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用于前列腺癌的 Ac 放射性药物的 3D 微尺度剂量学和肿瘤控制。

3D small-scale dosimetry and tumor control of Ac radiopharmaceuticals for prostate cancer.

机构信息

Department of Nuclear Engineering, University of California, Berkeley, CA, USA.

Department of Radiology and Biomedical Imaging, University of California, San Francisco, CA, USA.

出版信息

Sci Rep. 2024 Aug 27;14(1):19938. doi: 10.1038/s41598-024-70417-3.

Abstract

Radiopharmaceutical therapy using -emitting Ac is an emerging treatment for patients with advanced metastatic cancers. Measurement of the spatial dose distribution in organs and tumors is needed to inform treatment dose prescription and reduce off-target toxicity, at not only organ but also sub-organ scales. Digital autoradiography with -sensitive detection devices can measure radioactivity distributions at 20-40 resolution, but anatomical characterization is typically limited to 2D. We collected digital autoradiographs across whole tissues to generate 3D dose volumes and used them to evaluate the simultaneous tumor control and regional kidney dosimetry of a novel therapeutic radiopharmaceutical for prostate cancer, [Ac]Ac-Macropa-PEG-YS5, in mice. 22Rv1 xenograft-bearing mice treated with 18.5 kBq of [Ac]Ac-Macropa-PEG-YS5 were sacrificed at 24 h and 168 h post-injection for quantitative -particle digital autoradiography and hematoxylin and eosin staining. Gamma-ray spectroscopy of biodistribution data was used to determine temporal dynamics and Bi redistribution. Tumor control probability and sub-kidney dosimetry were assessed. Heterogeneous Ac spatial distribution was observed in both tumors and kidneys. Tumor control was maintained despite heterogeneity if cold spots coincided with necrotic regions. Ac dose-rate was highest in the cortex and renal vasculature. Extrapolation of tumor control suggested that kidney absorbed dose could be reduced by 41% while maintaining 90% TCP. The 3D dosimetry methods described allow for whole tumor and organ dose measurements following Ac radiopharmaceutical therapy, which correlate to tumor control and toxicity outcomes.

摘要

放射性核素治疗使用发射β-粒子的Ac 是治疗晚期转移性癌症患者的一种新兴疗法。为了告知治疗剂量处方并降低脱靶毒性,不仅需要器官尺度,还需要亚器官尺度的器官和肿瘤空间剂量分布测量。具有β-灵敏检测装置的数字放射自显影术可以以 20-40μm 的分辨率测量放射性分布,但解剖特征通常限于 2D。我们收集了整个组织的数字放射自显影图以生成 3D 剂量体积,并将其用于评估新型前列腺癌治疗放射性药物[Ac]Ac-Macropa-PEG-YS5 在小鼠中的肿瘤控制和局部肾脏剂量学。用 18.5 kBq [Ac]Ac-Macropa-PEG-YS5 处理的 22Rv1 异种移植荷瘤小鼠在注射后 24 h 和 168 h 处死,进行定量β-粒子数字放射自显影术和苏木精和伊红染色。生物分布数据的伽马射线光谱用于确定时间动态和 Bi 再分布。评估了肿瘤控制概率和亚肾剂量学。在肿瘤和肾脏中都观察到不均匀的 Ac 空间分布。如果冷点与坏死区域重合,则可以维持肿瘤控制,尽管存在异质性。在皮质和肾脏脉管系统中,Ac 剂量率最高。肿瘤控制的外推表明,在保持 90%TCP 的情况下,肾脏吸收剂量可以减少 41%。描述的 3D 剂量学方法允许在接受 Ac 放射性药物治疗后进行整个肿瘤和器官剂量测量,这与肿瘤控制和毒性结果相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fbcf/11358493/ef46dbd49a09/41598_2024_70417_Fig1_HTML.jpg

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