PSMA 放射引导手术后生化复发患者的失败模式

Lilit Schweiger, Tobias Maurer, Ricarda Simon, Thomas Horn, Matthias Heck, Wolfgang A. Weber, Matthias Eiber, Isabel Rauscher
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引用次数: 0

摘要

前列腺特异性膜抗原(PSMA)靶向放射引导手术(RGS)正在发展成为一种新的治疗方式,用于治疗前列腺癌早期生化复发患者,以及在PSMA配体PET/CT检查中病变局限于局部淋巴结的患者。然而,PSMA RGS 治疗失败的模式(局部与全身)仍然未知。因此,本回顾性分析旨在使用 PSMA 配体 PET 评估 PSMA RGS 后复发患者的疾病模式。方法:我们评估了 100 例接受 PSMA 配体 PET(前列腺特异性抗原 [PSA] 中位数,0.9 纳克/毫升;范围,0.2-14.2 纳克/毫升)的 PET 引导 PSMA RGS 后生化复发的患者。所有复发性前列腺癌可疑病灶均按照分子成像 TNM 分类系统进行分组。根据 PSA 值和国际泌尿病理学会的分级组别确定检测率和病灶定位,并进行分层。此外,还比较了 PSMA RGS 前后的病灶定位情况。结果:PSMA RGS与PSMA配体PET之间的中位复发时间为11.4个月(5.5-25.6个月)。在 100 例患者中,共有 91 例(91%)显示 PSMA 配体阳性。PSA 水平为 0.2-0.49、0.5-0.99、1-1.99 和至少 2 纳克/毫升的 PSMA PET 检测率分别为 82.6%、92.6%、91.3% 和 96.3%。一半以上的患者(53%;48/91)仅出现局部复发或盆腔淋巴结转移。出现盆腔外淋巴结转移、骨转移和内脏转移的患者分别占 22%(20/91)、16%(15/91)和 9%(8/91)。随着国际泌尿病理学会分级组别的增加,骨转移和内脏转移患者的比例也在增加,而仅有局部病变的患者人数则在减少。结论:PSMAPSMA配体PET是检测PSMA RGS生化治疗失败患者复发疾病并对其进行定位的有效方法,半数以上患者出现局部复发,为第二次局部治疗(如放疗或重复手术)提供了可能性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Pattern of Failure in Patients with Biochemical Recurrence After PSMA Radioguided Surgery

Prostate-specific membrane antigen (PSMA)–targeted radioguided surgery (RGS) is evolving as a new treatment modality for patients with early biochemical recurrence of prostate cancer and disease limited to locoregional lymph nodes on PSMA-ligand PET/CT. Nevertheless, the pattern of failure (locoregional vs. systemic) after PSMA RGS remains unknown. Therefore, the aim of this retrospective analysis was to evaluate the pattern of disease using PSMA-ligand PET in patients experiencing relapse after PSMA RGS. Methods: We evaluated 100 patients with biochemical recurrence after previous PET-guided PSMA RGS who underwent PSMA-ligand PET (median prostate-specific antigen [PSA], 0.9 ng/mL; range, 0.2–14.2 ng/mL). All suspicious lesions for recurrent prostate cancer were grouped according to the molecular imaging TNM classification system. Detection rates and lesion localization were determined and stratified by PSA values and the International Society of Urological Pathology grade group. Further, lesion localization was compared before and after PSMA RGS. Results: The median time between PSMA RGS and PSMA-ligand PET for relapse was 11.4 mo (range, 5.5–25.6 mo). In total, 91 of 100 (91%) patients showed PSMA-ligand–positive findings. PSMA PET detection rates were 82.6%, 92.6%, 91.3%, and 96.3% for PSA levels of 0.2–0.49, 0.5–0.99, 1–1.99, and at least 2 ng/mL, respectively. More than half of the patients (53%; 48/91) showed local recurrence or pelvic lymph node metastases only. Extrapelvic lymph node metastases, bone metastases, and visceral metastases were present in 22% (20/91), 16% (15/91), and 9% (8/91) of the patients, respectively. With increasing International Society of Urological Pathology grade group, the percentage of patients with bone and visceral metastases increased, whereas the number of patients with only locoregional disease decreased. Conclusion: PSMA-ligand PET is a useful method to detect and localize recurrent disease in patients with biochemical failure after PSMA RGS, with more than half of the patients presenting with locoregional recurrence, offering the potential for a second local therapy (e.g., radiation therapy or repeated surgery).

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