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首页> 外文期刊>Medical Physics >In vivo bioluminescence tomography with a blocking-off finite-difference SP3 method and MRI/CT coregistration.
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In vivo bioluminescence tomography with a blocking-off finite-difference SP3 method and MRI/CT coregistration.

机译:体内生物发光层析成像,采用有限差分SP3方法和MRI / CT配准。

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摘要

PURPOSE: Bioluminescence imaging is a research tool for studying gene expression levels in small animal models of human disease. Bioluminescence light, however, is strongly scattered in biological tissue and no direct image of the light-emitting reporter probe's location can be obtained. Therefore, the authors have developed a linear image reconstruction method for bioluminescence tomography (BLT) that recovers the three-dimensional spatial bioluminescent source distribution in small animals. METHODS: The proposed reconstruction method uses third-order simplified spherical harmonics (SP3) solutions to the equation of radiative transfer for modeling the bioluminescence light propagation in optically nonuniform tissue. The SP3 equations and boundary conditions are solved with a finite-difference (FD) technique on a regular grid. The curved geometry of the animal surface was taken into account with a blocking-off region method for regular grids. Coregistered computed tomography (CT) and magnetic resonance (MR) images provide information regarding the geometry of the skin surface and internal organs. The inverse source problem is defined as an algebraic system of linear equations for the unknown source distribution and is iteratively solved given multiview and multispectral boundary measurements. The average tissue absorption parameters, which are used for the image reconstruction process, were calculated with an evolution strategy (ES) from in vivo measurements using an implanted pointlike source of known location and spectrum. Moreover, anatomical information regarding the location of the internal organs and other tissue structures within the animal's body are provided by coregistered MR images. RESULTS: First, the authors recovered the wavelength-dependent absorption coefficients (average error of 14%) with the ES under ideal conditions by using a numerical mouse model. Next, they reconstructed the average absorption coefficient of a small animal by using an artificial implanted light source and the validated ES. Last, they conducted two in vivo animal experiments and recovered the spatial location of the implanted light source and the spatial distribution of a bioluminescent reporter system located in the kidneys. The source reconstruction results were coregistered to CT and MR images. They further found that accurate bioluminescence image reconstructions could be obtained when segmenting a voidlike cyst with low-scattering and absorption parameters, whereas inaccurate image reconstructions were obtained when assuming a uniform optical parameter distribution instead. The image reconstructions were completed within 23 min on a 3 GHz Intel processor. CONCLUSIONS: The authors demonstrated on in vivo examples that the combination of anatomical coregistration, accurate optical tissue properties, multispectral acquisition, and a blocking-off FD-SP3 solution of the radiative transfer model significantly improves the accuracy of the BLT reconstructions.
机译:目的:生物发光成像是研究人类疾病小动物模型中基因表达水平的研究工具。然而,生物发光光在生物组织中强烈散射,因此无法获得发光报告探针位置的直接图像。因此,作者开发了一种用于生物发光层析成像(BLT)的线性图像重建方法,该方法可恢复小型动物的三维空间生物发光源分布。方法:拟议的重建方法对辐射传递方程使用三阶简化球谐函数(SP3)解,以对生物发光在光学不均匀组织中的传播进行建模。 SP3方程和边界条件通过规则网格上的有限差分(FD)技术求解。对于常规栅格,使用遮挡区域方法考虑了动物表面的弯曲几何形状。配准的计算机断层扫描(CT)和磁共振(MR)图像可提供有关皮肤表面和内部器官的几何形状的信息。逆源问题定义为未知源分布的线性方程组的代数系统,在给定多视图和多光谱边界测量的情况下可以迭代求解。用于图像重建过程的平均组织吸收参数是使用进化策略(ES)通过植入已知位置和光谱的点状源体内测量得到的。此外,关于动物体内的内部器官和其他组织结构的位置的解剖学信息是通过共同配准的MR图像提供的。结果:首先,作者通过使用数字鼠标模型在理想条件下用ES恢复了波长相关的吸收系数(平均误差为14%)。接下来,他们通过使用人工植入的光源和经过验证的ES重建了小动物的平均吸收系数。最后,他们进行了两次体内动物实验,并恢复了植入光源的空间位置以及位于肾脏中的生物发光报告系统的空间分布。源重建结果被共配准到CT和MR图像。他们进一步发现,当以低散射和吸收参数分割空洞状囊肿时,可以获得准确的生物发光图像重建,而当假设均匀的光学参数分布时,将获得不准确的图像重建。在3 GHz Intel处理器上,图像重建在23分钟内完成。结论:作者在体内实例中证明,解剖学上的一致性,准确的光学组织特性,多光谱采集以及辐射转移模型的FD-SP3解决方案的组合显着提高了BLT重建的准确性。

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