vivo: raster scanned point-source imaging provides more accurate quantification than broad beam geometries.

作者信息

Pogue Brian W, Gibbs Summer L, Chen Bin, Savellano Mark

机构信息

Thayer School of Engineering, Dartmouth College, Hanover NH 03755, USA.

出版信息

Technol Cancer Res Treat. 2004 Feb;3(1):15-21. doi: 10.1177/153303460400300102.

Abstract

Two fluorescence imaging systems were compared for their ability to quantify mean fluorescence intensity from surface-weighted imaging of tissue. A broad beam CCD camera system was compared to a point sampling system that raster scans to create the image. The effects of absorption and scattering in the background tissue volume were shown to be similar in their effect upon the signal, but the effect of the three-dimensional shape of the tissue was shown to be a significant distortion upon the signal. Spherical phantoms with Intralipid and blood for absorber and scatterer were used with a fixed concentration of aluminum phthalocyanine fluorophore to illustrate that the mean intensity observed with the broad beam system increased with size, while the mean intensity observed with the raster scanned system was not as significantly affected. Similar results were observed in vivo with mice injected with the fluorophore and imaged multiple times to observe the pharmacokinetics of the drug. The fluorescence in the tumor observed with the broad beam system was higher than that observed with the raster scanned system. Based upon the phantom and animal observations in this study, it should be concluded that using broad beam fluorescence imaging systems to quantify fluorescence in vivo may be problematic when comparing tissues with different three dimensional characteristics. In particular, the ratio of fluorescence from tumor to normal tissue can yield inaccurate results when the tumor is large. However, similar measurements with a narrow beam system that is raster scanned to create the images are not as significantly affected by the three dimensional shape of the tissue. Raster scanned imaging appears to provide a more uniform and accurate way to quantify fluorescence signals from distributed tissues in vivo.

摘要

对两种荧光成像系统进行了比较,以评估它们从组织表面加权成像中量化平均荧光强度的能力。将宽光束电荷耦合器件(CCD)相机系统与通过光栅扫描来创建图像的点采样系统进行了比较。结果表明,背景组织体积中的吸收和散射对信号的影响相似,但组织三维形状的影响对信号造成了显著失真。使用含有作为吸收体和散射体的脂类乳剂和血液的球形模型,以及固定浓度的铝酞菁荧光团,以说明宽光束系统观察到的平均强度随尺寸增加,而光栅扫描系统观察到的平均强度受影响不那么显著。在给小鼠注射荧光团并多次成像以观察药物药代动力学的体内实验中也观察到了类似结果。宽光束系统观察到的肿瘤中的荧光高于光栅扫描系统观察到的荧光。基于本研究中的模型和动物观察结果,应该得出结论,当比较具有不同三维特征的组织时,使用宽光束荧光成像系统在体内量化荧光可能存在问题。特别是,当肿瘤较大时,肿瘤与正常组织的荧光比值可能会产生不准确的结果。然而,通过光栅扫描来创建图像的窄光束系统进行的类似测量受组织三维形状的影响不那么显著。光栅扫描成像似乎为在体内量化来自分布式组织的荧光信号提供了一种更均匀、准确的方法。

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