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放射性核素治疗转移性前列腺癌。

Radionuclide Therapy of Metastatic Prostate Cancer.

机构信息

Department of Nuclear Medicine, University Hospital Heidelberg, Heidelberg, Germany.

Department of Nuclear Medicine, University Hospital Heidelberg, Heidelberg, Germany; Cooperation Unit Nuclear Medicine, German Cancer Research Center (DKFZ), Heidelberg, Germany.

出版信息

Semin Nucl Med. 2019 Jul;49(4):313-325. doi: 10.1053/j.semnuclmed.2019.02.003. Epub 2019 Mar 2.

Abstract

The current mainstay of treatment in metastatic prostate cancer is based on hormonal manipulations. Standard androgen deprivation therapy and novel androgen axis drugs are commonly well tolerable and can stabilize metastatic hormone-sensitive prostate cancers for years. However, metastatic castration-resistant prostate cancer is still challenging to treat. Except taxanes, prostate cancer presents intrinsic resistance against conventional chemotherapies. The typically elderly patient population excludes more aggressive treatment regimens. First clinical trials evaluating immunotherapy or tyrosine-kinase-inhibitors against prostate cancer failed. In contrast, prostate cancer can be radiosensitive and external beam radiotherapy is effective in localized prostate cancer, thus providing a good rationale for the use of systemic radiopharmaceuticals in the metastatic setting. Beta-particle emitting "bone-seekers" have a long history and are effective as analgesics but do not improve survival because they are limited by red-marrow dose. Alpha emitting Radium can be used in a dose that prolongs survival but is restricted to bone-confined patients. Currently radiolabeled high-affinity ligands to the prostate-specific membrane antigen are in clinical evaluation. While radioimmunotherapy approaches were limited by the long circulation time and slow tumor-accumulation of antibodies, low molecular weight PSMA-specific ligands offer an approx. ten-fold improved tumor to red-marrow ratio in comparison to the unspecific bone-seekers. Early clinical studies demonstrate that regarding surrogate markers, such as >50% PSA reduction (60%) and radiologic response (80%), PSMA-therapy exceeds the antitumor activity of all approved or other recently tested compounds; for example, PSA-response was only observed in approx. a total of 10% of patients treated with ipilimumab, sunitinib, cabozantinib, or xofigo, respectively and in approx. 30, 40, 50% of patients treated with abiraterone, cabazitaxel, or enzalutamide. Also progression free and overall survivals of these single-arm studies appear promising when compared to historical controls. Consecutively, the first PSMA-RLT recently advanced into phase-3 (Lu-PSMA-617; VISION-trial). Future developments aim to avoid off-target radiation by ligand-optimization and to outperform the antitumor activity of beta-emitter PSMA-RLT by labeling with highly focused, high energy transferring alpha-nuclides; however the latter potentially also increasing the risk of side-effects and additional early phase studies are needed to improve treatment protocols. Academically clinical research is developing prognostic tools to improve treatment benefit by selecting the most appropriate patients in advance.

摘要

目前,转移性前列腺癌的主要治疗方法基于激素治疗。标准的雄激素剥夺疗法和新型雄激素轴药物通常具有良好的耐受性,并能使转移性激素敏感型前列腺癌多年稳定。然而,转移性去势抵抗性前列腺癌仍然难以治疗。除紫杉烷类药物外,前列腺癌对常规化疗具有内在耐药性。通常,老年患者群体排除了更具侵袭性的治疗方案。评估免疫疗法或酪氨酸激酶抑制剂治疗前列腺癌的首次临床试验均失败。相比之下,前列腺癌对放射治疗敏感,外照射放疗对局限性前列腺癌有效,因此为转移性疾病中使用全身放射性药物提供了合理的依据。β粒子发射的“骨靶向剂”具有悠久的历史,作为镇痛药有效,但不能提高生存率,因为它们受到骨髓剂量的限制。α发射镭可用于延长生存时间的剂量,但仅限于局限于骨的患者。目前,放射性标记的前列腺特异性膜抗原高亲和力配体正在进行临床评估。虽然放射免疫疗法因抗体的循环时间长和肿瘤积累缓慢而受到限制,但与非特异性骨靶向剂相比,低分子量 PSMA 特异性配体提供了约 10 倍的肿瘤与骨髓比值。早期临床研究表明,就替代标志物(如 PSA 降低>50%(60%)和影像学反应(80%))而言,PSMA 治疗超过了所有批准的或其他最近测试的化合物的抗肿瘤活性;例如,在分别用伊匹单抗、舒尼替尼、卡博替尼或 Xofigo 治疗的患者中,只有约 10%的患者观察到 PSA 反应,在分别用阿比特龙、卡巴他赛或恩扎鲁胺治疗的患者中,有 30%、40%和 50%的患者观察到 PSA 反应。与历史对照相比,这些单臂研究的无进展生存期和总生存期似乎也很有希望。随后,最近的第一种 PSMA-RLT 进入了 3 期(Lu-PSMA-617; VISION 试验)。未来的发展旨在通过配体优化避免非靶向辐射,并通过标记高聚焦、高能量转移的α核素来提高β发射 PSMA-RLT 的抗肿瘤活性;然而,后者也可能增加副作用的风险,需要进行更多的早期研究来改进治疗方案。在学术上,临床研究正在开发预后工具,通过提前选择最合适的患者来提高治疗效果。

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