用于对表达 PSMA 的前列腺癌进行 89Zr PET 成像和 177Lu 放射性药物治疗的单一螯合剂-微粒体 Theranostic 制剂。

Khanh-Van Ho, David S Tatum, Lisa Watkinson, Terry Carmack, Fang Jia, Alessandro Mascioni, Charles A Maitz, Darren Magda, Carolyn J Anderson
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引用次数: 0

摘要

在这里,我们描述了一种抗前列腺特异性膜抗原(PSMA)小体(IAB2MA),它与一种基于四个 1-hydroxypyridin-2-one 配位单元的八齿大环螯合剂(Lumi804 [L804])共轭,用 89Zr 标记(PET 成像)和 177Lu 标记(放射性药物治疗),目的是开发更安全、更有效的前列腺癌治疗方案。方法:将 L804 与目前的金标准螯合剂 DOTA 和去铁胺 (DFO) 进行比较,在 PSMA 阳性 PC3-PIP 肿瘤小鼠前列腺癌模型中进行细胞结合、临床前生物分布、成像、剂量测定和疗效研究。研究结果L804-IAB2MA 在环境温度下用 177Lu 或 89Zr 进行定量放射性标记(放射化学收率大于 99%)的时间不到 30 分钟,与 DFO-IAB2MA 的 89Zr 标记相当。相比之下,DOTA-IAB2MA 在 37°C 下用 177Lu 标记 30 分钟的放射化学收率约为 90%,需要进一步纯化。使用铕(III)作为发光替代物,在 PC3-PIP 细胞中证实了 Eu-L804-IAB2MA 与 PSMA 的高结合亲和力(解离常数为 4.6 ± 0.6 nM)。30 分钟后,所有 4 种放射性标记构建体在 PC3-PIP 细胞中的内化水平均明显高于 PSMA 阴性 PC3-FLU 细胞。注射后96小时和72小时,177Lu-和89Zr-L804-IAB2MA在PC3-PIP肿瘤和所有受检器官(即心脏、肝脏、脾脏、肾脏、肌肉、唾液腺、泪腺、躯体和骨骼)中的蓄积量分别明显低于177Lu-DOTA-IAB2MA和89Zr-DFO-IAB2MA。总体而言,SPECT/CT 和 PET/CT 成像数据显示,不同放射性racers 在肿瘤或肌肉的 SUV 均值上没有明显差异。通过器官水平和体素水平剂量计算方法进行的剂量测定分析表明,177Lu-DOTA-IAB2MA在肿瘤、肾脏、肝脏、肌肉和脾脏的吸收剂量明显高于177Lu-L804-IAB2MA。与未标记的小体对照组相比,接受单剂量 177Lu-L804-IAB2MA (18.4 或 22.2 MBq)治疗的 PC3-PIP 肿瘤小鼠生存期明显延长,肿瘤体积明显缩小。接受 177Lu-L804-IAB2MA 或 177Lu-DOTA-IAB2MA (18.4 或 22.2 MBq)治疗的各组小鼠存活率无明显差异。与 177Lu-DOTA-IAB2MA 相比,使用 177Lu-L804-IAB2MA 治疗肿瘤的吸收剂量更低,毒性更小。结论:89Zr-和177Lu-L804-IAB2MA可能是用于前列腺癌成像和治疗的一对前景看好的治疗剂。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Single Chelator-Minibody Theranostic Agents for 89Zr PET Imaging and 177Lu Radiopharmaceutical Therapy of PSMA-Expressing Prostate Cancer.

Here we describe an anti-prostate-specific membrane antigen (PSMA) minibody (IAB2MA) conjugated to an octadentate, macrocyclic chelator based on four 1-hydroxypyridin-2-one coordinating units (Lumi804 [L804]) labeled with 89Zr (PET imaging) and 177Lu (radiopharmaceutical therapy), with the goal of developing safer and more efficacious treatment options for prostate cancer. Methods: L804 was compared with the current gold standard chelators, DOTA and deferoxamine (DFO), conjugated to IAB2MA for radiolabeling with 177Lu and 89Zr in cell binding, preclinical biodistribution, imaging, dosimetry, and efficacy studies in the PSMA-positive PC3-PIP tumor-bearing mouse model of prostate cancer. Results: Quantitative radiolabeling (>99% radiochemical yield) of L804-IAB2MA with 177Lu or 89Zr was achieved at ambient temperature in under 30 min, comparable to 89Zr labeling of DFO-IAB2MA. In contrast, DOTA-IAB2MA was radiolabeled with 177Lu for 30 min at 37°C in approximately 90% radiochemical yield, requiring further purification. Using europium(III) as a luminescent surrogate, high binding affinity of Eu-L804-IAB2MA to PSMA was demonstrated in PC3-PIP cells (dissociation constant, 4.6 ± 0.6 nM). All 4 radiolabeled constructs showed significantly higher levels of internalization after 30 min in the PC3-PIP cells than in PSMA-negative PC3-FLU cells. The accumulation of 177Lu- and 89Zr-L804-IAB2MA in PC3-PIP tumors and all organs examined (i.e., heart, liver, spleen, kidney, muscle, salivary glands, lacrimal glands, carcass, and bone) was significantly lower than that of 177Lu-DOTA-IAB2MA and 89Zr-DFO-IAB2MA at 96 and 72 h after injection, respectively. Generally, SPECT/CT and PET/CT imaging data showed no significant difference in the SUVmean of the tumors or muscle between the radiotracers. Dosimetry analysis via both organ-level and voxel-level dose calculation methods indicated significantly higher absorbed doses of 177Lu-DOTA-IAB2MA in tumors, kidney, liver, muscle, and spleen than of 177Lu-L804-IAB2MA. PC3-PIP tumor-bearing mice treated with single doses of 177Lu-L804-IAB2MA (18.4 or 22.2 MBq) exhibited significantly prolonged survival and reduced tumor volume compared with unlabeled minibody control. No significant difference in survival was observed between groups of mice treated with 177Lu-L804-IAB2MA or 177Lu-DOTA-IAB2MA (18.4 or 22.2 MBq). Treatment with 177Lu-L804-IAB2MA resulted in lower absorbed doses in tumors and less toxicity than that of 177Lu-DOTA-IAB2MA. Conclusion: 89Zr- and 177Lu-L804-IAB2MA may be a promising theranostic pair for imaging and therapy of prostate cancer.

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