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前列腺癌患者常规影像阴性或不确定的复发:F-氟代脱氧葡萄糖-PET/CT 在勾画复发部位和识别寡转移疾病患者中的作用。

Prostate cancer recurrence in patients with negative or equivocal conventional imaging: A role for F-fluciclovine-PET/CT in delineating sites of recurrence and identifying patients with oligometastatic disease.

机构信息

Division of Urologic Surgery, Department of Surgery and the Alvin J. Siteman Cancer Center, Washington University School of Medicine, St. Louis, MO,.

Division of Nuclear Medicine, Mallinckrodt Institute of Radiology and the Alvin J. Siteman Cancer Center, Washington University School of Medicine, St. Louis, MO.

出版信息

Urol Oncol. 2021 Jun;39(6):365.e9-365.e16. doi: 10.1016/j.urolonc.2020.10.017. Epub 2020 Nov 5.

Abstract

INTRODUCTION

Despite improvements in overall survival, biochemical recurrence of prostate cancer, characterized by rising prostate-specific antigen (PSA) levels after curative intent primary therapy, remains common. With the advent of highly sensitive molecular imaging, men with limited metastatic disease burden, or oligometastatic prostate cancer, are increasingly being identified. The LOCATE trial (NCT02680041) assessed the impact of positron emission tomography (PET) with F-fluciclovine on management of men with prostate cancer recurrence after curative intent primary therapy and negative/equivocal conventional imaging. Here, we use LOCATE data to characterize the sites of disease recurrence and explore the potential for F-fluciclovine-PET/CT to evaluate oligometastatic disease.

METHODS

Eligible men (≥18 years; prior curative intent treatment of prostate cancer; recurrence based on rising PSA; negative/equivocal conventional imaging) underwent F-fluciclovine-PET/CT according to standard protocols. The primary outcome measure of the LOCATE trial was a revised management plan post-scan. We performed a secondary analysis of the LOCATE imaging data to characterize anatomical sites of disease recurrence and to explore the potential for F-fluciclovine-PET/CT to evaluate oligometastatic disease. Imaging results were stratified by baseline PSA levels and prior treatment(s) and the Fisher exact test used to analyze differences between groups. Oligometastatic disease was defined as 1-5 extraprostatic lesions (≤3 lesions in any single organ system) plus negative prostate/bed imaging (as a surrogate for primary tumor control).

RESULTS

Of 213 enrolled patients, 164 (77%) had undergone prostatectomy as their initial treatment; their median PSA was 0.57ng/ml. For the 49 patients with an intact prostate, the median PSA was 5.5ng/ml. The overall F-fluciclovine-PET/CT detection rate was 57%. Detection rates were 84% in men with intact prostates and 49% in those who had undergone prostatectomy, with the difference being attributable to prostate/bed findings (71% vs. 18%, respectively). The detection rate in lymph nodes was 29% and in bone was 11%. In total, 53/213 (25%) had oligometastatic disease. Twenty (38%) oligometastatic patients had PSA ≤1.0 ng/ml. Forty-two (79%) experienced a change to their management plan following the scan, commonly to target a lesion identified by F-fluciclovine-PET/CT. The majority of management changes (74%) involved a new treatment modality; however, 10 patients (24%) experienced a modification of the existing plan for radiotherapy to incorporate a boost to an area guided by the F-fluciclovine-PET/CT results.

CONCLUSION

Even at low PSA levels, F-fluciclovine-PET/CT identified a diverse pattern of recurrence missed with conventional imaging. One-quarter of men had oligometastatic disease, raising the potential for F-fluciclovine-PET/CT to guide targeted treatment of oligometastases.

摘要

简介

尽管整体生存率有所提高,但前列腺癌的生化复发(以根治性初始治疗后前列腺特异性抗原 [PSA] 水平升高为特征)仍然很常见。随着高灵敏度分子成像的出现,患有有限转移性疾病负担或寡转移性前列腺癌的男性越来越多地被发现。LOCATE 试验(NCT02680041)评估了 F-氟代赖氨酸正电子发射断层扫描(PET)对根治性初始治疗后前列腺癌复发且常规成像阴性/不确定的男性管理的影响。在这里,我们使用 LOCATE 数据来描述疾病复发的部位,并探讨 F-氟代赖氨酸-PET/CT 评估寡转移性疾病的潜力。

方法

符合条件的男性(≥18 岁;先前接受过根治性前列腺癌治疗;基于 PSA 升高的复发;阴性/不确定的常规成像)根据标准方案接受 F-氟代赖氨酸-PET/CT。LOCATE 试验的主要结局指标是扫描后修订的管理计划。我们对 LOCATE 成像数据进行了二次分析,以描述疾病复发的解剖部位,并探讨 F-氟代赖氨酸-PET/CT 评估寡转移性疾病的潜力。根据基线 PSA 水平和先前的治疗方法对成像结果进行分层,并使用 Fisher 精确检验分析组间差异。寡转移性疾病定义为 1-5 个前列腺外病变(任何单个器官系统中≤3 个病变)加上前列腺/床成像阴性(作为原发性肿瘤控制的替代)。

结果

在 213 名入组患者中,164 名(77%)患者最初接受了前列腺切除术治疗;他们的中位 PSA 为 0.57ng/ml。对于 49 名保留前列腺的患者,中位 PSA 为 5.5ng/ml。总体而言,F-氟代赖氨酸-PET/CT 的检测率为 57%。在保留前列腺的男性中,检测率为 84%,在接受前列腺切除术的男性中为 49%,差异归因于前列腺/床的发现(分别为 71%和 18%)。淋巴结的检测率为 29%,骨骼的检测率为 11%。总共,213 名患者中有 53 名(25%)患有寡转移性疾病。20 名(38%)寡转移患者的 PSA≤1.0ng/ml。42 名(79%)患者在扫描后改变了管理计划,通常是为了靶向 F-氟代赖氨酸-PET/CT 识别的病变。大多数管理变更(74%)涉及新的治疗方式;然而,10 名患者(24%)对现有的放疗计划进行了修改,以纳入 F-氟代赖氨酸-PET/CT 结果指导的区域增强。

结论

即使在 PSA 水平较低的情况下,F-氟代赖氨酸-PET/CT 也能识别出常规成像遗漏的多种复发模式。四分之一的男性患有寡转移性疾病,这增加了 F-氟代赖氨酸-PET/CT 引导寡转移靶向治疗的潜力。

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