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Treatment planning in PRRT based on simulated PET data and a PBPK model

机译:基于模拟PET数据和PBPK模型的PRRT治疗计划

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摘要

Aim: To investigate the accuracy of treatment planning in peptide-receptor radionuclide therapy (PRRT) based on simulated PET data (using a PET noise model) and a physiologically based pharmacokinetic (PBPK) model. Methods: The parameters of a PBPK model were fitted to the biokinetic data of 15 patients. True mathematical phantoms of patients (MPPs) were the PBPK model with the fitted parameters. PET measurements after bolus injection of 150 MBq Ga-68-DOTATATE were simulated for the true MPPs. PET noise with typical noise levels was added to the data (i.e. c=0.3 [low], 3, 30 and 300 [high]). Organ activity data in the kidneys, tumour, liver and spleen were simulated at 0.5, 1 and 4 h p.i. PBPK model parameters were fitted to the simulated noisy PET data to derive the PET-predicted MPPs. Therapy was simulated assuming an infusion of 3.3 GBq of Y-90-DOTATATE over 30 min. Time-integrated activity coefficients (TIACs) of simulated therapy in tumour, kidneys, liver, spleen and remainder were calculated from both, true MPPs (true TIACs) and predicted MPPs (predicted TIACs). Variability v between true TIACs and predicted TIACs were calculated and analysed. Variability <= 10% was considered to be an accurate prediction. Results: For all noise level, variabilities for the kidneys, liver, and spleen showed an accurate prediction for TIACs, e.g. c=300: v(kidney)=(5 +/- 2)%, v(liver)= 5 +/- 2)%, V-spleen = (4 +/- 2)%. However, tumour TIAC predictions were not accurate for all noise levels, e.g. c=0.3: v(tumour) = (8 +/- 5)%. Conclusion: PET- based treatment planning with kidneys as the dose limiting organ seems possible for all reported noise levels using an adequate PBPK model and previous knowledge about the individual patient.
机译:目的:研究基于模拟PET数据(使用PET噪声模型)和基于生理学的药代动力学(PBPK)模型的肽受体放射性核素治疗(PRRT)治疗计划的准确性。方法:将PBPK模型的参数与15例患者的生物动力学数据进行拟合。患者的真实数学模型(MPP)是具有拟合参数的PBPK模型。在大剂量注射150 MBq Ga-68-多塔酸盐后,对真实MPP进行PET测量。将具有典型噪声级的PET噪声添加到数据中(即c=0.3[低]、3、30和300[高])。在0.5、1和4 h p.i.时模拟肾脏、肿瘤、肝脏和脾脏中的器官活动数据。将PBPK模型参数拟合到模拟的噪声PET数据中,以得出PET预测的MPP。假设在30分钟内输注3.3 GBq的Y-90-多塔酸盐,模拟治疗。根据真实MPPs(真实TIACs)和预测MPPs(预测TIACs)计算肿瘤、肾脏、肝脏、脾脏和剩余部分模拟治疗的时间积分活度系数(TIACs)。计算并分析了真实TIAC和预测TIAC之间的变异性v。变异性<=10%被认为是一个准确的预测。结果:对于所有噪声水平,肾脏、肝脏和脾脏的变异性显示出对TIAC的准确预测,例如c=300:v(肾脏)=(5+/-2%),v(肝脏)=5+/-2%,v-脾脏=(4+/-2)%。然而,肿瘤TIAC预测并非对所有噪声水平都准确,例如c=0.3:v(肿瘤)=(8+/-5)%。结论:基于PET的治疗计划,以肾脏作为剂量限制器官,似乎可以使用适当的PBPK模型和之前对个体患者的了解,对所有报告的噪声水平进行治疗。

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  • 来源
    《Nuclearmedicine》 |2017年第1期|共8页
  • 作者单位

    Heidelberg Univ Univ Med Mannheim Med Fac Mannheim Med Radiat Phys Radiat Protect Mannheim;

    Heidelberg Univ Univ Med Mannheim Med Fac Mannheim Med Radiat Phys Radiat Protect Mannheim;

    Heidelberg Univ Univ Med Mannheim Med Fac Mannheim Med Radiat Phys Radiat Protect Mannheim;

    Univ Ulm Dept Nucl Med Med Radiat Phys D-89069 Ulm Germany;

    Rhein Westfal TH Aachen Univ Hosp Klin Nukl Med Aachen Germany;

    Heidelberg Univ Univ Med Mannheim Med Fac Mannheim Med Radiat Phys Radiat Protect Mannheim;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 放射医学;
  • 关键词

    PBPK Model; PRRT; PET; PET noise model;

    机译:PBPK模型;PRRT;PET;宠物噪音模型;

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