放射性核素治疗骨转移的潜在药物- Lu-177-EDTMP的药代动力学和剂量学特性计算

A. V. Matveev, V. Petriev, V. Tishchenko, N. G. Minaeva
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摘要

用β -放射核素标记膦酸是一种很有前途的用于骨转移姑息治疗的放射性药物。目前,正在研究一种新的促骨化合物N,N,N ',N ' -乙二胺四基(亚甲基膦酸)与镥-177 (177Lu-EDTMP)的可能性。本研究的目的是建立177Lu标记的促骨药物在实验动物体内动力学的隔室数学模型,并在此基础上计算其药代动力学和剂量学特性。为了评估177Lu-EDTMP在体内的稳定性,我们还研究了游离镥以177LuCl3形式的分布特征。为了确定模型参数和计算放射性药物的特性,我们使用了177Lu-EDTMP和177LuCl3在完整Wistar大鼠体内生物分布的定量数据。建立了动力学的室室模型,并提出了两种确定其输运常数的方法-通过残差泛函和使用单指数函数近似。根据药代动力学模型,发现177Lu-EDTMP在骨组织中沉积(高达给药剂量的55%)。177Lu-EDTMP的表观分布体积的计算值约为血浆体积的200倍,骨组织的生物半衰期比内脏高10-20倍。177Lu-EDTMP主要通过肾脏清除排出体外。与177LuCl3的比较模型显示,177Lu-EDTMP在体内具有较高的耐药性。吸收剂量的最大值在骨骼和肾脏中形成,对其他内脏和血液的辐射负荷最小。本研究结果为177Lu-EDTMP的进一步研究和临床应用于骨骼转移瘤的治疗提供了前景。
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Calculation of pharmacokinetic and dosimetric characteristics of Lu-177-EDTMP – a potential drug for radionuclide therapy of bone metastases
Phosphonic acids labeled with beta-emitting radionuclides are promising radiopharmaceutical drugs for palliative therapy of bone metastases. Currently, the possibility of using a new osteotropic compound N,N,N’,N’-ethylenediaminetetrakis (methylene phosphonic acid) with lutetium-177 (177Lu-EDTMP) is being studied. The aim of the work is to develop a compartment mathematical model of the kinetics of 177Lu labeled osteotropic radiopharmaceutical drugs in the body of laboratory animals and calculate their pharmacokinetic and dosimetric characteristics based on it. To assess the stability of 177Lu-EDTMP in vivo, the characteristics of the distribution of free lutetium in the form of 177LuCl3 were also studied. To identify the model parameters and calculate the characteristics of radiopharmaceutical drugs, quantitative data on the bio-distribution of 177Lu-EDTMP and 177LuCl3 in the body of intact Wistar rats were used. A compartment model of kinetics has been developed and two approaches to the identification of its transport constants have been proposed – through the residual functional and using approximation by monoexponential functions. According to pharmacokinetic modeling, it was found that 177Lu-EDTMP is deposited in bone tissues (up to 55% of the administered dose). The calculated value of the apparent volume of distribution of 177Lu-EDTMP is approximately 200 times greater than the volume of blood plasma, the values of biological half-lives from bone tissues are 10-20 times higher than from internal organs. The excretion of 177Lu-EDTMP from the body occurs mainly through renal clearance. Comparative modeling with 177LuCl3 revealed high resistance of 177Lu-EDTMP in vivo. The highest values of absorbed doses are formed in the skeleton and kidneys with minimal radiation load on other internal organs and blood. The results obtained indicate the prospects for further studies of 177Lu-EDTMP and the possibility of its clinical application for the treatment of skeletal metastases.
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