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前列腺特异性膜抗原 (PSMA) PET 成像用冷试剂盒:Ga-Tris(羟基亚乙基二膦酸)-PSMA PET/CT 用于前列腺癌患者的 1 期研究。

Cold Kit for Prostate-Specific Membrane Antigen (PSMA) PET Imaging: Phase 1 Study of Ga-Tris(Hydroxypyridinone)-PSMA PET/CT in Patients with Prostate Cancer.

机构信息

Sir Peter MacCallum Department of Oncology, University of Melbourne, Melbourne, Victoria, Australia

Cancer Imaging, Peter MacCallum Cancer Centre, Melbourne, Victoria, Australia.

出版信息

J Nucl Med. 2018 Apr;59(4):625-631. doi: 10.2967/jnumed.117.199554. Epub 2017 Oct 6.

DOI:10.2967/jnumed.117.199554
PMID:28986512
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7116766/
Abstract

Ga-labeled urea-based inhibitors of the prostate-specific membrane antigen (PSMA), such as Ga-labeled ,'-bis(2-hydroxybenzyl)ethylenediamine-,'-diacetic acid (HBED)-PSMA-11, are promising small molecules for targeting prostate cancer. A new radiopharmaceutical, Ga-labeled tris(hydroxypyridinone) (THP)-PSMA, has a simplified design for single-step kit-based radiolabeling. It features the THP ligand, which forms complexes with Ga rapidly at a low concentration, at room temperature, and over a wide pH range, enabling direct elution from a Ge/Ga generator into a lyophilized radiopharmaceutical kit in 1 step without manipulation. The aim of this phase 1 study was to assess the safety and biodistribution of Ga-THP-PSMA. Cohort A comprised 8 patients who had proven prostate cancer and were scheduled to undergo prostatectomy; they had Gleason scores of 7-10 and a mean prostate-specific antigen level of 7.8 μg/L (range, 5.4-10.6 μg/L). They underwent PET/CT after the administration of Ga-THP-PSMA. All patients proceeded to prostatectomy (7 with pelvic nodal dissection). Dosimetry from multi-time-point PET imaging was performed with OLINDA/EXM. Cohort B comprised 6 patients who had positive Ga-HBED-PSMA-11 PET/CT scanning results and underwent comparative Ga-THP-PSMA scanning. All patients were monitored for adverse events. No adverse events occurred. In cohort A, 6 of 8 patients had focal uptake in the prostate (at 2 h: average SUV, 5.1; range, 2.4-9.2) and correlative 3+ staining of prostatectomy specimens on PSMA immunohistochemistry. The 2 Ga-THP-PSMA scans with negative results had only 1+/2+ staining. The mean effective dose was 2.07E-02 mSv/MBq. In cohort B, Ga-THP-PSMA had lower physiologic background uptake than Ga-HBED-PSMA-11 (in the parotid glands, the mean SUV for Ga-THP-PSMA was 3.6 [compared with 19.2 for Ga-HBED-PSMA-11]; the respective corresponding values in the liver were 2.7 and 6.3, and those in the spleen were 2.7 and 10.5; < 0.001 for all). In 5 of 6 patients, there was concordance in the number of metastases identified with Ga-HBED-PSMA-11 and Ga-THP-PSMA. Thirteen of 15 nodal abnormalities were subcentimeter. In 22 malignant lesions, the tumor-to-liver contrast with Ga-THP-PSMA was similar to that with Ga-HBED-PSMA (4.7 and 5.4, respectively; = 0.15), despite a higher SUV for Ga-HBED-PSMA than for Ga-THP-PSMA (30.3 and 10.7, respectively; < 0.01). Ga-THP-PSMA is safe and has a favorable biodistribution for clinical imaging. Observed focal uptake in the prostate was localized to PSMA-expressing malignant tissue on histopathology. Metastatic PSMA-avid foci were also visualized with Ga-THP-PSMA PET. Single-step production from a Good Manufacturing Practice cold kit may enable rapid adoption.

摘要

镓标记的前列腺特异性膜抗原(PSMA)的基于尿素的抑制剂,如镓标记的`,'-双(2-羟基苄基)乙二胺-,' - 二乙酸(HBED)-PSMA-11,是靶向前列腺癌的有前途的小分子。一种新的放射性药物,镓标记的三(羟基吡啶酮)(THP)-PSMA,具有简化的设计,可用于单步试剂盒放射性标记。它具有 THP 配体,该配体在室温下以低浓度、在宽 pH 范围内迅速与 Ga 形成配合物,能够直接从 Ge/Ga 发生器洗脱到冻干的放射性药物试剂盒中,无需操作。这项 1 期研究的目的是评估 Ga-THP-PSMA 的安全性和生物分布。A 队列包括 8 名已确诊患有前列腺癌且计划接受前列腺切除术的患者;他们的 Gleason 评分为 7-10,前列腺特异性抗原水平平均为 7.8 μg/L(范围为 5.4-10.6 μg/L)。他们在给予 Ga-THP-PSMA 后进行了 PET/CT 检查。所有患者均进行了前列腺切除术(7 例伴盆腔淋巴结清扫术)。通过 OLINDA/EXM 进行了多时间点 PET 成像的剂量测定。B 队列包括 6 名 Ga-HBED-PSMA-11 PET/CT 扫描结果阳性且接受 Ga-THP-PSMA 扫描比较的患者。所有患者均监测不良事件。没有发生不良事件。在 A 队列中,8 例患者中有 6 例前列腺有局灶性摄取(2 h:平均 SUV,5.1;范围,2.4-9.2),前列腺切除术标本的 PSMA 免疫组织化学染色呈 3+染色。2 例结果为阴性的 Ga-THP-PSMA 扫描仅有 1+/2+染色。平均有效剂量为 2.07E-02 mSv/MBq。在 B 队列中,Ga-THP-PSMA 的生理背景摄取低于 Ga-HBED-PSMA-11(在腮腺中,Ga-THP-PSMA 的平均 SUV 为 3.6[与 Ga-HBED-PSMA-11 的 19.2 相比];相应的肝脏值分别为 2.7 和 6.3,脾脏值分别为 2.7 和 10.5;所有值均<0.001)。在 6 例患者中的 5 例中,Ga-HBED-PSMA-11 和 Ga-THP-PSMA 识别的转移数量一致。15 个淋巴结异常中有 13 个为亚厘米。在 22 个恶性病变中,Ga-THP-PSMA 的肿瘤与肝脏的对比度与 Ga-HBED-PSMA 相似(分别为 4.7 和 5.4;=0.15),尽管 Ga-HBED-PSMA 的 SUV 高于 Ga-THP-PSMA(分别为 30.3 和 10.7;<0.01)。Ga-THP-PSMA 是安全的,具有有利的临床成像生物分布。在组织病理学上观察到的前列腺局灶性摄取定位于 PSMA 表达的恶性组织。用 Ga-THP-PSMA PET 还可以观察到转移性 PSMA 摄取的焦点。从良好生产规范冷试剂盒进行的单步生产可能会使其迅速采用。

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