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首页> 外文期刊>Medical Physics >Technical Note: Simplified and practical pretherapy tumor dosimetry - A feasibility study for I-131-MIBG therapy of neuroblastoma using I-124-MIBG PET/CT
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Technical Note: Simplified and practical pretherapy tumor dosimetry - A feasibility study for I-131-MIBG therapy of neuroblastoma using I-124-MIBG PET/CT

机译:技术说明:简化实用的前颈肿瘤剂量术 - 使用I-124-MIBG PET / CT的神经母细胞瘤I-131-MIBG治疗的可行性研究

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Purpose Radiation dose calculated on tumors for radiopharmaceutical therapy varies significantly from tumor to tumor and from patient to patient. Accurate estimation of radiation dose requires multiple time point measurements using radionuclide imaging modalities such as SPECT or PET. In this report, we show our technical development of reducing the number of scans needed for reasonable estimation of tumor and normal organ dose in our pretherapy imaging and dosimetry platform of I-124-metaiodobenzylguanidine (MIBG) positron emission tomography/computed tomography (PET/CT) for I-131-MIBG therapy of neuroblastoma. Methods We analyzed the simplest kinetic data, areas of two-time point data for five patients with neuroblastoma who underwent 3 or 4 times of I-124-MIBG PET/CT scan prior to I-131-MIBG therapy. The data for which we derived areas were percent of injected activity (%IA) and standardized uptake value of tumors. These areas were correlated with time-integrated activity coefficients (TIACs) from full data (3 or 4 time points). TIACs are direct correlates with radiation dose as long as the volume and the radionuclide are known. Results The areas of %IAs between data obtained from all the two-time points with time points 1 and 2 (day 0 and day 1), time points 2 and 3 (day 1 and day 2), and time points 1 and 3 (day 0 and day 2) showed reasonable correlation (Pearson's correlation coefficient |r| > 0.5) with not only tumor and organ TIACs but also tumor and organ absorbed doses. The tumor and organ doses calculated using %IA areas of time point 1 and time point 2 were our best fits at about 20% individual percent difference compared to doses calculated using 3 or 4 time points. Conclusions We could achieve reasonable accuracy of estimating tumor doses for subsequent radiopharmaceutical therapy using only the two-time point imaging sessions. Images obtained from these time points (within the 48-h after administration of radiopharmaceutical) were also viewed as useful for diagnostic reading. Although our analysis was specific to I-124-MIBG PET/CT pretherapy imaging data for I-131-MIBG therapy of neuroblastoma and the number of imaging datasets was not large, this feasible methodology would generally be applicable to other imaging and therapeutic radionuclides with an appropriate data analysis similar to our analysis to other imaging and therapeutic radiopharmaceuticals. (c) 2019 American Association of Physicists in Medicine
机译:针对放射性药物疗法的肿瘤计算的目的辐射剂量从肿瘤与肿瘤和患者的肿瘤显着不同。准确估计辐射剂量需要使用诸如SPECT或PET的放射性核素成像模态进行多次测量。在本报告中,我们展示了我们在我们的前颈部成像和I-124-碘苯苄基胍(MIBG)正电子发射断层扫描/计算断层扫描/计算断层扫描/计算机断层扫描/计算机断层扫描/计算机断层扫描/计算断层扫描/计算机断层扫描/计算机断层扫描/计算断层扫描(PET / CT)对于神经母细胞瘤的I-131-MIBG治疗。方法分析了最简单的动力学数据,对于在I-131-MIBG治疗之前,在I-124-MIBG PET / CT扫描中进行3或4次的神经母细胞瘤的五名患者的两次点数据。我们所衍生的区域的数据是注射活性(%IA)的百分比和标准化的肿瘤摄取值。这些区域与来自全数据(3或4个时间点)的时间综合活性系数(TIACS)相关。由于体积和放射性核素是已知的,Tiacs与辐射剂量直接相关。结果从带时间点1和2(日0和第1天),时间点2和3(第1天和第2天),时间点1和3(第0天和第2天)显示出合理的相关性(Pearson的相关系数| R | 0.5),不仅具有肿瘤和器官菌,而且还具有肿瘤和器官吸收剂量。使用%IA时间点1和时间点2计算的肿瘤和器官剂量是我们最佳拟合,与使用3或4个时间点计算的剂量相比,百分比差异约20%。结论我们可以达到估算肿瘤剂量的合理准确性,以便仅使用双重点成像疗程进行后续放射性药物治疗。还观察到从这些时间点获得的图像(在给药后给药后的48小时内)可用于诊断读数。虽然我们的分析特定于I-124-MIBG PET / CT PROFERACE成像数据,但对于神经母细胞瘤的I-131-MIBG治疗,但成像数据集的数量不大,但这种可行的方法通常适用于其他成像和治疗放射性核素适当的数据分析与我们对其他成像和治疗放射性药物的分析类似。 (c)2019年美国物理学家协会

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