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阿伐氟斑素 PSMA-Q 的合成、临床前评估和用于前列腺癌成像的人体首次研究。

Synthesis, preclinical evaluation, and first-in-human study of AlF-PSMA-Q for prostate cancer imaging.

机构信息

Department of Nuclear Medicine, Chinese PLA General Hospital, No. 28 Fu-Xing Rd., Beijing, 100853, China.

出版信息

Eur J Nucl Med Mol Imaging. 2022 Jul;49(8):2774-2785. doi: 10.1007/s00259-022-05775-z. Epub 2022 Apr 9.

DOI:10.1007/s00259-022-05775-z
PMID:35396969
Abstract

PURPOSE

To investigate the potential of a novel AlF-labeled PSMA-targeted radiotracer for PCa diagnosis through both preclinical and pilot clinical studies.

METHODS

AlF-PSMA-Q was prepared automatically. The binding affinity to PSMA was evaluated in vitro using the 22Rv1 (PSMA +) and PC-3 (PSMA -) cell lines. Pharmacokinetics evaluation, biodistribution study, Micro-PET imaging of AlF-PSMA-Q in normal mice and tumor-bearing mice, and a comparison with F-DCFPyL were performed. PET/CT imaging was performed on 8 healthy volunteers and 20 newly diagnosed PCa patients at 1 h post-injection (p.i.). The biodistribution in human and preliminary diagnostic efficacy of AlF-PSMA-Q were evaluated, and the radiation dosimetry was estimated using OLINDA/EXM 2.0 software.

RESULT

Qualified AlF-PSMA-Q was efficiently prepared with a non-decay-corrected radiochemical yield (RCY) of 22.0-28.3%, a specific activity (SA) of > 50 GBq/μmol. The hydrophilicity was comparably high with a log P value of - 3.69 ± 0.39. AlF-PSMA-Q was found to bind to PSMA specifically with a Ki value of 17.05 ± 1.14 nM. The distribution and elimination half-lives of AlF-PSMA-Q were 3.93 min and 14.22 min, respectively, which were shorter than those of F-DCFPyL. Micro-PET imaging of AlF-PSMA-Q can clearly differentiate 22Rv1 tumors from PC-3 tumors and background with a high SUVmax of 2.17 ± 0.42 and a tumor-to-muscle ratio of 84.37 ± 31.62, which were higher than those of F-DCFPyL (1.79 ± 0.39 and 13.25 ± 1.65). The uptake of AlF-PSMA-Q in 22Rv1 cells and tumors can be substantially blocked by 2-PMPA. High level accumulation of AlF-PSMA-Q was observed in organs physiologically expressing PSMA. Twenty-six tumor lesions were detected in 20 PCa patients, and the mean SUVmax values of primary tumors, lymph node metastasis, bone metastases, and tumor-muscle ratios were 19.71 ± 16.52, 5.11, 31.30 ± 29.85, and 44.77 ± 22.29, respectively. The mean SUVmax of tumors in patients with PSA > 10 ng/mL was significantly higher than that in patients with PSA ≤ 10 ng/mL (25.97 ± 18.64 vs. 10.33 ± 3.74). Meanwhile, the mean SUVmax of tumors in patients with a Gleason score ≥ 8 was significantly higher than that in patients with a Gleason score < 8 (31.85 ± 22.09 vs. 13.18 ± 11.58). The kidneys received the highest estimated dose of 0.098 ± 0.006 mGy/MBq, and the effective dose was calculated as 0.0128 ± 0.007 mGy/MBq.

CONCLUSION

The novel qualified PSMA-targeted radiotracer AlF-PSMA-Q was conveniently prepared with favorable yield and SA. The results of preclinical and pilot clinical studies exhibited a high specific uptake in PCa lesions and an excellent tumor-to-background ratio with a reasonable radiation exposure, which indicated the great potential of AlF-PSMA-Q for PCa imaging.

TRIAL REGISTRATION

Chinese Clinical trial registry ChiCTR2100053507, Registered 23 November 2021, retrospectively registered.

摘要

目的

通过临床前和初步临床研究,研究一种新型的 AlF 标记 PSMA 靶向放射性示踪剂在前列腺癌诊断中的潜力。

方法

自动制备 AlF-PSMA-Q。使用 22Rv1(PSMA+)和 PC-3(PSMA-)细胞系评估其与 PSMA 的结合亲和力。在正常小鼠和荷瘤小鼠中进行药代动力学评估、生物分布研究、AlF-PSMA-Q 的 Micro-PET 成像,并与 F-DCFPyL 进行比较。在注射后 1 小时(p.i.)对 8 名健康志愿者和 20 名新诊断的前列腺癌患者进行 PET/CT 成像。评估 AlF-PSMA-Q 在人体中的生物分布和初步诊断疗效,并使用 OLINDA/EXM 2.0 软件估计辐射剂量。

结果

高效制备了合格的 AlF-PSMA-Q,非衰变校正的放射化学产率(RCY)为 22.0-28.3%,比活度(SA)>50GBq/μmol。亲水性相当高,log P 值为-3.69±0.39。AlF-PSMA-Q 被发现与 PSMA 特异性结合,Ki 值为 17.05±1.14 nM。AlF-PSMA-Q 的分布和消除半衰期分别为 3.93 分钟和 14.22 分钟,均短于 F-DCFPyL。AlF-PSMA-Q 的 Micro-PET 成像可以清晰地区分 22Rv1 肿瘤和 PC-3 肿瘤与背景,SUVmax 高达 2.17±0.42,肿瘤与肌肉的比值为 84.37±31.62,均高于 F-DCFPyL(1.79±0.39 和 13.25±1.65)。AlF-PSMA-Q 在 22Rv1 细胞和肿瘤中的摄取可被 2-PMPA 显著阻断。AlF-PSMA-Q 在生理性表达 PSMA 的器官中有高水平的蓄积。在 20 名前列腺癌患者中检测到 26 个肿瘤病灶,原发性肿瘤、淋巴结转移、骨转移和肿瘤-肌肉比值的平均 SUVmax 值分别为 19.71±16.52、5.11、31.30±29.85 和 44.77±22.29。PSA>10ng/mL 患者的肿瘤平均 SUVmax 值明显高于 PSA≤10ng/mL 的患者(25.97±18.64 比 10.33±3.74)。同时,Gleason 评分≥8 的患者的肿瘤平均 SUVmax 值明显高于 Gleason 评分<8 的患者(31.85±22.09 比 13.18±11.58)。肾脏接受的估计剂量最高,为 0.098±0.006mGy/MBq,有效剂量计算为 0.0128±0.007mGy/MBq。

结论

新型合格的 PSMA 靶向放射性示踪剂 AlF-PSMA-Q 具有良好的产量和比活度,方便制备。临床前和初步临床研究结果显示,前列腺癌病灶具有高特异性摄取和良好的肿瘤与背景比,具有合理的辐射暴露,表明 AlF-PSMA-Q 具有前列腺癌成像的巨大潜力。

临床试验注册

中国临床试验注册中心 ChiCTR2100053507,于 2021 年 11 月 23 日注册,回顾性注册。

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