Department of Nuclear Medicine, Faculty of Medicine, Yeditepe University, Istanbul, Turkey.
Department of Radiology, University of Missouri, Columbia, Missouri.
J Nucl Med. 2023 Oct;64(10):1574-1580. doi: 10.2967/jnumed.123.265546. Epub 2023 Aug 24.
For patients with advanced-stage metastatic castration-resistant prostate cancer (mCRPC) who do not respond to [Lu]Lu-PSMA therapy, there are limited treatment options. Clinical results obtained with [Ac]Ac-PSMA are promising. We retrospectively analyzed the outcomes of patients treated with [Ac]Ac-PSMA between December 2018 and October 2022. We evaluated the treatment results of 23 patients (mean age, 70.3 ± 8.8 y) with mCRPC who were refractory to treatment with [Lu]Lu-PSMA (2-9 cycles). The safety profile was assessed according to Common Technology Criteria for Adverse Events version 5.0. Treatment efficacy was assessed using prostate-specific membrane antigen PET progression criteria and prostate-specific antigen (PSA) response according to Prostate Cancer Working Group 2 criteria after the first cycle of [Ac]Ac-PSMA treatment. All patients received androgen-deprivation therapy, whereas 22 (96%) and 19 (83%) patients received chemotherapy and second-generation antiandrogen therapy, respectively. One patient received 4 cycles, 2 received 3 cycles, 8 received 2 cycles, and 12 received 1 cycle of [Ac]Ac-PSMA. The median interval between cycles was 13 wk (range, 8-28 wk). [Ac]Ac-PSMA was administered with a mean activity of 7.6 MBq (range, 6.2-10.0 MBq) in each cycle. Patients were at an advanced stage of disease, and tumor burden was very high. Although the best PSA response was observed in 5 patients (26%) after [Ac]Ac-PSMA treatment, there was at least some level of decline in PSA observed in 11 patients (58%; = 19). Treatment response was assessed in patients who underwent [Ga]Ga-PSMA PET/CT imaging. After the first cycle of treatment ( = 18), 50% of patients ( = 9) showed disease progression according to prostate-specific membrane antigen PET progression criteria, and the disease control rate was calculated to be 50%. Median progression-free survival was 3.1 mo, and median overall survival was 7.7 mo. Grade 3 hematologic toxicity occurred in 1 patient, and grade 3 nephrotoxicity was observed in another patient. Parotid SUV decreased by 33%, although all patients complained of dry mouth before treatment. We observed that [Ac]Ac-PSMA therapy was safe and showed potential even in cases with advanced-stage mCRPC in which all other treatment options were completed.
对于接受 [Lu]Lu-PSMA 治疗后无反应的晚期转移性去势抵抗性前列腺癌(mCRPC)患者,治疗选择有限。[Ac]Ac-PSMA 的临床结果很有前景。我们回顾性分析了 2018 年 12 月至 2022 年 10 月期间接受 [Ac]Ac-PSMA 治疗的 23 例 mCRPC 患者的治疗结果。我们评估了 23 例对 [Lu]Lu-PSMA(2-9 个周期)治疗有抗药性的 mCRPC 患者的治疗结果(平均年龄 70.3±8.8 岁)。根据通用技术标准 5.0 评估安全性概况。使用前列腺特异性膜抗原 PET 进展标准和前列腺特异性抗原(PSA)根据前列腺癌工作组 2 标准在接受第一周期 [Ac]Ac-PSMA 治疗后评估治疗效果。所有患者均接受去势治疗,22 例(96%)和 19 例(83%)患者分别接受化疗和第二代抗雄激素治疗。1 例患者接受 4 个周期,2 例患者接受 3 个周期,8 例患者接受 2 个周期,12 例患者接受 1 个周期的 [Ac]Ac-PSMA 治疗。周期之间的中位间隔为 13 周(范围,8-28 周)。每个周期中 [Ac]Ac-PSMA 的平均活性为 7.6 MBq(范围,6.2-10.0 MBq)。患者处于疾病的晚期,肿瘤负担非常高。尽管在 [Ac]Ac-PSMA 治疗后 5 例患者(26%)观察到最佳 PSA 反应,但 11 例患者(58%; = 19)观察到 PSA 至少有一定程度下降。在接受 [Ga]Ga-PSMA PET/CT 成像的患者中评估了治疗反应。在第一周期治疗后( = 18),根据前列腺特异性膜抗原 PET 进展标准,50%的患者( = 9)出现疾病进展,疾病控制率计算为 50%。中位无进展生存期为 3.1 个月,中位总生存期为 7.7 个月。1 例患者出现 3 级血液学毒性,另 1 例患者出现 3 级肾毒性。虽然所有患者在治疗前都抱怨口干,但腮腺 SUV 下降了 33%。我们观察到,即使在所有其他治疗选择均已完成的晚期 mCRPC 患者中,[Ac]Ac-PSMA 治疗也是安全且有潜力的。
