Department of Radiation Oncology, UCLA, Los Angeles, California.
Ahmanson Translational Theranostics Division, Department of Molecular and Medical Pharmacology, UCLA, Los Angeles, California.
J Nucl Med. 2024 Sep 3;65(9):1387-1394. doi: 10.2967/jnumed.124.267922.
Systemic treatments for metastatic castration-resistant prostate cancer (mCRPC) include androgen deprivation therapy, androgen receptor pathway inhibitors, chemotherapy, and radiopharmaceuticals, all of which have associated toxicity. Prostate-specific membrane antigen (PSMA) PET/CT allows for higher sensitivity in detecting metastatic disease than is possible with conventional imaging. We hypothesized that PSMA PET/CT-guided, metastasis-directed radiotherapy may offer durable disease control with low toxicity rates in patients with mCRPC who have a limited number of metastases. We retrospectively screened 5 prospective PSMA PET/CT studies for patients with mCRPC who had up to 5 sites of oligorecurrent or oligoprogressive disease on PSMA PET/CT and subsequently received definitive-intent, metastasis-directed radiotherapy to all new or progressing sites with concurrent androgen deprivation therapy. Progression-free survival, freedom from new lines of systemic therapy, and overall survival (OS) were calculated from the start of metastasis-directed radiotherapy using Kaplan-Meier analysis. Biochemical response was defined as at least a 50% decrease in prostate-specific antigen 6 mo after the start of treatment. Toxicity was graded using the Common Terminology Criteria for Adverse Events, version 5. Twenty-four patients met the inclusion criteria with a median follow-up of 33.8 mo (interquartile range, 27.6-45.1 mo). Between October 2017 and April 2023, 11 patients (45.8%) had 1 treated site, 10 patients (41.7%) had 2, and 3 patients (12.5%) had 3. Five sites were prostate or prostate bed, 15 were nodal, 19 were osseous, and 1 was visceral. Seventeen patients (70.8%) continued their preexisting systemic therapy, whereas 7 (29.2%) started a new systemic therapy. Median progression-free survival was 16.4 mo (95% CI, 9.8-23.0 mo). The biochemical response rate was 66.7%. Median freedom from a new line of systemic therapy was 29.0 mo (95% CI, 7.6-50.4 mo). Median OS was not reached. The 2- and 4-y OS rates were 91.1% (95% CI, 79.3%-100%) and 68.8% (95% CI, 45.1%-92.5%), respectively. Grade 2 and grade 3 or higher toxicity rates were 4.2% and 0%, respectively. PSMA PET/CT-guided, metastasis-directed radiotherapy appears to offer durable disease control with low toxicity rates for oligometastatic castration-resistant prostate cancer. Further prospective studies are needed to compare metastasis-directed radiotherapy with systemic therapy versus systemic therapy alone and PSMA PET/CT-guided versus conventional imaging-guided radiotherapy.
对于转移性去势抵抗性前列腺癌(mCRPC),全身治疗包括雄激素剥夺疗法、雄激素受体通路抑制剂、化疗和放射性药物治疗,所有这些治疗都有相关的毒性。前列腺特异性膜抗原(PSMA)PET/CT 比传统影像学检查具有更高的检测转移性疾病的敏感性。我们假设,对于 mCRPC 患者,PSMA PET/CT 引导的、针对转移灶的放射治疗可能会在具有有限数量转移灶的患者中提供低毒性的持久疾病控制。
我们回顾性筛选了 5 项前瞻性 PSMA PET/CT 研究,这些研究纳入了 mCRPC 患者,他们在 PSMA PET/CT 上有最多 5 个寡转移或寡进展病灶,随后接受了针对所有新发或进展病灶的根治性、针对转移灶的放射治疗,同时联合雄激素剥夺治疗。使用 Kaplan-Meier 分析,从针对转移灶的放射治疗开始计算无进展生存期、无新的系统治疗生存期和总生存期(OS)。生化缓解定义为治疗开始后至少前列腺特异性抗原下降 50%。毒性分级采用不良事件通用术语标准,版本 5。
24 例患者符合纳入标准,中位随访时间为 33.8 个月(四分位距,27.6-45.1 个月)。2017 年 10 月至 2023 年 4 月期间,11 例患者(45.8%)有 1 个治疗部位,10 例患者(41.7%)有 2 个,3 例患者(12.5%)有 3 个。5 个部位为前列腺或前列腺床,15 个部位为淋巴结,19 个部位为骨,1 个部位为内脏。17 例患者(70.8%)继续接受原有系统治疗,而 7 例患者(29.2%)开始新的系统治疗。中位无进展生存期为 16.4 个月(95%CI,9.8-23.0 个月)。生化缓解率为 66.7%。中位无新的系统治疗生存期为 29.0 个月(95%CI,7.6-50.4 个月)。中位总生存期未达到。2 年和 4 年的总生存率分别为 91.1%(95%CI,79.3%-100%)和 68.8%(95%CI,45.1%-92.5%)。2 级和 3 级或更高级别的毒性发生率分别为 4.2%和 0%。
PSMA PET/CT 引导的、针对转移灶的放射治疗似乎为寡转移性去势抵抗性前列腺癌提供了持久的疾病控制,毒性发生率低。需要进一步的前瞻性研究来比较针对转移灶的放射治疗与系统治疗与系统治疗相比,以及 PSMA PET/CT 引导与常规影像学引导的放射治疗。
