基于图像的病变和肾脏剂量测定方案在有或无延迟SPECT/CT采集的Lu-PSMA-I&T治疗中的研究。
Investigation of image-based lesion and kidney dosimetry protocols for Lu-PSMA-I&T therapy with and without a late SPECT/CT acquisition.
作者信息
Resch Sandra, Takayama Fouladgar Sarah, Zacherl Mathias, Sheikh Gabriel T, Liubchenko Grigory, Rumiantcev Mikhail, Unterrainer Lena M, Wenter Vera, Bartenstein Peter, Ziegler Sibylle I, Ilhan Harun, Beyer Leonie, Böning Guido, Delker Astrid
机构信息
Department of Nuclear Medicine, University Hospital, LMU Munich, Munich, Germany.
出版信息
EJNMMI Phys. 2023 Feb 9;10(1):11. doi: 10.1186/s40658-023-00529-8.
BACKGROUND
Lu-PSMA therapy has been successfully used to prolong the survival of patients with metastatic castration-resistant prostate cancer. Patient-specific dosimetry based on serial quantitative SPECT/CT imaging can support the understanding of dose-effect relationships. However, multiple SPECT/CT measurements can be challenging for patients, which motivates the investigation of efficient sampling schedules and their impact on dosimetry. In this study, different time samplings with respect to the number and timing of SPECT/CT acquisitions with and without a late measurement were investigated.
MATERIALS AND METHODS
In total, 43 lesions and 10 kidneys of 5 patients receiving Lu-PSMA-I&T therapy were investigated. Whole-body SPECT/CT measurements were performed at 1, 2, 3 and 7 days post-injection. For both lesions (isocontour-based segmentation) and kidneys (CT-based segmentation), a reference model was employed including all four time points. To identify the best-matching fit function out of a pre-defined set of models, visual inspection, coefficients of variation and sum of squared errors were considered as goodness-of-fit criteria. Biologically effective doses (BEDs) calculated with different time samplings (days 1, 2, 3/1, 2, 7/1, 3, 7/2, 3, 7 and 1, 2/1, 3/1, 7) were compared to the reference.
RESULTS
The best-fit function was found to be a mono-exponential model for lesions and a bi-exponential model with a population-based parameter and two free parameters for kidneys. The BEDs calculated with the time sampling 1, 3, 7 days showed the lowest deviations from the reference for lesions with 4 ± 5%. Without day 7, still 86% of all lesions showed deviations from the reference < 10%. The outlier deviations showed a positive correlation with the effective half-life of the respective lesions. For kidneys, including days 1, 2, 3 achieved the best results with 0 ± 1%. Generally, deviations for kidneys were found to be small for all time samplings (max. 13%).
CONCLUSIONS
For combined optimization of the SPECT/CT time sampling for kidney and lesion dosimetry during Lu-PSMA-I&T therapy, the sampling with days 1, 3, 7 showed the smallest deviation from the reference. Without a late acquisition, using the schedule with days 1, 2, 3 is likewise feasible.
背景
镥-前列腺特异性膜抗原(Lu-PSMA)疗法已成功用于延长转移性去势抵抗性前列腺癌患者的生存期。基于系列定量单光子发射计算机断层扫描/计算机断层扫描(SPECT/CT)成像的个体化剂量测定有助于理解剂量效应关系。然而,多次SPECT/CT测量对患者来说可能具有挑战性,这促使人们研究有效的采样方案及其对剂量测定的影响。在本研究中,针对有无晚期测量情况下SPECT/CT采集的次数和时间进行了不同的时间采样研究。
材料与方法
共研究了5例接受Lu-PSMA-碘代托品酸盐(I&T)治疗患者的43个病灶和10个肾脏。在注射后1、2、3和7天进行全身SPECT/CT测量。对于病灶(基于等轮廓分割)和肾脏(基于CT分割),采用包含所有四个时间点的参考模型。为了从预定义的一组模型中识别最佳拟合函数,将目视检查、变异系数和平方误差总和作为拟合优度标准。比较了不同时间采样(第1、2、3天/第1、2、7天/第1、3、7天/第2、3、7天以及第1、2天/第1、3天/第1、7天)计算的生物等效剂量(BED)与参考值。
结果
发现病灶的最佳拟合函数为单指数模型,肾脏的最佳拟合函数为具有群体参数和两个自由参数的双指数模型。对于病灶,采用第1、3、7天时间采样计算的BED与参考值的偏差最小,为4±5%。不包括第7天,所有病灶中仍有86%的偏差<10%。异常值偏差与各个病灶的有效半衰期呈正相关。对于肾脏,采用第1、2、3天的时间采样效果最佳,偏差为0±1%。一般来说,所有时间采样的肾脏偏差都较小(最大为13%)。
结论
在Lu-PSMA-I&T治疗期间,为了联合优化肾脏和病灶剂量测定的SPECT/CT时间采样,采用第1、3、7天的采样与参考值的偏差最小。如果没有晚期采集,采用第1、2、3天的方案同样可行。
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