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个体内比较 F-PSMA-1007 与肾排泄 PSMA 配体在复发性前列腺癌患者 PSMA PET 成像中的应用。

Intraindividual Comparison of F-PSMA-1007 with Renally Excreted PSMA Ligands for PSMA PET Imaging in Patients with Relapsed Prostate Cancer.

机构信息

Department of Nuclear Medicine, University Hospital of Cologne, Cologne, Germany.

Department of Medical Oncology, Dana-Farber Cancer Institute, Harvard Medical School, Boston, Massachusetts.

出版信息

J Nucl Med. 2020 May;61(5):729-734. doi: 10.2967/jnumed.119.234898. Epub 2019 Oct 18.

Abstract

F-prostate-specific membrane antigen (PSMA)-1007 is excreted mainly through the liver. We benchmarked the performance of F-PSMA-1007 against 3 renally excreted PSMA tracers. Among 668 patients, we selected 27 in whom PET/CT results obtained with Ga-PSMA-11, F-DCFPyL (2-(3-(1-carboxy-5-[(6-[F]fluoro-pyridine-3-carbonyl)-amino]-pentyl)-ureido)-pentanedioic acid), or F-JK-PSMA-7 (JK, Juelich-Koeln) were interpreted as equivocal or negative or as oligometastatic disease (PET-1). Within 3 wk, a second PET scan with F-PSMA-1007 was performed (PET-2). The confidence in the interpretation of PSMA-positive locoregional findings was scored on a 5-point scale, first in routine diagnostics (reader 1) and then by an independent second evaluation (reader 2). Discordant PSMA-positive skeletal findings were examined by contrast-enhanced MRI. For both readers, F-PSMA-1007 facilitated the interpretability of 27 locoregional lesions. In PET-2, the clinical readout led to a significantly lower number of equivocal locoregional lesions ( = 0.024), and reader 2 reported a significantly higher rate of suspected lesions that were falsely interpreted as probably benign in PET-1 ( = 0.023). Exclusively in PET-2, we observed a total of 15 PSMA-positive spots in the bone marrow of 6 patients (22%). None of the 15 discordant spots had a morphologic correlate on the corresponding CT scan or on the subsequent MRI scan. Thus, F-PSMA-1007 exhibits a significantly higher rate of unspecific medullary spots ( = 0.0006). F-PSMA-1007 may increase confidence in interpreting small locoregional lesions adjacent to the urinary tract but may decrease the interpretability of skeletal lesions.

摘要

F-前列腺特异性膜抗原(PSMA)-1007 主要通过肝脏排泄。我们将 F-PSMA-1007 的性能与 3 种经肾脏排泄的 PSMA 示踪剂进行了基准测试。在 668 名患者中,我们选择了 27 名患者,他们的 Ga-PSMA-11、F-DCFPyL(2-(3-(1-羧基-5-[(6-[F]氟吡啶-3-羰基)-氨基]-戊基)-脲基)戊二酸)或 F-JK-PSMA-7(JK,Juelich-Koeln)的 PET/CT 结果被解释为不确定或阴性或寡转移疾病(PET-1)。在 3 周内,用 F-PSMA-1007 进行了第二次 PET 扫描(PET-2)。PSMA 阳性局部区域发现的解释置信度在 5 分制上进行评分,首先在常规诊断中(读者 1),然后由独立的第二次评估(读者 2)进行评分。通过对比增强 MRI 检查不一致的 PSMA 阳性骨骼发现。对于两位读者,F-PSMA-1007 均有助于解释 27 个局部区域病变。在 PET-2 中,临床读片导致不确定的局部区域病变数量显著减少(=0.024),并且读者 2 报告了疑似病变的比例显著增加,这些病变在 PET-1 中被错误地解释为可能良性(=0.023)。仅在 PET-2 中,我们在 6 名患者(22%)的骨髓中总共观察到 15 个 PSMA 阳性斑点。在相应的 CT 扫描或随后的 MRI 扫描上,这 15 个不一致的斑点均无形态学相关性。因此,F-PSMA-1007 表现出明显更高的骨髓特异性斑点率(=0.0006)。F-PSMA-1007 可能会增加对邻近泌尿道的小局部区域病变的解释信心,但可能会降低对骨骼病变的解释能力。

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