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基于简化球谐方程的激发分辨荧光层析成像

Excitation-resolved fluorescence tomography with simplified spherical harmonics equations.

机构信息

Department of Radiology, Columbia University Medical Center, New York, NY 10032, USA.

出版信息

Phys Med Biol. 2011 Mar 7;56(5):1443-69. doi: 10.1088/0031-9155/56/5/015. Epub 2011 Feb 15.

Abstract

Fluorescence tomography (FT) reconstructs the three-dimensional (3D) fluorescent reporter probe distribution inside biological tissue. These probes target molecules of biological function, e.g. cell surface receptors or enzymes, and emit fluorescence light upon illumination with an external light source. The fluorescence light is detected on the tissue surface and a source reconstruction algorithm based on the simplified spherical harmonics (SP(N)) equations calculates the unknown 3D probe distribution inside tissue. While current FT approaches require multiple external sources at a defined wavelength range, the proposed FT method uses only a white light source with tunable wavelength selection for fluorescence stimulation and further exploits the spectral dependence of tissue absorption for the purpose of 3D tomographic reconstruction. We will show the feasibility of the proposed hyperspectral excitation-resolved fluorescence tomography method with experimental data. In addition, we will demonstrate the performance and limitations of such a method under ideal and controlled conditions by means of a digital mouse model and synthetic measurement data. Moreover, we will address issues regarding the required amount of wavelength intervals for fluorescent source reconstruction. We will explore the impact of assumed spatially uniform and nonuniform optical parameter maps on the accuracy of the fluorescence source reconstruction. Last, we propose a spectral re-scaling method for overcoming the observed limitations in reconstructing accurate source distributions in optically non-uniform tissue when assuming only uniform optical property maps for the source reconstruction process.

摘要

荧光层析成像(FT)重建生物组织内三维(3D)荧光报告探针的分布。这些探针针对生物功能的分子,例如细胞表面受体或酶,并在外部光源照射下发出荧光。荧光光在组织表面被检测到,基于简化的球谐(SP(N))方程的源重建算法计算组织内未知的 3D 探针分布。虽然当前的 FT 方法需要在定义的波长范围内使用多个外部光源,但所提出的 FT 方法仅使用具有可调波长选择的白光光源进行荧光刺激,并进一步利用组织吸收的光谱依赖性来进行 3D 层析重建。我们将用实验数据展示所提出的高光谱激发分辨荧光层析成像方法的可行性。此外,我们将通过数字小鼠模型和合成测量数据,在理想和受控条件下演示这种方法的性能和局限性。此外,我们将解决荧光源重建所需的波长间隔数量的问题。我们将探讨假设空间均匀和非均匀光学参数图对荧光源重建准确性的影响。最后,我们提出了一种光谱重新缩放方法,用于克服在假设源重建过程中仅使用均匀光学属性图时,在非均匀光学组织中重建准确源分布的观察到的限制。

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