Department of Nuclear Medicine, Klinikum rechts der Isar, Technical University of Munich, Munich, Germany; and.
Chair for Pharmaceutical Radiochemistry, Technical University of Munich, Garching, Germany.
J Nucl Med. 2021 Aug 1;62(8):1106-1111. doi: 10.2967/jnumed.120.254516. Epub 2020 Dec 18.
Radiohybrid prostate-specific membrane antigen (rhPSMA) ligands are applicable as radiochemical twins for both diagnostic PET imaging and endoradiotherapy. On the basis of preliminary data as a diagnostic ligand, the isomer rhPSMA-7.3 is a promising candidate for potential endoradiotherapy. The aim of this preclinical evaluation was to assess the biodistribution, dosimetry, and therapeutic efficacy of F/Lu-rhPSMA-7.3 in comparison to the established therapeutic agent Lu-PSMA I&T (imaging and therapy). The biodistribution of F/Lu-rhPSMA-7.3 and Lu-PSMA I&T was determined in LNCaP tumor-bearing severe combined immunodeficiency (SCID) mice after sacrifice at defined time points up to 7 d ( = 5). Organs and tumors were dissected, percentage injected dose per gram (%ID/g) was determined, and dosimetry was calculated using OLINDA/EXM, version 1.0. The therapeutic efficacy of a single 30-MBq dose of F/Lu-rhPSMA-7.3 ( = 7) was compared with that of Lu-PSMA I&T in treatment groups ( = 7) and control groups ( = 6-7) using C4-2 tumor-bearing SCID mice by evaluating tumor growth and survival over 6 wk after treatment. The biodistribution of F/Lu-rhPSMA-7.3 revealed fast blood clearance (0.63 %ID/g at 1 h after injection), and the highest activity uptake was in the spleen and kidneys, particularly in the first hour (33.25 %ID/g and 207.6 %ID/g, respectively, at 1 h after injection), indicating a renal excretion pathway. Compared with Lu-PSMA I&T, F/Lu-rhPSMA-7.3 exhibited an initial (1 h) 2.6-fold higher tumor uptake in LNCaP xenografts and a longer retention (4.5 %ID/g vs. 0.9 %ID/g at 168 h). The tumor dose of F/Lu-rhPSMA-7.3 was substantially higher (e.g., 7.47 vs. 1.96 µGy/MBq at 200 mm) than that of Lu-PSMA I&T. In most organs, absorbed doses were higher for Lu-PSMA I&T. A significantly greater tumor size reduction was shown for a single dose of F/Lu-rhPSMA-7.3 than for Lu-PSMA I&T at the end of the experiment ( = 0.0167). At the predefined termination of the experiment at 6 wk, 7 of 7 and 3 of 7 mice were still alive in the F/Lu-rhPSMA-7.3 and Lu-PSMA I&T groups, respectively, compared with the respective control groups, with 0 of 7 and 0 of 6 mice. Compared with Lu-PSMA I&T, F/Lu-rhPSMA-7.3 can be considered a suitable candidate for clinical translation because it has similar clearance kinetics and a similar radiation dose to healthy organs but superior tumor uptake and retention. Preliminary treatment experiments showed a favorable antitumor response.
放射性杂交前列腺特异性膜抗原(rhPSMA)配体可用作正电子发射断层扫描(PET)成像和放射性核素内照射治疗的化学双胞胎。基于作为诊断配体的初步数据,异构体 rhPSMA-7.3 是潜在放射性核素内照射治疗的有前途的候选物。本临床前评估的目的是评估 F/Lu-rhPSMA-7.3 与已建立的治疗剂 Lu-PSMA I&T(成像和治疗)相比的生物分布、剂量学和治疗效果。 在牺牲后,在 7 天(= 5)的时间点内,确定 F/Lu-rhPSMA-7.3 和 Lu-PSMA I&T 在 LNCaP 荷瘤严重联合免疫缺陷(SCID)小鼠中的生物分布。 解剖器官和肿瘤,测定每克注射剂量的百分比(%ID/g),并用 OLINDA/EXM 版本 1.0 计算剂量学。 比较了 F/Lu-rhPSMA-7.3(= 7)和 Lu-PSMA I&T(= 7)单次 30-MBq 剂量的治疗效果,以及使用 C4-2 荷瘤 SCID 小鼠,通过在治疗后 6 周内评估肿瘤生长和存活情况。 F/Lu-rhPSMA-7.3 的生物分布显示出快速的血液清除(注射后 1 小时为 0.63%ID/g),最高的活性摄取发生在脾脏和肾脏中,尤其是在第一个小时(注射后 1 小时分别为 33.25%ID/g 和 207.6%ID/g),表明存在肾脏排泄途径。 与 Lu-PSMA I&T 相比,F/Lu-rhPSMA-7.3 在 LNCaP 异种移植瘤中具有初始(1 小时)高 2.6 倍的肿瘤摄取和更长的保留时间(168 小时时为 4.5%ID/g 与 0.9%ID/g)。 F/Lu-rhPSMA-7.3 的肿瘤剂量明显高于 Lu-PSMA I&T(例如,200 mm 时为 7.47 与 1.96 µGy/MBq)。 在大多数器官中,Lu-PSMA I&T 的吸收剂量更高。 在实验结束时,F/Lu-rhPSMA-7.3 的肿瘤体积缩小明显大于 Lu-PSMA I&T(= 0.0167)。 在实验结束时(= 0.0167),与各自的对照组相比,F/Lu-rhPSMA-7.3 和 Lu-PSMA I&T 组的 7/7 和 3/7 只小鼠仍然存活,而对照组的 7/7 和 6/6 只小鼠仍然存活。 与 Lu-PSMA I&T 相比,F/Lu-rhPSMA-7.3 可被认为是一种适合临床转化的候选物,因为它具有相似的清除动力学和对健康器官的相似辐射剂量,但具有更高的肿瘤摄取和保留。初步治疗实验显示出良好的抗肿瘤反应。
