Li Wei Bo, Höllriegl Vera, Roth Paul, Oeh Uwe
Institute of Radiation Protection, GSF-National Research Center for Environment and Health, 85746 Neuherberg, Germany.
Radiat Environ Biophys. 2008 Apr;47(2):225-39. doi: 10.1007/s00411-007-0154-8. Epub 2008 Jan 19.
The objective of the present work is to apply the plasma clearance parameters to strontium, previously determined in our laboratory, to improve the biokinetic and dosimetric models of strontium-90 ((90)Sr) used in radiological protection; and also to apply this data for the estimation of the radiation doses from strontium-89 ((89)Sr) after administration to patients for the treatment of the painful bone metastases. Plasma clearance and urinary excretion of stable strontium tracers of strontium-84 ((84)Sr) and strontium-86 ((86)Sr) were measured in GSF-National Research Center for Environment and Health (GSF) in 13 healthy German adult subjects after intravenous injection and oral administration. The biological half-life of strontium in plasma was evaluated from 49 plasma concentration data sets following intravenous injections. This value was used to determine the transfer rates from plasma to other organs and tissues. At the same time, the long-term retention of strontium in soft tissue and whole body was constrained to be consistent with measured values available. A physiological urinary path was integrated into the biokinetic model of strontium. Parameters were estimated using our own measured urinary excretion values. Retention and excretion of strontium were modeled using compartmental transfer rates published by the International Commission on Radiological Protection (ICRP), the SENES Oak Ridge Inc. (SENES), and the Urals Research Center for Radiation Medicine (TBM). The results were compared with values calculated by applying our GSF parameters (GSF). For the dose estimation of (89)Sr, a bone metastases model (GSF-M) was developed by adding a compartment, representing the metastases, into the strontium biokinetic model. The related parameters were evaluated based on measured data available in the literature. A set of biokinetic parameters was optimized to represent not only the early plasma kinetics of strontium but also the long-term retention measured in soft tissue and whole body. The ingestion dose coefficients of (90)Sr were computed and compared with different biokinetic model parameters. The ingestion dose coefficients were calculated as 2.8 x 10(-8), 2.1 x 10(-8), 2.5 x 10(-8) and 3.8 x 10(-8) Sv Bq(-1) for ICRP, SENES, TBM and GSF model parameters, respectively. Moreover, organ absorbed dose for the radiopharmaceutical of (89)Sr in bone metastases therapy was estimated based on the GSF and ICRP biokinetic model parameters. The effective doses were 3.3, 1.8 and 1.2 mSv MBq(-1) by GSF, GSF-M, and ICRP Publication 67 model parameters, respectively, compared to the value of 3.1 mSv MBq(-1) reported by ICRP Publication 80. The absorbed doses of red bone marrow and bone surface, 17 and 21 mGy MBq(-1) calculated by GSF parameters, and 7.1 and 8.8 mGy MBq(-1) by GSF-M parameters, are comparable to the clinical results of 3-19 mGy MBq(-1) for bone marrow and 16 mGy MBq(-1) for bone surface. Based on the GSF-M model, the absorbed dose of (89)Sr to metastases was estimated to be 434 mGy MBq(-1). The strontium clearance half-life of 0.25 h from the plasma obtained in the present study is obviously faster than the value of 1.1 h recommended by ICRP. There are no significant changes for ingestion dose coefficients of (90)Sr using different model parameters. A model including the metastases was particularly developed for dose estimation of (89)Sr treatment for the pain of bone metastases.
本研究的目的是将我们实验室先前测定的血浆清除参数应用于锶,以改进放射防护中使用的锶 - 90(90Sr)生物动力学和剂量学模型;并将此数据用于估算给患者施用锶 - 89(89Sr)以治疗疼痛性骨转移后产生的辐射剂量。在德国环境与健康国家研究中心(GSF)对13名健康德国成年受试者静脉注射和口服后,测量了稳定锶示踪剂锶 - 84(84Sr)和锶 - 86(86Sr)的血浆清除率和尿排泄率。根据静脉注射后的49个血浆浓度数据集评估了血浆中锶的生物半衰期。该值用于确定从血浆到其他器官和组织的转移率。同时,锶在软组织和全身的长期滞留被限制为与现有测量值一致。将生理性尿路纳入锶的生物动力学模型。使用我们自己测量的尿排泄值估算参数。使用国际放射防护委员会(ICRP)、橡树岭SENES公司(SENES)和乌拉尔辐射医学研究中心(TBM)公布的隔室转移率对锶的滞留和排泄进行建模。将结果与应用我们的GSF参数(GSF)计算的值进行比较。对于89Sr的剂量估算,通过在锶生物动力学模型中添加一个代表转移灶的隔室,建立了一个骨转移模型(GSF - M)。基于文献中可用的测量数据评估相关参数。优化了一组生物动力学参数,以不仅代表锶的早期血浆动力学,还代表在软组织和全身测量的长期滞留。计算了90Sr的摄入剂量系数,并与不同的生物动力学模型参数进行比较。对于ICRP、SENES、TBM和GSF模型参数,摄入剂量系数分别计算为2.8×10−8、2.1×10−8、2.5×10−8和3.8×10−8 Sv Bq−1。此外,基于GSF和ICRP生物动力学模型参数估算了骨转移治疗中89Sr放射性药物的器官吸收剂量。与ICRP第80号出版物报告的3.1 mSv MBq−1的值相比,GSF、GSF - M和ICRP第67号出版物模型参数的有效剂量分别为3.3、1.8和1.2 mSv MBq−1。GSF参数计算的红骨髓和骨表面的吸收剂量分别为17和21 mGy MBq−1,GSF - M参数计算的为7.1和8.
