PSMA-PET/CT response after metastasis-directed radiotherapy of bone oligometastases in prostate cancer.

EJNMMI reports Pub Date : 2024-08-19 DOI:10.1186/s41824-024-00212-w

Gabriel T Sheikh, Christian Trapp, Nina-Sophie Schmidt-Hegemann, Alexander Buchner, Christian G Stief, Marcus Unterrainer, Wolfgang G Kunz, Clemens C Cyran, Freba Grawe, Astrid Delker, Mathias J Zacherl, Adrien Holzgreve, Lena M Unterrainer, Matthias Brendel, Claus Belka, Minglun Li, Paul Rogowski

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Abstract

Objective: Bone metastases are very common in advanced prostate cancer and can sensitively be detected utilizing PSMA-PET/CT. Therefore, our goal was to evaluate the suitability of PSMA-PET/CT-guided metastasis-directed external beam radiotherapy (MDT) as treatment option for patients with biochemical recurrence and oligometastatic bone lesions.

Materials & methods: We retrospectively examined 32 prostate cancer patients with biochemical recurrence and PSMA-positive oligometastatic disease limited to the bone (n = 1-3). A total of 49 bone lesions were treated with MDT. All patients received a post-radiotherapy PSMA-PET/CT-Scan. Changes in SUV_max, PSMA-positive tumor volume per lesion and PSA, as well as the correlation between the PET/CT-interval and SUV_max response were calculated.

Results: MDT lead to a SUV_max decrease in 46/49 (94%) of the lesions. The median relative decline of SUV_max was 60.4%, respectively. Based on PSMA-positive lesion volume with a SUV cut-off of 4, 46/49 (94%) of lesions showed complete response, two (4%) partial response and one lesion (2%) was stable on PSMA-PET/CT after MDT. Most of the treated patients (56.3%) showed an initial PSA decline at three months and a PSA nadir of median 0.14 ng/ml after a median time of 3.6 months after MDT. The median relative PSA change at three months after MDT was 3.9%.

Conclusion: MDT is a very effective treatment modality for prostate cancer bone oligometastases and lesion response to MDT can be assessed using the (semi-)quantitative parameters SUV_max and PSMA-positive lesion volume with established SUV cut-offs.

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前列腺癌骨寡转移灶转移导向放疗后的 PSMA-PET/CT 反应。

目的：骨转移在晚期前列腺癌中非常常见，利用 PSMA-PET/CT 可以灵敏地检测到骨转移。因此，我们的目标是评估 PSMA-PET/CT 引导下的转移灶定向外照射放疗（MDT）是否适合作为生化复发和寡转移骨病灶患者的治疗方案：我们回顾性研究了32例生化复发且PSMA阳性寡转移病灶局限于骨的前列腺癌患者（n = 1-3）。共有 49 例骨病变接受了 MDT 治疗。所有患者均接受了放疗后 PSMA-PET/CT 扫描。计算了SUVmax、每个病灶的PSMA阳性肿瘤体积和PSA的变化，以及PET/CT间隔与SUVmax反应之间的相关性：MDT导致46/49（94%）个病灶的SUVmax下降。SUVmax相对下降的中位数分别为60.4%。基于 PSMA 阳性病灶体积（SUV 临界值为 4），46/49（94%）个病灶在 MDT 后出现完全反应，2 个（4%）部分反应，1 个病灶（2%）在 PSMA-PET/CT 上表现稳定。大多数接受治疗的患者（56.3%）的 PSA 在三个月后开始下降，在 MDT 后的 3.6 个月后，PSA 的中位数降至 0.14 ng/ml。MDT 后三个月的 PSA 相对变化中位数为 3.9%：结论：MDT是一种非常有效的前列腺癌骨寡转移治疗方法，病灶对MDT的反应可通过（半）定量参数SUVmax和PSMA阳性病灶体积以及已确定的SUV临界值进行评估。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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EJNMMI reports

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