Whole-Body Voxel-Based Personalized Dosimetry: The Multiple Voxel S-Value Approach for Heterogeneous Media with Nonuniform Activity Distributions

被引:38
|
作者
Lee, Min Sun [1 ,2 ]
Kim, Joong Hyun [3 ]
Paeng, Jin Chul [1 ]
Kang, Keon Wook [1 ,4 ]
Jeong, Jae Min [1 ,2 ,4 ]
Lee, Dong Soo [1 ]
Lee, Jae Sung [1 ,2 ,4 ]
机构
[1] Seoul Natl Univ, Dept Nucl Med, Coll Med, 103 Daehak Ro, Seoul 03080, South Korea
[2] Seoul Natl Univ, Interdisciplinary Program Radiat Appl Life Sci, Seoul, South Korea
[3] Korea Res Inst Stand & Sci, Ctr Ionizing Radiat, 267 Gajeong Ro, Daejeon 34113, South Korea
[4] Seoul Natl Univ, Dept Biomed Sci, Coll Med, Seoul, South Korea
基金
新加坡国家研究基金会;
关键词
radiation dosimetry; Monte Carlo simulation; voxel S value; heterogeneous medium; PATIENT-SPECIFIC DOSIMETRY; MONTE-CARLO; SIMULATION TOOLKIT; INTERNAL DOSIMETRY; NUCLEAR-MEDICINE; RADIONUCLIDE THERAPY; KERNEL CONVOLUTION; DOSE KERNELS; SOFTWARE; GATE;
D O I
10.2967/jnumed.117.201095
中图分类号
R8 [特种医学]; R445 [影像诊断学];
学科分类号
1002 ; 100207 ; 1009 ;
摘要
Personalized dosimetry with high accuracy is becoming more important because of the growing interest in personalized medicine and targeted radionuclide therapy. Voxel-based dosimetry using dose point kernel or voxel S-value (VSV) convolution is available. However, these approaches do not consider the heterogeneity of the medium. Here, we propose a new method for whole-body voxel-based personalized dosimetry in heterogeneous media with nonuniform activity distributions-a method we refer to as the multiple VSV approach. Instead of using only a single VSV, as found in water, the method uses multiple numbers (N) of VSVs to cover media of various density ranges, as found in the whole body. Methods: The VSVs were precalculated using GATE Monte Carlo simulation and were convoluted with the time-integrated activity to generate density-specific dose maps. CT-based segmentation was performed to generate a binary mask image for each density region. The final dose map was acquired by the summation of N segmented density-specific dose maps. We tested several sets of VSVs with different densities: N = 1 (single water VSV), 4, 6, 8, 10, and 20. To validate the proposed method, phantom and patient studies were conducted and compared with the direct Monte Carlo approach, which was considered the ground truth. Finally, dosimetry on 10 patients was performed using the multiple VSV approach and compared with the single VSV and organ-based approaches. Errors at the voxel and organ levels were reported for 8 organs. Results: In the phantom and patient studies, the multiple VSV approach showed significant decreases in voxel-level errors, especially for the lung and bone regions. As the number of VSVs increased, voxel-level errors decreased, although some overestimations were observed at the lung boundaries. For the multiple VSVs (N 5 8), we achieved a voxel-level error of 2.06%. In the dosimetry study, our proposed method showed greatly improved results compared with single VSV and organ-based dosimetry. Errors at the organ level were -6.71%, 2.17%, and 227.46% for single VSV, multiple VSV, and organ-based dosimetry, respectively. Conclusion: The multiple VSV approach for heterogeneous media with nonuniform activity distributions offers fast personalized dosimetry at the whole-body level, yielding results comparable to those of the direct Monte Carlo approach.
引用
收藏
页码:1133 / 1139
页数:7
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