Preclinical dosimetric studies of 177Lu‐scFvD2B and comparison with 177Lu‐PSMA‐617 and 177Lu‐iPSMA endoradiotherapeutic agents

体内分布 核医学 放射免疫疗法 剂量学 多塔 放射性核素治疗 内化 吸收剂量 结合 LNCaP公司 放射化学 内部剂量学 医学 化学 前列腺癌 癌症 螯合作用 抗体 体外 内科学 受体 数学分析 生物化学 数学 有机化学 单克隆抗体 免疫学
作者
Laura Meléndez‐Alafort,Guillermina Ferro‐Flores,Clara Santos‐Cuevas,Blanca Ocampo‐García,Sofia Turato,Giulio Fracasso,Cristina Bolzati,Antonio Rosato,L. De Nardo
出处
期刊:Medical Physics [Wiley]
卷期号:48 (7): 4064-4074 被引量:4
标识
DOI:10.1002/mp.14936
摘要

Purpose Internal dosimetry has become a very important tool to evaluate the risks and benefits of new endoradiotherapeutic agents. Nowadays, some of the most successful targeted radionuclide therapy (TRT) agents are 177 Lu‐DOTA conjugates based on low molecular weight (LMW) Glu‐ureido PSMA inhibitors. It has, however, been demonstrated that the DOTA chelating moiety reduces the internalization of the LMW‐PSMA agent and its radiation dose to the tumor. Previously, we reported that 177 Lu‐scFvD2B, an antibody‐based construct, demonstrated statistically significant higher cell uptake and internalization in LNCaP prostate cancer (PCa) cells (PSMA‐positive) when compared to the LMW‐PSMA agents, 177 Lu‐PSMA‐617 and 177 Lu‐iPSMA, two of the endoradiotherapeutic agents which currently are the most used in PCa therapy. The aim of this study is to estimate the preclinical 177 Lu‐scFvD2B organ and tumor‐absorbed doses, and to compare the values with those of 177 Lu‐PSMA‐617 and 177 Lu‐iPSMA. Methods 177 Lu‐scFvD2B, 177 Lu‐PSMA‐617, and 177 Lu‐iPSMA were prepared and their radiochemical purity determined. Biodistribution studies of each radiopharmaceutical were then carried out in healthy mice to define the main source organs (SO) and to calculate the number of disintegrations in each source organs per unit of administered activity (N SO ). Absorbed dose in the main organs were then calculated for each 177 Lu‐conjugate by means of OLINDA/EXM 2.1.1 software, using the calculated N SO for both the adult male and the mouse phantoms as program inputs. Images of mice bearing micropulmonary tumors injected with 177 Lu‐conjugates were also obtained. Tumor standardized uptake values (SUV) for the different conjugates, obtained from the 3D SPECT image reconstruction of these mice, were used as the number of disintegrations in a tumor site per unit of administered activity (N T ). The tumor‐absorbed dose was calculated using the published electron dose S‐values for sphere models with diameters ranging from 10 µm to 10 mm and considering a uniform activity distribution and tumor density equivalent to water density. Results All 177 Lu‐labeled agents were obtained in high yield (98%). Dosimetric studies carried out using mouse phantoms demonstrated that organ absorbed doses of 177 Lu‐scFvD2B were from 1.4 to 2.3 times higher than those for 177 Lu‐iPSMA and from 1.5 to 2.6 times higher than those for 177 Lu‐PSMA‐617. However, the 177 Lu‐scFvD2B values of tumor‐absorbed doses for all investigated tumor sizes were from 2.8 to 3.0 times greater than those calculated for 177 Lu‐iPSMA and 177 Lu‐PSMA‐617, respectively. Moreover, 177 Lu‐scFvD2B showed the highest tumor/kidney ratio when compared to those reported for 177 Lu‐albumin conjugates. Conclusions In this preclinical study, we demonstrated the potential of 177 Lu‐scFvD2B as a therapeutic agent for PSMA‐expressing tumors, due to its higher tumor‐absorbed dose when compared with 177 Lu‐LMW agents.

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