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Dynamic cone beam X-ray luminescence computed tomography with principal component analysis

机译:动态锥梁X射线发光与主成分分析的计算机断层扫描

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Cone beam X-ray luminescence computed tomography (CB-XLCT) has recently been proposed as a new molecular imaging modality for various biomedical applications. It utilizes X-ray excitable nanophosphors to produce visible or near-infrared (NIR) luminescence and combines the high sensitivity of optical imaging with the high spatial resolution of X-ray imaging. With the development of the nanophosphors and reconstruction methods, dynamic XLCT imaging, which can reflect the dynamic course of absorption, distribution, and elimination of the nanophosphors in vivo, has demonstrated its initial prospect in biological and biochemical studies. However, challenges remain in resolving nanophosphors (drug) distributions inside the imaging object due to the high light scattering and complex dynamics of nanophosphor's delivery. Considering that target with different functions may have different kinetic behaviors, in this paper we present a method to resolve targets with different kinetics by utilizing principal component analysis (PCA). The metabolic processes of nanophosphors (Y_2O_3:Eu~(3+)) of two targets were simulated and imaged using a CB-XLCT system, with two targets located at different edge-to-edge distances of 0.12 cm. Simulation and experiment studies validate the performance of the proposed algorithm. The results suggest that two adjacent targets of different kinetic behaviors can be extracted and illustrated by the proposed method, at an edge-to-edge distance of 0.12 cm.
机译:最近提出了锥形光束X射线发光计算断层扫描(CB-XLCT)作为各种生物医学应用的新分子成像模型。它利用X射线激发纳米膦酰源以产生可见光或近红外(NIR)发光,并结合光学成像与X射线成像的高空间分辨率的高灵敏度。随着纳米膦群和重建方法的发展,动态XLCT成像,可以反映体内体内纳米膦的吸收,分布和消除动力学过程,已经证明了其在生物化学和生物化学研究中的初步前景。然而,由于纳米磷的递送的高光散射和复杂的动态,挑战在成像对象内的纳米膦(药物)分布中仍然存在。考虑到具有不同功能的目标可以具有不同的动力学行为,本文我们介绍了一种通过利用主成分分析(PCA)来解决不同动力学的目标的方法。使用CB-XLCT系统模拟和成像两种靶标的代谢过程(Y_2O_3:Eu〜(3+)),两个靶位于0.12cm的不同边缘距离。仿真和实验研究验证了所提出的算法的性能。结果表明,可以通过所提出的方法在0.12cm的边缘到边缘距离处提取和示出不同动力学行为的两个相邻目标。

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